• Breaking: Nano/Microbot Self Assembly Of Rubbery Clot Filmed In C19 Unvaxxed - Same as Vaxxed and Deceased Clots. Clot Develops Despite Being On Blood Thinners In Patient With Strokes & Heart Attack
    Ana Maria Mihalcea, MD, PhD

    Image: Left: 30 cc COVID19 unvaccinated blood was drawn, after 3 hours rubbery clot formation can be seen. Right: Rubbery Clot

    Here I document investigation of rubbery clots in a COVID19 unvaccinated patient mid 60’s with history of acute myocardial infarction in 2020, who developed multiple embolic strokes from blood clots after heart catheterisation. He was treated with Aspirin, Plavix and Eliquis - all three are blood thinners. In 2022 the patient developed congestive heart failure and Atrial fibrillation, hence remained on Eliquis. In August 2024, after receiving dental anesthetics during another hospitalization a clot in his left ventricle was found while on Eliquis. The patient came to me for second opinion on self assembly nanotechnology possibly causing ongoing blood clotting.

    I had previously reported rubbery blood clot formation from shedding in a patient on multiple blood thinners:

    Rubbery Clot Development In C19 Unvaccinated Individual With Previous Deep Vein Thrombosis and Massive Pulmonary Emboli - While On Eliquis, Nattokinase, Lumbrokinase and Serreptase

    I also showed that COVID19 unvaccinated blood creates rubbery clots that can be inhibited by EDTA/ Vitamin C and Methylene Blue:

    C19 Unvaccinated Have Same Blood Clotting Problem As C19 Vaccinated - EDTA And Vitamin C Prevents Blood Clotting In C19 Unvaccinated

    Methylene Blue Prevents Rubbery Clot Formation, Essential Oils Help Too - Experiment Documentation

    I have been reporting on unvaccinated rubbery clots since 2022:

    Huge Rubbery Blood Clots In An Unvaccinated Individual - From Shedding? What Are They Made Of? A Call For Help To Analyze

    Clifford Carnicom and I also investigated rubbery clots of deceased vaccinated, living vaccinated and living unvaccinated people:

    Blood Clot Analysis From Living & Deceased Individuals Shows Consistent Findings: A Rubber Like Polymerized Protein - Microscopy Shows Filaments. Part 1 of 3 - Dr. Ana Mihalcea With Clifford Carnicom

    Blood Clot Analysis From Living And Deceased Individuals Near Infrared Spectroscopy Shows Multiple Hydrogel Polymer Components - Part 2 of 3 - Dr. Ana Mihalcea With Clifford Carnicom

    Blood Clot Analysis From Living And Deceased Individuals - Preliminary Chemical Solubility Testing - Part 3 of 3 - Dr. Ana Mihalcea With Clifford Carnicom

    The clot was completely rubbery as you can see in this video:

    I then did microscopy on the rubber top part and the transition to the red part of the clot. The yellow rubbery part looks exactly like the polymer sheets that I found in COVID19 vaccinated blood clots:

    Microscopic Analysis Of A Blood Clot From A C19 Vaccine Injured Individual


    Image: COVID19 unvaccinated polymer sheets. Rubbery part of the clot

    The red part of the clot also contained polymer with more cells as well as the spherical liposomes:


    Then I found how the liposomes are assembling the rubbery clot by using up the red blood cells to form large polymer mesh networks:


    Image: spherical polymer micelles and red blood cells within the unvaccinated clot

    Below you can see at 4000x magnification that nano and microbots are self assembling the polymer clot part while interacting with the already present micellar mesh network:

    Below you can see that nanobots, barely visible ( estimated maybe 500nm) are working to create the polymer backbone for the rubbery clot:

    In this video you can see the work is dimensional - you can see a larger light emitting microrobot at work on the micellar polymer clot. Tiny nanobots can also be seen swarming and using the red blood cells as a substrate to create solid polymer sheets. 4000x magnification:

    Summary:

    For the first time, the self assembly process of self assembly nanotechnology creating the rubbery clots is documented here - however that only confirms many other research articles linked above and findings that are now compiled in the two books TransHuman.

    I have some ethical questions regarding doctors who continue to ignore this information, while routine blood thinners do not work and people continue to have severe adverse health events. Because of the nature of my clinic, I see patients having blood clots on routine blood thinners a lot, as well as unvaccinated turbo cancer patients with self assembly nanotechnology in their blood. The cause is not addressed by the “regular doctors”.

    It is known that EDTA and Vitamin C inhibits nanoparticles from self assembling according to the Moderna patent.

    Another Confirmation: EDTA Combined With Vitamin C And Other Antioxidants Inhibits Nano Particle Polymerization In New Moderna Patent

    Breaking News: Calcium Disodium EDTA +Vitamin C Deactivates Nano/Microrobots And Dissolves All Microchips In Pfizer COVID19 "Vaccine"- Darkfield Microscopy

    Should the doctors who continue to ignore this and fail to investigate be tried for negligence and complicitness in genocide in a court of law? Would that wake up the medical community? Should the media that is not willing to report on the self assembly nanotechnology be made liable? The fact that we can find this in unvaccinated blood does not concern people?

    How many people have to die while this information continues to be ignored by mainstream and even much of the “health freedom movement”? What kind of health freedom do you have if people knowingly are unwilling to look at the facts?

    Self assembly nanotechnology is an inconvenient truth. But it certainly is not as inconvenient as dying suddenly.

    Unless people start to get really mad that their health concerns are not addressed appropriately by looking at this research, we will not have change in the system.

    How hard is it to draw 30ml of blood, let it sit for a few hours or overnight and take a look at the rubbery clot formation? HOW HARD IS THAT WHEN YOU COULD SAVE A LIFE DOING IT???? What kind of an ethical and moral standard do you have as a health care provider if you don’t do it?

    Is it time for you as a “healthcare consumer and patient” to demand it?


    TransHuman books

    https://anamihalceamdphd.substack.com/p/breaking-nanomicrobot-self-assembly?triedRedirect=true
    Breaking: Nano/Microbot Self Assembly Of Rubbery Clot Filmed In C19 Unvaxxed - Same as Vaxxed and Deceased Clots. Clot Develops Despite Being On Blood Thinners In Patient With Strokes & Heart Attack Ana Maria Mihalcea, MD, PhD Image: Left: 30 cc COVID19 unvaccinated blood was drawn, after 3 hours rubbery clot formation can be seen. Right: Rubbery Clot Here I document investigation of rubbery clots in a COVID19 unvaccinated patient mid 60’s with history of acute myocardial infarction in 2020, who developed multiple embolic strokes from blood clots after heart catheterisation. He was treated with Aspirin, Plavix and Eliquis - all three are blood thinners. In 2022 the patient developed congestive heart failure and Atrial fibrillation, hence remained on Eliquis. In August 2024, after receiving dental anesthetics during another hospitalization a clot in his left ventricle was found while on Eliquis. The patient came to me for second opinion on self assembly nanotechnology possibly causing ongoing blood clotting. I had previously reported rubbery blood clot formation from shedding in a patient on multiple blood thinners: Rubbery Clot Development In C19 Unvaccinated Individual With Previous Deep Vein Thrombosis and Massive Pulmonary Emboli - While On Eliquis, Nattokinase, Lumbrokinase and Serreptase I also showed that COVID19 unvaccinated blood creates rubbery clots that can be inhibited by EDTA/ Vitamin C and Methylene Blue: C19 Unvaccinated Have Same Blood Clotting Problem As C19 Vaccinated - EDTA And Vitamin C Prevents Blood Clotting In C19 Unvaccinated Methylene Blue Prevents Rubbery Clot Formation, Essential Oils Help Too - Experiment Documentation I have been reporting on unvaccinated rubbery clots since 2022: Huge Rubbery Blood Clots In An Unvaccinated Individual - From Shedding? What Are They Made Of? A Call For Help To Analyze Clifford Carnicom and I also investigated rubbery clots of deceased vaccinated, living vaccinated and living unvaccinated people: Blood Clot Analysis From Living & Deceased Individuals Shows Consistent Findings: A Rubber Like Polymerized Protein - Microscopy Shows Filaments. Part 1 of 3 - Dr. Ana Mihalcea With Clifford Carnicom Blood Clot Analysis From Living And Deceased Individuals Near Infrared Spectroscopy Shows Multiple Hydrogel Polymer Components - Part 2 of 3 - Dr. Ana Mihalcea With Clifford Carnicom Blood Clot Analysis From Living And Deceased Individuals - Preliminary Chemical Solubility Testing - Part 3 of 3 - Dr. Ana Mihalcea With Clifford Carnicom The clot was completely rubbery as you can see in this video: I then did microscopy on the rubber top part and the transition to the red part of the clot. The yellow rubbery part looks exactly like the polymer sheets that I found in COVID19 vaccinated blood clots: Microscopic Analysis Of A Blood Clot From A C19 Vaccine Injured Individual Image: COVID19 unvaccinated polymer sheets. Rubbery part of the clot The red part of the clot also contained polymer with more cells as well as the spherical liposomes: Then I found how the liposomes are assembling the rubbery clot by using up the red blood cells to form large polymer mesh networks: Image: spherical polymer micelles and red blood cells within the unvaccinated clot Below you can see at 4000x magnification that nano and microbots are self assembling the polymer clot part while interacting with the already present micellar mesh network: Below you can see that nanobots, barely visible ( estimated maybe 500nm) are working to create the polymer backbone for the rubbery clot: In this video you can see the work is dimensional - you can see a larger light emitting microrobot at work on the micellar polymer clot. Tiny nanobots can also be seen swarming and using the red blood cells as a substrate to create solid polymer sheets. 4000x magnification: Summary: For the first time, the self assembly process of self assembly nanotechnology creating the rubbery clots is documented here - however that only confirms many other research articles linked above and findings that are now compiled in the two books TransHuman. I have some ethical questions regarding doctors who continue to ignore this information, while routine blood thinners do not work and people continue to have severe adverse health events. Because of the nature of my clinic, I see patients having blood clots on routine blood thinners a lot, as well as unvaccinated turbo cancer patients with self assembly nanotechnology in their blood. The cause is not addressed by the “regular doctors”. It is known that EDTA and Vitamin C inhibits nanoparticles from self assembling according to the Moderna patent. Another Confirmation: EDTA Combined With Vitamin C And Other Antioxidants Inhibits Nano Particle Polymerization In New Moderna Patent Breaking News: Calcium Disodium EDTA +Vitamin C Deactivates Nano/Microrobots And Dissolves All Microchips In Pfizer COVID19 "Vaccine"- Darkfield Microscopy Should the doctors who continue to ignore this and fail to investigate be tried for negligence and complicitness in genocide in a court of law? Would that wake up the medical community? Should the media that is not willing to report on the self assembly nanotechnology be made liable? The fact that we can find this in unvaccinated blood does not concern people? How many people have to die while this information continues to be ignored by mainstream and even much of the “health freedom movement”? What kind of health freedom do you have if people knowingly are unwilling to look at the facts? Self assembly nanotechnology is an inconvenient truth. But it certainly is not as inconvenient as dying suddenly. Unless people start to get really mad that their health concerns are not addressed appropriately by looking at this research, we will not have change in the system. How hard is it to draw 30ml of blood, let it sit for a few hours or overnight and take a look at the rubbery clot formation? HOW HARD IS THAT WHEN YOU COULD SAVE A LIFE DOING IT???? What kind of an ethical and moral standard do you have as a health care provider if you don’t do it? Is it time for you as a “healthcare consumer and patient” to demand it? TransHuman books https://anamihalceamdphd.substack.com/p/breaking-nanomicrobot-self-assembly?triedRedirect=true
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  • UPDATED: Graphene Oxide The Vector For Covid-19 Democide
    Dr. Ariyana Love (ND)
    On July 28, 2021, I wrote the article entitled, Graphene Oxide The Vector For Covid-19 Democide and published it on my Ambassador Love website.


    Following the publication of my article, I reported that Pfizer and Covid-19 vaccines are aerosolized (using graphene oxide lipid-nanoparticles) in a podcast on October 26, 2021.

    Fast-forward to July 14, 2023, when the FDA confirms that Graphene Oxide is in the mRNA COVID-19 vaccines after being forced to publish confidential Pfizer documents by order of the US Federal Court.

    Here’s the Pfizer document:


    Here’s Karen Kingston’s Substack on the disclosure of graphene oxide in Pfizer’s poison death jabs.

    Pfizer whistleblower Melissa McAtee has also revealed that up to 1/3rd Pfizer vials contained graphene oxide which Pfizer ignored.


    Please watch: BREAKING: Inside the Moderna Patent's Devastating Ingredients!


    Graphene Oxide The Vector For Covid-19 Democide

    by Dr. Ariyana Love (ND)

    A shocking new discovery was revealed in April 2021, when Health Canada recalled over a million KN95 face masks containing the highly toxic industrial chemical called GRAPHENE. The poisonous masks came from China’s Shandong Shengquan New Materials Co. Ltd.

    Following the announcement, Spain recalled millions of masks containing GRAPHENE yet children worldwide are still being forced to wear these poisonous masks in schools.

    I wrote about the GRAPHENE based hydrogels back in April. They’re scientifically called “Nanotubes” or “Nanoworms” and they’re being used in face masks and PCR swabs: Masks And Covid Tests Contain Nanotech Vaccines Without Informed Consent.

    Global Research published this article entitled: Face Masks Contain Graphene, A Poisonous Substance.

    GRAPHENE hydrogels are being intentionally marketed to kids as “nano-silver” and sold online in face masks. — See report.

    LA QUINTA COLUMNA

    I was approached by the Spanish-speaking WikiLeaks / Anonymous group in mid-June and asked to look into La Quinta Columna’s extensive research into Graphene Oxide as the potential vector for Covid-19 drug delivery. I especially trust the Spanish Wiki-Anons because they stood beside me when I was wrongfully targeted and cancel cultured by black anons and obvious gatekeepers, in 2019.

    On June 25, La Quinta Columna (The Fifth Column) broke the news on a Spanish television show — El Gato al Agua, that toxic GRAPHENE OXIDE had been found in massive quantities in the Pfizer “vaccine” analyzed by Dr. Pablo Campra of Madrid and other biochemists and academics at the University of Almeria, on the initiative of La Quinta Columna. The small group of Spanish researchers is headed by Dr. Ricardo Delgado and Dr. José Luis Sevillano, Investigative Journalist Ramola D. revealed.

    On June 29th, Europe Reloaded covered La Quinta Columna’s analysis of the Pfizer serum under microscopy that was published by Orwell City.

    La Quinta Columna then released a game-changing report on June 30th, demonstrating that GRAPHENE OXIDE is the key ingredient in Pfizer’s “Covid-19 vaccine” serum. It’s evident from La Quinta Columna’s website the amount of time they invested in researching GRAPHENE OXIDE.

    From Quinta Columna’s research, I learned that a company named Nanografi is manufacturing GRAPHENE OXIDE Nanotubes and intranasal vaccines for Covid-19 drug delivery. Nanografi also manufactures face masks! Now that’s very damning evidence!!

    Ramola D. then published an excellent article to The Everyday Concerned Citizen on July 5th, highlighting La Quinta Columna’s discovery and how GRAPHENE OXIDE causes blood clotting and magnetism.

    A second Spanish research team independent from Quinta Columna found GRAPHENE OXIDE as the predominant ingredient in AstraZeneca’s serum, reported State of The Nation.

    Dr. Jane Ruby, a medical professional of 20-years and a pharmaceutical drug development expert, picked up the story and discussed these vital revelations on the Stew Peters Show, on July 14th. She emphasized that the only reason Pfizer’s Covid-19 serum would contain over 99% GRAPHENE OXIDE “would be to mass murder people”.

    Dr. Ruby then returned to the Stew Peter’s Show on July 21st, to release more groundbreaking news about the horrific blood contamination of people who took the Pfizer and AstraZeneca injections. AstraZeneca by the way means “weapon that kills” in Sanskrit.

    A third research team from Argentina analyzed a vial of Moderna’s Covid-19 serum on July 21st and found that it contained 99.5% GRAPHENE OXIDE under spectroscopy, as reported by Orwell City.

    We now have not one, but three independent scientific studies establishing that the Pfizer, Moderna, and AstraZeneca serum’s all contain over 98% to 99.5% GRAPHENE OXIDE NANOPARTICLES!

    MAGNETISM AND MIND CONTROL

    All the “Covid-19 vaccines” and now flu “vaccines” are manufactured using the same GRAPHENE OXIDE nano-technology.

    There are hundreds of videos online demonstrating how the vaxxed have become magnetized. The unvaxxed are also becoming magnetized by transmission from the vaxxed to the unvaxxed.

    GRAPHENE OXIDE is a nanoparticle. These nanoparticles become magnetic when they reach the same temperature as the human body, according to scientific reports.

    Global Research news channel is also covering Quinta Columna’s research and the magnetism phenomenon: Graphene Oxide Particles in Covid mRNA “Vaccines” Causing Magnetism?.

    World renown scientist and media mogul Mike Adams from Natural News, is also researching and reporting on this developing story where he reveals that: Graphene-based “neuromodulation” technology is REAL: Press release from INBRAIN Neuroelectronics describes brain controlling biocircuits using AI-powered graphene.


    This graphene-based fitness patch was developed under the EU’s Graphene Flagship, by the Institute of Photonic Sciences in Spain can measure heart rate, breathing rate, and body temperature.
    Nano-tech GRAPHENE OXIDE is superconductive and highly integrative with neuron cells in the brain, as this scientific paper reveals.

    The molecules of GRAPHENE can interact with neurons in the brain in a remote mode using different radio-frequencies (5G could be one of these). They can map the brain and transmit and receive INSTRUCTIONS remotely.

    The European Union invested one billion euros in a project called “The Graphene Flagship“ in 2019, spawning nine companies and 46 new GRAPHENE-based products.

    INDUSTRIALIZED GRAPHENE OXIDE

    GRAPHENE OXIDE is already being widely used as an industrial chemical. We find it in electronics, aeronautics, energy, agriculture, cosmetics, medicine, textile production (also clothing), food processing, and buildings. The globalists intend to build “smart cities” using this nano-particulate substance and it’s already being sprayed on humanity via Bill Gates “smart dust”.

    Graphene Oxide Nanoparticles Are Being Sprayed On Humanity

    GRAPHENE OXIDE has already been aerosolized for dissemination over populations through aerial spraying (chemtrails). Pentagon scientists developed the technology in a Kazakhstan bioweapons lab. Please see this video (2 min.).

    This NATO plane was filmed spraying GRAPHENE OXIDE from above. Please see the video (.17 seconds). And finally, this Italian study provides additional proof that we are being sprayed with GRAPHENE FAMILY NANOPARTICLES.

    We’re literally being saturated with this industrial poison which has been intentionally inserted into everyday items such as face masks, food, clothing, water filtration, sanitary pads, tampons, diapers, and more. It’s being used in the Covid-19 “testing” swabs and now we know it’s the key ingredient in the “Covid-19 vaccines”. This article highlights 60 uses of GRAPHENE.

    Here’s a one-minute video clip of Moderna’s CEO Stephane Brancel bragging to the World Economic Forum about it taking just two days to create their “Covid-19 vaccine”. How is that possible unless it’s synthetic?

    GRAPHENE OXIDE MEDICAL APPLICATIONS

    In recent years, GRAPHENE has been exploited in the biomedical field, particularly for DNA sequencing and the development of biosensors. It’s presently being used for gene delivery and to administer drugs into biological cells.

    This article by Natural News contains links to the exact science papers describing two decades of research into all this: IT’S REAL: Science paper documents “self-assembled magnetic nanosystems” for cybernetic biocircuitry interface and control systems in humans, including “DNA hydrogel” tech.

    Dr. Carrie Madej and I have been reporting on the GRAPHENE Oxide Hydrogels which allow for self-replication, disassembling, and reassembling, and ballistic drug delivery to cells. The programmable nanoparticles also pass through the blood/brain barrier, causing PRION (auto-immune disease).

    WATCH! Graphene Oxide Activates By Cell Phone EMF Frequency Radiation

    The GRAPHENE Hydrogels literally grow a new neural network inside the human body and do so extremely rapidly. This was observed by a Slovakia team of researchers.

    GRAPHENE’s thermal property and electrical conductivity make it a superconductor. The artificial neuron network can receive and transmit signals and can be externally controlled through 5G frequency and AI. GRAPHENE Family Nanoparticles contain drug-chemical payloads for mRNA “gene therapy” and it’s being deployed without Informed Consent. GRAPHENE OXIDE is the vector for Moderna’s “operating system” and the sad reality is that the vaxxed will transform into genetically modified humans rapidly after inoculation because the technology is very advanced.

    CRISPR

    The first human genome project using GRAPHENE was initiated in 2001. GRAPHENE OXIDE was developed by CRSPR, Pfizer, Moderna, and BioNTech as mRNA gene therapy to cure cancer but due to its cytotoxicity (cell death) in healthy cells, this highly toxic industrial nano-chemical was never approved for use in humans.

    CRISPR accelerated the development of the first Genome Sensor, the world’s first DNA search engine that runs on CRISPR-Chip technology. It can literally google genomes to detect genetic mutations and variations.

    The jagged edges of GRAPHENE OXIDE Nanoparticles are super sharp and super strong, easily piercing through cell membranes in human lung, skin, and immune cells, suggesting the potential to do quite serious damage in humans and other animals.

    GRAPHENE OXIDE is great for DNA sequencing (cutting and splicing of genes) and it’s perfect for evil eugenicists who want to pretend to be God’s and genetically enslave the rest of humanity. This substance is extremely dangerous to humans and to the environment.

    TRANSMISSION

    Europe Reloaded reports: “Graphene Oxide has a certain magnetic resonance band, beyond which it becomes excited, which in turn leads to rapid oxidization of the material. When the oxidization level exceeds certain body biomarkers, it triggers a collapse of the immune system and a cytokine storm, typical of “severe Covid-19” symptoms.

    At least 90 scientific studies show the toxic effect of GRAPHENE OXIDE in the human body produces the same clinical effects as Covid-19. These symptoms include programmable cell death, blood coagulation, platelet aggregation, clotting, cytokine storms, thromboses, pneumonia (flu-like symptoms), inflammation of the mucous membranes, loss of taste and smell. It blocks detoxification in the body by blocking glutathione, creates a metallic taste in the mouth, destroys the immune system, and magnetizes people, especially at the injection site.

    Please see: Graphene Oxide Blockbuster: It Causes CV Symptoms and is Present in all Aspects of Diagnosis and Treatment

    Also see: Video: Graphene Oxide: A Toxic Substance in the Vial of the COVID-19 mRNA Vaccine

    GRAPHENE OXIDE Toxicity was researched and discovered to be a vector for transmission in mice, enabling Pfizer’s “self-replicating vaccines”.

    “The common administration routes in animal models include AIRWAY EXPOSURE (intranasal insufflation, intratracheal instillation, and inhalation), oral administration, intravenous injection, intraperitoneal injection and subcutaneous injection. The major exposure route for GFNs (Graphene Family Nanoparticles) in the working environment is AIRWAY EXPOSURE, thus INHALATION and intratracheal instillation are used mostly in mice to simulate human exposure to GFNs.”

    Here’s a second peer-reviewed study confirming that Graphene Oxide toxicity transmission from the vaxxed to the unvaxxed is airborne. This means GRAPHENE OXIDE is received from the vaxxed to the unvaxxed by inhalation.

    GRAPHENE OXIDE COLOR


    Graphene Oxide (GO) and Reduced Graphene Oxide (RGO)
    Cytotoxicity depends on the size of the GRAPHENE flakes and the content of oxygen. It’s possible to tweak the GRAPHENE to be more or less toxic. It is in fact possible to get GRAPHENE OXIDE in a clear liquid serum by reducing its oxygen content into a Reduced Graphene Oxide (RHO). By doing so, it will increase toxicity.

    Treating GRAPHENE OXIDE with hydrazine both removes the debris and reduces (both deoxygenations) the dark GRAPHENE sheets. Reduction of a clear GRAPHENE OXIDE solution using Sodium Dithionite will cause the microscopic GRAPHENE flakes to reappear “out of nothing”.

    Reduced Graphene Oxide is sold as a clear serum in India for example, here.

    Conclusion: DEMOCIDE

    These were never “vaccines” against a virus, instead all the time it was a secret nanotech project developed to reach and control the brains of the human population. People have been already magnetized with GRAPHENE which is present in masks, Covid tests, chemtrails, influenza, and Covid “vaccines”.

    We now have three comparative studies proving that GRAPHENE OXIDE is the vector for the Covid-19 BIOWEAPONS drug/chemical delivery. These are not “vaccines” but mRNA gene therapies and industrial chemicals without authorized use in humans.

    The pharma cartel is finished! People will never trust big pharma again. These companies are making a killing poisoning us and terraforming our environment. Nanoparticles are programmed either for good and healing or for ill intent. These programmable robots aren’t just randomly used. This technology obviously got into the hands of the wrong people (eugenicists) or it was developed with the intent to Democide.

    GRAPHENE OXIDE NANOPARTICLES is the perfect vector to carry the spike protein poisons that were cultivated in moths, enhanced, and weaponized in labs. GRAPHENE OXIDE NANOPARTICLES is the perfect vector for transmission into healthy cells by injection, air inhalation, and medical devices (masks, swabs, needles).

    Transmission is not caused by the shedding of viral loads because there is no virus. “Coronavirus” and Covid-19 are the distractions while governments conduct Democide on all the world’s population. This is a biological attack on our DNA. We are being literally saturated with GRAPHENE FAMILY NANOPARTICLES and the only good news is that you can detox it out of your body.

    Our best legal teams, World Freedom Alliance and World Doctors Alliance have advised that we are now beyond Genocide and surviving a DEMOCIDE. This is an extinction-level mass culling. Genocide is when a government targets a specific demographic or religious group like Africans, Native Americans, Jews, Muslims or poor people, for example. Democide is far worse than Genocide because governments are targeting the entire population of men, women, and children for worldwide depopulation.

    So please, STOP paying taxes at once! The only way this war will end is when we end it and the only way to do that is to stop feeding the Beast. We must march in droves to ALL federal, state, and local parliaments and city council buildings. Surround those buildings until government leaders come out. We must take back what’s ours. Remember, we own it all. We The People already have the legal backing of Reiner Fuellmich’s team at the World Freedom Alliance.

    Finally, I agree with La Quinta Columna’s assessment when they said, “Every person who has been inoculated with this substance with that graphene oxide nanotechnology has a fuse, dynamite, a time bomb that’s ready to explode by the activation of a microwave.”

    DETOX

    I have two published protocols for detoxing graphene oxide nanoparticles and for boosting immunity. My premium detox protocol and my affordable for all detox protocol.

    Please schedule a health consultation with me for customized protocol support.

    ADDITIONAL ARTICLES

    Please see: Latest news release from Quinta Columna here.

    Please see: FEMA whistleblower with Celeste Solum in her latest interview (very important!) on Frequency Wars, here.

    Please see: Dr. Roger Hodkinson Blows Whistle To Reiner Fuellmich and reveals that Covid-19 is aerosolized through the sweat glands.

    Please see: CDC withdraws fraudulent PCR testing protocol that was used to falsify covid “positives” to push the plandemic

    Please see: The Vaxxed Are Being Liquefied & Spread On Crops (Video 1 min.)

    https://drloveariyana.substack.com/p/updated-graphene-oxide-the-vector
    UPDATED: Graphene Oxide The Vector For Covid-19 Democide Dr. Ariyana Love (ND) On July 28, 2021, I wrote the article entitled, Graphene Oxide The Vector For Covid-19 Democide and published it on my Ambassador Love website. Following the publication of my article, I reported that Pfizer and Covid-19 vaccines are aerosolized (using graphene oxide lipid-nanoparticles) in a podcast on October 26, 2021. Fast-forward to July 14, 2023, when the FDA confirms that Graphene Oxide is in the mRNA COVID-19 vaccines after being forced to publish confidential Pfizer documents by order of the US Federal Court. Here’s the Pfizer document: Here’s Karen Kingston’s Substack on the disclosure of graphene oxide in Pfizer’s poison death jabs. Pfizer whistleblower Melissa McAtee has also revealed that up to 1/3rd Pfizer vials contained graphene oxide which Pfizer ignored. Please watch: BREAKING: Inside the Moderna Patent's Devastating Ingredients! Graphene Oxide The Vector For Covid-19 Democide by Dr. Ariyana Love (ND) A shocking new discovery was revealed in April 2021, when Health Canada recalled over a million KN95 face masks containing the highly toxic industrial chemical called GRAPHENE. The poisonous masks came from China’s Shandong Shengquan New Materials Co. Ltd. Following the announcement, Spain recalled millions of masks containing GRAPHENE yet children worldwide are still being forced to wear these poisonous masks in schools. I wrote about the GRAPHENE based hydrogels back in April. They’re scientifically called “Nanotubes” or “Nanoworms” and they’re being used in face masks and PCR swabs: Masks And Covid Tests Contain Nanotech Vaccines Without Informed Consent. Global Research published this article entitled: Face Masks Contain Graphene, A Poisonous Substance. GRAPHENE hydrogels are being intentionally marketed to kids as “nano-silver” and sold online in face masks. — See report. LA QUINTA COLUMNA I was approached by the Spanish-speaking WikiLeaks / Anonymous group in mid-June and asked to look into La Quinta Columna’s extensive research into Graphene Oxide as the potential vector for Covid-19 drug delivery. I especially trust the Spanish Wiki-Anons because they stood beside me when I was wrongfully targeted and cancel cultured by black anons and obvious gatekeepers, in 2019. On June 25, La Quinta Columna (The Fifth Column) broke the news on a Spanish television show — El Gato al Agua, that toxic GRAPHENE OXIDE had been found in massive quantities in the Pfizer “vaccine” analyzed by Dr. Pablo Campra of Madrid and other biochemists and academics at the University of Almeria, on the initiative of La Quinta Columna. The small group of Spanish researchers is headed by Dr. Ricardo Delgado and Dr. José Luis Sevillano, Investigative Journalist Ramola D. revealed. On June 29th, Europe Reloaded covered La Quinta Columna’s analysis of the Pfizer serum under microscopy that was published by Orwell City. La Quinta Columna then released a game-changing report on June 30th, demonstrating that GRAPHENE OXIDE is the key ingredient in Pfizer’s “Covid-19 vaccine” serum. It’s evident from La Quinta Columna’s website the amount of time they invested in researching GRAPHENE OXIDE. From Quinta Columna’s research, I learned that a company named Nanografi is manufacturing GRAPHENE OXIDE Nanotubes and intranasal vaccines for Covid-19 drug delivery. Nanografi also manufactures face masks! Now that’s very damning evidence!! Ramola D. then published an excellent article to The Everyday Concerned Citizen on July 5th, highlighting La Quinta Columna’s discovery and how GRAPHENE OXIDE causes blood clotting and magnetism. A second Spanish research team independent from Quinta Columna found GRAPHENE OXIDE as the predominant ingredient in AstraZeneca’s serum, reported State of The Nation. Dr. Jane Ruby, a medical professional of 20-years and a pharmaceutical drug development expert, picked up the story and discussed these vital revelations on the Stew Peters Show, on July 14th. She emphasized that the only reason Pfizer’s Covid-19 serum would contain over 99% GRAPHENE OXIDE “would be to mass murder people”. Dr. Ruby then returned to the Stew Peter’s Show on July 21st, to release more groundbreaking news about the horrific blood contamination of people who took the Pfizer and AstraZeneca injections. AstraZeneca by the way means “weapon that kills” in Sanskrit. A third research team from Argentina analyzed a vial of Moderna’s Covid-19 serum on July 21st and found that it contained 99.5% GRAPHENE OXIDE under spectroscopy, as reported by Orwell City. We now have not one, but three independent scientific studies establishing that the Pfizer, Moderna, and AstraZeneca serum’s all contain over 98% to 99.5% GRAPHENE OXIDE NANOPARTICLES! MAGNETISM AND MIND CONTROL All the “Covid-19 vaccines” and now flu “vaccines” are manufactured using the same GRAPHENE OXIDE nano-technology. There are hundreds of videos online demonstrating how the vaxxed have become magnetized. The unvaxxed are also becoming magnetized by transmission from the vaxxed to the unvaxxed. GRAPHENE OXIDE is a nanoparticle. These nanoparticles become magnetic when they reach the same temperature as the human body, according to scientific reports. Global Research news channel is also covering Quinta Columna’s research and the magnetism phenomenon: Graphene Oxide Particles in Covid mRNA “Vaccines” Causing Magnetism?. World renown scientist and media mogul Mike Adams from Natural News, is also researching and reporting on this developing story where he reveals that: Graphene-based “neuromodulation” technology is REAL: Press release from INBRAIN Neuroelectronics describes brain controlling biocircuits using AI-powered graphene. This graphene-based fitness patch was developed under the EU’s Graphene Flagship, by the Institute of Photonic Sciences in Spain can measure heart rate, breathing rate, and body temperature. Nano-tech GRAPHENE OXIDE is superconductive and highly integrative with neuron cells in the brain, as this scientific paper reveals. The molecules of GRAPHENE can interact with neurons in the brain in a remote mode using different radio-frequencies (5G could be one of these). They can map the brain and transmit and receive INSTRUCTIONS remotely. The European Union invested one billion euros in a project called “The Graphene Flagship“ in 2019, spawning nine companies and 46 new GRAPHENE-based products. INDUSTRIALIZED GRAPHENE OXIDE GRAPHENE OXIDE is already being widely used as an industrial chemical. We find it in electronics, aeronautics, energy, agriculture, cosmetics, medicine, textile production (also clothing), food processing, and buildings. The globalists intend to build “smart cities” using this nano-particulate substance and it’s already being sprayed on humanity via Bill Gates “smart dust”. Graphene Oxide Nanoparticles Are Being Sprayed On Humanity GRAPHENE OXIDE has already been aerosolized for dissemination over populations through aerial spraying (chemtrails). Pentagon scientists developed the technology in a Kazakhstan bioweapons lab. Please see this video (2 min.). This NATO plane was filmed spraying GRAPHENE OXIDE from above. Please see the video (.17 seconds). And finally, this Italian study provides additional proof that we are being sprayed with GRAPHENE FAMILY NANOPARTICLES. We’re literally being saturated with this industrial poison which has been intentionally inserted into everyday items such as face masks, food, clothing, water filtration, sanitary pads, tampons, diapers, and more. It’s being used in the Covid-19 “testing” swabs and now we know it’s the key ingredient in the “Covid-19 vaccines”. This article highlights 60 uses of GRAPHENE. Here’s a one-minute video clip of Moderna’s CEO Stephane Brancel bragging to the World Economic Forum about it taking just two days to create their “Covid-19 vaccine”. How is that possible unless it’s synthetic? GRAPHENE OXIDE MEDICAL APPLICATIONS In recent years, GRAPHENE has been exploited in the biomedical field, particularly for DNA sequencing and the development of biosensors. It’s presently being used for gene delivery and to administer drugs into biological cells. This article by Natural News contains links to the exact science papers describing two decades of research into all this: IT’S REAL: Science paper documents “self-assembled magnetic nanosystems” for cybernetic biocircuitry interface and control systems in humans, including “DNA hydrogel” tech. Dr. Carrie Madej and I have been reporting on the GRAPHENE Oxide Hydrogels which allow for self-replication, disassembling, and reassembling, and ballistic drug delivery to cells. The programmable nanoparticles also pass through the blood/brain barrier, causing PRION (auto-immune disease). WATCH! Graphene Oxide Activates By Cell Phone EMF Frequency Radiation The GRAPHENE Hydrogels literally grow a new neural network inside the human body and do so extremely rapidly. This was observed by a Slovakia team of researchers. GRAPHENE’s thermal property and electrical conductivity make it a superconductor. The artificial neuron network can receive and transmit signals and can be externally controlled through 5G frequency and AI. GRAPHENE Family Nanoparticles contain drug-chemical payloads for mRNA “gene therapy” and it’s being deployed without Informed Consent. GRAPHENE OXIDE is the vector for Moderna’s “operating system” and the sad reality is that the vaxxed will transform into genetically modified humans rapidly after inoculation because the technology is very advanced. CRISPR The first human genome project using GRAPHENE was initiated in 2001. GRAPHENE OXIDE was developed by CRSPR, Pfizer, Moderna, and BioNTech as mRNA gene therapy to cure cancer but due to its cytotoxicity (cell death) in healthy cells, this highly toxic industrial nano-chemical was never approved for use in humans. CRISPR accelerated the development of the first Genome Sensor, the world’s first DNA search engine that runs on CRISPR-Chip technology. It can literally google genomes to detect genetic mutations and variations. The jagged edges of GRAPHENE OXIDE Nanoparticles are super sharp and super strong, easily piercing through cell membranes in human lung, skin, and immune cells, suggesting the potential to do quite serious damage in humans and other animals. GRAPHENE OXIDE is great for DNA sequencing (cutting and splicing of genes) and it’s perfect for evil eugenicists who want to pretend to be God’s and genetically enslave the rest of humanity. This substance is extremely dangerous to humans and to the environment. TRANSMISSION Europe Reloaded reports: “Graphene Oxide has a certain magnetic resonance band, beyond which it becomes excited, which in turn leads to rapid oxidization of the material. When the oxidization level exceeds certain body biomarkers, it triggers a collapse of the immune system and a cytokine storm, typical of “severe Covid-19” symptoms. At least 90 scientific studies show the toxic effect of GRAPHENE OXIDE in the human body produces the same clinical effects as Covid-19. These symptoms include programmable cell death, blood coagulation, platelet aggregation, clotting, cytokine storms, thromboses, pneumonia (flu-like symptoms), inflammation of the mucous membranes, loss of taste and smell. It blocks detoxification in the body by blocking glutathione, creates a metallic taste in the mouth, destroys the immune system, and magnetizes people, especially at the injection site. Please see: Graphene Oxide Blockbuster: It Causes CV Symptoms and is Present in all Aspects of Diagnosis and Treatment Also see: Video: Graphene Oxide: A Toxic Substance in the Vial of the COVID-19 mRNA Vaccine GRAPHENE OXIDE Toxicity was researched and discovered to be a vector for transmission in mice, enabling Pfizer’s “self-replicating vaccines”. “The common administration routes in animal models include AIRWAY EXPOSURE (intranasal insufflation, intratracheal instillation, and inhalation), oral administration, intravenous injection, intraperitoneal injection and subcutaneous injection. The major exposure route for GFNs (Graphene Family Nanoparticles) in the working environment is AIRWAY EXPOSURE, thus INHALATION and intratracheal instillation are used mostly in mice to simulate human exposure to GFNs.” Here’s a second peer-reviewed study confirming that Graphene Oxide toxicity transmission from the vaxxed to the unvaxxed is airborne. This means GRAPHENE OXIDE is received from the vaxxed to the unvaxxed by inhalation. GRAPHENE OXIDE COLOR Graphene Oxide (GO) and Reduced Graphene Oxide (RGO) Cytotoxicity depends on the size of the GRAPHENE flakes and the content of oxygen. It’s possible to tweak the GRAPHENE to be more or less toxic. It is in fact possible to get GRAPHENE OXIDE in a clear liquid serum by reducing its oxygen content into a Reduced Graphene Oxide (RHO). By doing so, it will increase toxicity. Treating GRAPHENE OXIDE with hydrazine both removes the debris and reduces (both deoxygenations) the dark GRAPHENE sheets. Reduction of a clear GRAPHENE OXIDE solution using Sodium Dithionite will cause the microscopic GRAPHENE flakes to reappear “out of nothing”. Reduced Graphene Oxide is sold as a clear serum in India for example, here. Conclusion: DEMOCIDE These were never “vaccines” against a virus, instead all the time it was a secret nanotech project developed to reach and control the brains of the human population. People have been already magnetized with GRAPHENE which is present in masks, Covid tests, chemtrails, influenza, and Covid “vaccines”. We now have three comparative studies proving that GRAPHENE OXIDE is the vector for the Covid-19 BIOWEAPONS drug/chemical delivery. These are not “vaccines” but mRNA gene therapies and industrial chemicals without authorized use in humans. The pharma cartel is finished! People will never trust big pharma again. These companies are making a killing poisoning us and terraforming our environment. Nanoparticles are programmed either for good and healing or for ill intent. These programmable robots aren’t just randomly used. This technology obviously got into the hands of the wrong people (eugenicists) or it was developed with the intent to Democide. GRAPHENE OXIDE NANOPARTICLES is the perfect vector to carry the spike protein poisons that were cultivated in moths, enhanced, and weaponized in labs. GRAPHENE OXIDE NANOPARTICLES is the perfect vector for transmission into healthy cells by injection, air inhalation, and medical devices (masks, swabs, needles). Transmission is not caused by the shedding of viral loads because there is no virus. “Coronavirus” and Covid-19 are the distractions while governments conduct Democide on all the world’s population. This is a biological attack on our DNA. We are being literally saturated with GRAPHENE FAMILY NANOPARTICLES and the only good news is that you can detox it out of your body. Our best legal teams, World Freedom Alliance and World Doctors Alliance have advised that we are now beyond Genocide and surviving a DEMOCIDE. This is an extinction-level mass culling. Genocide is when a government targets a specific demographic or religious group like Africans, Native Americans, Jews, Muslims or poor people, for example. Democide is far worse than Genocide because governments are targeting the entire population of men, women, and children for worldwide depopulation. So please, STOP paying taxes at once! The only way this war will end is when we end it and the only way to do that is to stop feeding the Beast. We must march in droves to ALL federal, state, and local parliaments and city council buildings. Surround those buildings until government leaders come out. We must take back what’s ours. Remember, we own it all. We The People already have the legal backing of Reiner Fuellmich’s team at the World Freedom Alliance. Finally, I agree with La Quinta Columna’s assessment when they said, “Every person who has been inoculated with this substance with that graphene oxide nanotechnology has a fuse, dynamite, a time bomb that’s ready to explode by the activation of a microwave.” DETOX I have two published protocols for detoxing graphene oxide nanoparticles and for boosting immunity. My premium detox protocol and my affordable for all detox protocol. Please schedule a health consultation with me for customized protocol support. ADDITIONAL ARTICLES Please see: Latest news release from Quinta Columna here. Please see: FEMA whistleblower with Celeste Solum in her latest interview (very important!) on Frequency Wars, here. Please see: Dr. Roger Hodkinson Blows Whistle To Reiner Fuellmich and reveals that Covid-19 is aerosolized through the sweat glands. Please see: CDC withdraws fraudulent PCR testing protocol that was used to falsify covid “positives” to push the plandemic Please see: The Vaxxed Are Being Liquefied & Spread On Crops (Video 1 min.) https://drloveariyana.substack.com/p/updated-graphene-oxide-the-vector
    DRLOVEARIYANA.SUBSTACK.COM
    UPDATED: Graphene Oxide The Vector For Covid-19 Democide
    On July 28, 2021, I wrote the article entitled, Graphene Oxide The Vector For Covid-19 Democide and published it on my Ambassador Love website.
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  • University of Tokyo - Scientists cool positronium to near absolute zero for antimatter research:

    https://phys.org/news/2024-09-scientists-cool-positronium-absolute-antimatter.html

    #Positronium #Positron #Antimatter #Spectroscopy #Supercooling #ChirpedLaser #LASER #Cosmology #Physics
    University of Tokyo - Scientists cool positronium to near absolute zero for antimatter research: https://phys.org/news/2024-09-scientists-cool-positronium-absolute-antimatter.html #Positronium #Positron #Antimatter #Spectroscopy #Supercooling #ChirpedLaser #LASER #Cosmology #Physics
    PHYS.ORG
    Scientists cool positronium to near absolute zero for antimatter research
    Most atoms are made from positively charged protons, neutral neutrons and negatively charged electrons. Positronium is an exotic atom composed of a single negative electron and a positively charged antimatter positron. It is naturally very short-lived, but researchers including those from the University of Tokyo successfully cooled and slowed down samples of positronium using carefully tuned lasers.
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  • EDTA Snakeoil! Ana Maria Mihalcea's Medical Malfeasance Exposed
    “I already have had.. uh.. patients die from shedding” - Ana Maria Mihalcea, M.D.

    Dr. Ariyana Love (ND)
    “My people are destroyed for lack of knowledge: because thou hast rejected knowledge, I will also reject thee, that thou shalt be no priest to me: seeing thou hast forgotten the law of thy God, I will also forget thy children.” ~ Hosea 4:6 KJV

    Rockefeller Medicine

    Around 1900, the science world was getting excited about new “petrochemicals” and the ability to create a variety of new compounds from oil. Some of the first products derived from petrochemicals were plastics.

    In 1908, modern medicine was established by the Rockefeller’s and dubbed “Allopathy”. The Rockefeller’s created the business of modern medicine which has always been about poisoning people, Eustice Mullen explains.

    This is the definition of Allopathic medicine according to the NIH:

    “A system in which medical doctors and other health care professionals (such as nurses, pharmacists, and therapists) treat symptoms and diseases using drugs, radiation, or surgery.”

    The Rockefeller Institute for Medicine, founded in 1908, marked the advent of the re-creation of synthetic versions of natural cures. Prior to 1908, every place of healing in America, Europe and the world, used only ancient traditional natural medicinal cures. Every hospital was a “Homeopathic Hospital”. Most of these magnificent buildings were converted into mental health asylums where a system of torture and electric shock was established to “cure” mental illness.


    John D. Rockefeller created the oil industry and used it to crush traditional medicine in order to enslave people. They also financed the Eugenics movement. One of the perks of modern medicine is depopulation.

    “Everyone knows that the infamous Roe v. Wade opinion legalized abortion, but almost no one knows that legal abortion was a strategy by eugenicists, as early as 1939, to “genetically improve” the population by “reducing” it.”

    In the book, “Rockefeller Medicine Men: Medicine and Capitalism in America”, authored by E. Richard Brown, he tells the hidden story of the financial, political, and institutional manipulations whereby a diverse and eclectic range of traditional healing modalities available to the North American public was summarily canceled and pared down to a singular style of medicine that would become the predominant medicine of the Western world and a major force in global medical culture during the 20th century. This was brought about largely by the collaboration of the American Medical Association, the philanthropies of Andrew Carnegie and John D. Rockefeller, and the development of a revolutionary curriculum by the Johns Hopkins School of Medicine. Brown documents the story of how a powerful professional elite gained virtual hegemony in the Western theatre of healing by effectively taking control of the ethos and practice of Western medicine. E. Richard Brown describes how, in 1905, the American Medical Association’s new Council on Medical Education funded by Carnegie and Rockefeller commenced serious activity. They employed the services of Abraham Flexner who proceeded to visit and “assess” every single medical school in the US and Canada. Within a short time of this development, medical schools all around the US began to collapse or consolidate. By 1910, 30 schools had merged, and 21 had closed their doors. Of the 166 medical schools operating in 1904, 133 had survived by 1910, and 104 by 1915. Fifteen years later, only 76 schools of medicine existed in the US and they all followed the same curriculum.

    The 1910 Flexner Report laid the foundations of the modern medical system, dubbed “Rockefeller medicine” (Allopathy). Since 1910, corporate interests have established near total control of the medical field, both though pharmacology and through their impact on medical education.

    In 1935, vitamin C became the first vitamin to be artificially synthesized in Switzerland. Rockefeller saw a big opportunity with the possibility that vitamins and medications could be developed from petroleum. He saw the chance to control and monopolize multiple industries at once: petroleum, chemical and medical. Petrochemicals were ideal from a business perspective because they could be patented, owned and sold for high profits.

    Today, the petrochemicals in plastics are causing a slew of illnesses including neurodevelopmental disorders, diabetes, chronic respiratory disease, and cancer, which have increased between 28% and 150% between 1990 and 2019. Petrochemicals in microplastics are also rapidly reducing fertility in males in particular, and polluting our environment. Please also read more here, here, and here.

    The first pharmaceutical drug was an arsenic named Salvarsan. That’s right, an ARSENIC!

    DEATH is an all-to-common side effect of pharmaceutical drugs which is only logical when you administer poisons internally. The following pages demonstrate the many deaths of people around the world, most of them children, who were fatally poisoned during the first mass medication experiments with Rockefeller’s Allopathic health. The paper is entitled, Toward Responsibility in International Health: Death following Treatment in Rockefeller Hookworm Campaigns, 1914–1934.

    What is EDTA?

    EDTA is synthesized on an industrial scale using 1, 2-diaminoethane (ethylene diamine), formaldehyde, water and sodium cyanide.

    Ethylene diamine induced acute and subchronic toxicity in lab animals, also allergic hypersensitivity. The liver and kidneys are target organs of ethylenediamine, where they simply stop working.


    Read more: Is C60 And EDTA Safe? Clinical Review


    Absorption of large amounts of formaldehyde via any route can cause severe systemic toxicity, leading to metabolic acidosis, tissue and organ damage, and coma, according to the CDC.

    Exposure to sodium cyanide can be rapidly fatal. It has whole-body (systemic) effects, particularly affecting those organ systems most sensitive to low oxygen levels: the central nervous system (brain), the cardiovascular system (heart and blood vessels), and the pulmonary system (lungs), according to the CDC.

    EDTA is an industrial poison. The textile industry required a chelating agent to remove calcium during textile processing and this led to the synthesis of polyamino-carboxylic acids, one of which was EDTA. A patent was filed for EDTA in Germany in 1935, for industrial chemical use. EDTA is a synthetic acid effectively used to clean boiler rooms in nuclear power plants. In 1945, Franz Munz obtained a US EDTA patent in 1945. In 1947, EDTA was approved by the US Food and Drug Administration (FDA) as a food additive in “low doses” because it’s a forever chemical and a preservative.

    There are two different types of EDTA approved by the U.S. FDA. In 1953, Edetate calcium disodium also known as Calcium EDTA (marketed under the trade name Calcium Disodium Versenate registered ) was approved for the treatment of lead poisoning. Three years later, in 1956, a related EDTA compound, Edetate disodium, was also approved for clinical use. This compound, also known as Disodium EDTA, has been marketed under the trade names Disotate (registered) and Endrate (registered). The essential difference between these two compounds is that Calcium EDTA's structure has an incorporated Ca super(2+) moiety while Disodium EDTA does not. The use of the latter compound, Disodium EDTA, has been associated with life-threatening and fatal hypocalcemia.

    EDTA trial DEATHS

    An EDTA trial (Sloth-Nielsen et al., 1981) on the possible antiatherogenic effect of EDTA with 6 patients, showed clinical signs of potentially lethal hypocalcemia from abnormally low calcium levels caused by EDTA.

    Another EDTA chelation human trial in 2003-2005 resulted in DEATHS due to hypocalcemia.

    A 2006 EDTA chelation trial also resulted in DEATHS due to hypocalcemia.

    There were several DEATHS reported from cardiac arrest due to lethal hypocalcemia in EDTA trials in 2006 and 2008 and (Brown, Willis, Omalu, & Leiker, 2006; Baxter & Krenzelok, 2008), from calcium deficiency inducing alterations in the brain, and osteoporosis, which causes the bones to become brittle.

    In 2008, a clinical trial with EDTA chelation on autistic children also proved fatal, resulting in DEATHS of children.

    A 2007 EDTA chelation study proved KIDNEY FAILURE in humans.

    Decades of clinical studies demonstrate that EDTA treatment is associated with severe, life-threatening adverse effects, as Science Direct explained in 2016.

    “It should be emphasized that EDTA treatment is associated with severe, life-threatening adverse effects.

    EDTA for cardiovascular disease DEBUNKED

    Many Allopathic specialists tried to popularize the use of EDTA for chelation, to no avail. In the 1980s, Richard Casdorph, a practicing cardiologist, claimed improvements in ejection fractions of the heart and in cerebral blood flow with EDTA chelation therapy in several articles. McDonagh, Rudolph, and Cheraskin published about 30 articles documenting various positive effects of EDTA chelation. This group wrote articles showing no problems with kidney function in patients treated with EDTA according to the published protocol. At the same time, conventional cardiologists wrote several editorials against EDTA chelation. So the American Medical Association called for studies to see if chelation worked. The American Board of Chelation Therapy in 1983 was formed to certify doctors who give the therapy. It was later called the American Board of Clinical Metal Toxicology. ACAM also certified doctors who took its workshop on chelation therapy and passed its written and oral examinations. The Great Lakes College of Clinical Medicine, later called the International College of Integrative Medicine (ICIM), was formed in 1983 to teach and do research on chelation and other integrative therapies. After complex negotiations, in the late 1980's Walter Reed Army Hospital agreed to do a randomized clinical trial on EDTA chelation therapy, but part way through the study it was suddenly discontinued for unknown reasons.

    However, in a paper by Seely, Wu, and Mills, (2005), a systematic review of published articles in this field was undertaken. The authors concluded that the best current available evidence did not support the therapeutic use of EDTA chelation therapy in the treatment of cardiovascular disease. Similar results have been reported in review papers by Shrihari, Roy, Prabhakaran, and Reddy (2006) and Crisponi et al. (2015).

    While a 2002 EDTA large randomized clinical trial “showed benefit”, smaller studies were inconsistent.

    In the 1990s, the Federal Trade Commission filed a complaint against ACAM for making a claim in a brochure that chelation was effective for vascular disease. ACAM submitted almost 100 articles in support of the claim, but the FTC insisted that a large randomized trial was required to make that claim. ACAM finally gave up after spending a million dollars in legal fees and signed a consent order saying they would not make such a claim anymore, based on the evidence at that time.

    In conclusion, our study shows that in a population of stable, largely asymptomatic coronary artery disease patients with prior myocardial infarction, use of EDTA chelation therapy did not produce a measurable change in health-related quality of life over 2 years of follow-up.

    A slew of other adverse events such as lacrimation, nasal congestion, mucocutaneous lesions, glycosuria, hypotension, and ECG abnormalities (DISEASE OF THE HEART AND LUNGS) have also been reported as well as allergic reactions (Wax, 2013) to EDTA. Prolonged treatment with calcium EDTA gives rise to depletion of magnesium and trace-metal depletion, the most marked being due to the excretion of zinc. Zinc depletion destroys your cells’ ability to absorb nutrients and leads to diabetes.

    A 2015 study entitled, Quality of Life Outcomes with a Disodium EDTA Chelation Regimen for Coronary Disease: Results from the TACT Randomized Trial concluded with this statement:

    “In conclusion, our study shows that in a population of stable, largely asymptomatic coronary artery disease patients with prior myocardial infarction, use of EDTA chelation therapy did not produce a measurable change in health-related quality of life over 2 years of follow-up.”

    Severe kidney damage from EDTA chelation therapy was reported in a (Nissel 1986) trial. In a very short period of time, EDTA causes kidneys to shut down in complete failure.

    A study from 2015 suggests EDTA chelation for myocardial infarction with “modest” benefits to cardio health. However, I would suggest that the moderate benefits of this study were due to the high doses of vitamin C administered.

    A 2017 study on EDTA chelation for atherosclerosis and Miocardial Infraction concluded:

    “Unsubstantiated claims of chelation therapy as an effective treatment of atherosclerosis should be avoided and patients made aware of the inadequate evidence for efficacy and potential adverse effects, especially the harm that can occur if used as a substitute for proven therapies.”

    In a 2018 EDTA trial it was concluded:

    “These results… are not sufficient to support the routine use of chelation therapy for treatment of patients who have had an MI (Miocardial Infraction)”.

    A study from 2023 entitled, Chelation Therapy Associated with Antioxidant Supplementation Can Decrease Oxidative Stress and Inflammation in Multiple Sclerosis: Preliminary Results proved a flop with two participants discontinuing their trial participation.

    EDTA for lead poisoning DEBUNKED

    EDTA has also been touted as a treatment for lead poisoning. Because of its adverse effects, calcium EDTA was replaced by DMSA in the treatment of lead poisoning (Aposhian et al., 1995) in 1995. CaEDTA has also been used for the treatment of cases with manganese toxicity, but the result was neurotoxic symptoms resembling PARKINSONISM (Andersen, 1999).

    A 2004 trial showed that EDTA actually REDISTRIBUTES LEAD TO THE BRAIN after acute or chronic lead exposure (Andersen, 2004).

    Another trial proved adverse effects in 5 patients receiving EDTA at an outpatient chelation clinic in 2002, and all patients experienced gastrointestinal and musculoskeletal symptoms.

    Oral exposure to EDTA (2002) had produced adverse reproductive and developmental effects in animals. EDTA did not make it past the animal or human trials, so why are medical doctors using it in humans?

    A 2002 EDTA trial was performed on humans as a test for “chelation” therapy by a chelation clinic, demonstrating adverse events in 5 out of 5 patients.

    Additionally, EDTA is a persistent organic pollutant (POP). In that case, each intake would only be partially excreted, while the remaining chemicals build up in the body and produce cell death. And long-term exposure to calcium disodium EDTA creates toxicity and kidney damage.

    EDTA Snakeoil Salesmen

    In March 2023, Ana Maria Mihalcea interviewed Dr. Michael Roth who claims that EDTA is a “synthetic amino acid related to vinegar.” Together they make a slew of medical claims that are not scientifically proven, such as that EDTA “detoxifies covid vaccine, heavy metals, graphene oxide, parasites, hydrogels, and nanoparticles”.

    The only scientific tool Ana Maria uses to back her claims is dark field microscopy. You cannot see nanoparticles with a dark field microscope. It takes a spectroscopy microscope to identify nanoparticles. Her medical claims are simply fabricated and unscientific lies.

    Ana Maria and Dr. Ross made additional unproven medical statements that “EDTA removes the effects of a heart attack, can bring back the elderly from senility and Alzheimer’s, reduces blood pressure, detoxifies several snake and spider venoms, lowers insulin, smooths skin and wrinkles, ” and a host of other laughable health claims that aren’t backed by anything.

    Incidentally, Dr. Ross is now dead.

    “Dr. Roth sadly passed away on March 11/2023”


    My sources informed me that Dr. Rashid Buttar was using EDTA. Given that he was already severely poisoned as Stew Peter’s reported, using EDTA Acid would have been enough to tip him over the edge and kill him.

    EDTA is not an approved pharmaceutical drug. It was Covid Emergency approved by the FDA under an Emergency Use Authorization (EUA), just like the modified RNA (modRNA) Covid-19 vaccine nanotechnology.

    The National Center for Complementary and Integrative Health (.gov) makes it clear that the use of EDTA chelation for heart disease has not been approved by the FDA.

    Ana Maria has been touting EDTA as an “antioxidant” when it is not. She even published to her Substack that EDTA is an “Antioxidant” when in fact it’s an acid poison and an oxidant. Many people saw it on her Substack before she removed it.

    I’ve had over a dozen clients come to me extremely sick from EDTA pills and EDTA IV infusion. Some told me they thought it was a natural substance due to Ana Maria’s false advertising and medical malfeasance. A Medical Doctor is licensed to know wether EDTA Acid is an oxidant poison or an antioxidant. Not knowing this and inducing the death of a patient is not an acceptable excuse. Ana Maria is criminally liable.


    EDTA is an oxidant when used internally. The studies that refer to EDTA as an “antioxidant” are in vitro lab studies, not in vivo (inside the body).

    EDTA is used to preserve cell specimens for chemistry lab work because it prevents blood coagulation and oxidation of cells in a petri dish where it’s used for diagnostic purposes. This is the kind of “antioxidant” the studies are referring to. But when you infuse EDTA Acid into the human body, it acts as an oxidant poison.

    EDTA also will not decoagulate the blood in vivo (inside the body). But I can see how people who cannot read peer-reviewed literature could be deceived and manipulated by snake oil salesmen.

    For example, a study entitled, “Comparative study of the antioxidant capability of EDTA and Irganox”. EDTA is a preservative used in laboratories to preserve cells for scientific lab research. EDTA prevents the oxidation of cells in a petri dish. Oxygen causes cells to deteriorate, but labs need them to last longer for research purposes. When used inside the human body (in vivo), it’s a different story. Then EDTA acts as an oxidant poison, not an antioxidant. So this has a very different meaning.

    One of the well documented and widely known adverse events from EDTA “chelation” is DEATH, according to Mount Sinai.

    Other serious side effects that have been reported include low blood sugar, diminished calcium levels, headache, nausea, dangerously low blood pressure, kidney failure, organ damage, irregular heartbeat, seizures, or even death.

    I have to wonder if Ana Maria Mihalcea is informing her patients that death is a potential adverse event to EDTA chelation? In a March 24, 2024, broadcast that Ana Maria released, at the 53:24 minute mark, she makes a chilling confession:

    “I already have had… uh… patients die from the shedding”

    How many of Ana Maria Mihalcea’s patients have been killed by her EDTA infusion protocol? I was horrified when I heard Ana Maria’s confession because I haven’t had any clients die from shedding! I’ve treated many people who were extremely sick from shedding, and I helped them all to detox effectively. Some clients came to me after several hospitalizations from extreme shedding but none of them died in my care! Nobody needs to die from shedding if they use an effective detox protocol.

    Between 1-2 years, Ana Maria has been claiming that EDTA detoxes graphene, dissolves graphene and chelates heavy metals, but experts such as Dr. Robert Young and Dr. Judy Mikovitz told me this is impossible.

    Ana Maria has gone so far as to produce a medical study with unscientific claims right in the title, “EDTA Chelation Dissolves the Artificial Intelligence Magnetic Hydrogel Weapon”. The study was also promoted by Health Canada. In her study, Ana Maria claims that EDTA can “detoxify the body even from Graphene”.

    EDTA is not a detox agent! Again, it’s an oxidant that degrades cells whereas genuine antioxidants repair cells.

    Ana Maria does in fact know about oxidant poisons. In an interview from December 2022, she referred to graphene as an oxidant. At least she’s correct about something.

    Saul Green, Ph.D., and Wallace I. Sampson, M.D. wrote in great detail about the Implausibility of EDTA Chelation Therapy, stating:

    “EDTA chelation effectiveness is implausible; (2) the preponderance of evidence shows ineffectiveness; and (3) EDTA augments oxidative reactions involving iron instead of inhibiting them, resulting in increased likelihood of production of oxygen free radicals rather than neutralization of them, as claimed.”

    EDTA a precurser to cellular transfection

    The Rockefeller Institue of Medicine has done clinical research on EDTA. One particular study entitled, Studies of Cell Deformity from 1967, shows that cells will degrade from EDTA exposure, which also induces “deformation” on their surfaces. The trial demonstrated that EDTA stops cellular synthesis of calcium. They learned that calcium is bound to anionic sites at the cell periphery, some of which are located at the cellular electrokinetic surface.

    Due to Rockefeller’s research, EDTA is now used in electrophoresis which is a laboratory technique used to separate DNA, RNA or protein molecules based on their size and electrical charge. An electric current is used to move the molecules through a gel or other matrix, according to the National Human Genome Research Institute.

    In agarose gel electrophoresis, EDTA is added for chelating the magnesium ions which are cofactors for DNA nucleases. Hence, activity of DNA nucleases that may be present is inhibited, and “DNA is protected from degrading”. This is why EDTA is an effective transfection agent because it dissolves parts of your DNA, preserving cells for lab research in vitro.

    Gel electrophoresis using EDTA is routinely used for detection and size analysis of proteins and nucleic acid. DMSO is used with EDTA in this process. This destruction of cells makes transfection (gene editing) of cells easier using CRISPR-Cas9 which splices and dices the genome in vivo, as this study explains entitled, “Inhibition of CRISPR-Cas9 ribonucleoprotein complex assembly by anti-CRISPR AcrIIC2”.


    EDTA was found to be genotoxic in laboratory animals. A study from 1983 demonstrates that EDTA induces gene mutations and chromosomal breakage, meaning that genetic mutations will be passed on your offspring, affecting generations to come, according to this Genetic Toxicology of EDTA study from 1983.

    Calcium chelate of EDTA (CaEDTA) “chelation” has shown teratogenic effects (Catsch & Harmuth-Hoene, 1976), which are central nervous system depression and peripheral neuropathy. EDTA produced abnormalities in pups of rats removed by cesarian section on day 21 of the study. Increases in several abnormalities (cleft palate, adactyly or syndactyly, abnormal rib or abnormal vertebrae) were observed with increased doses of CaEDTA.

    EDTA improves transfection of embryonic stem cells lines (hESC) in cells, according to the NIH.

    According to a peer reviewed paper from the NIH, EDTA is a precursor to cellular transfection.

    “We found that chemically abrading the differentiated CACO-2 human intestinal epithelial cell layer by a trypsin and EDTA pretreatment (before the use of detergent-like transfection reagents) dramatically improved transfection efficiency in this polar, differentiated model. Although this treatment did improve the transfection efficiency, it also induced leakiness in the epithelial barrier by both opening tight junctional complexes and by creating holes in the cell layer because of low-level cell death and detachment. Thus, this approach to enhance the transfection efficiency of polar, differentiated cells will be useful for assessment of the effect of the transfected/expressed protein on (re)formation of an epithelial barrier..."

    Thermo Fisher Scientific Inc. Fetal Bovine Serum for human transfection also uses EDTA.


    An NIH study entitled, “Kinetic Basis for DNA Target Specificity of CRISPR-Cas12a” reveals that EDTA enables rapid binding to DNA during gene editing (transfection).

    Another study entitled, “Improved genome editing by an engineered CRISPR-Cas12a” explains:

    “CAS12a is an RNA-guided, programmable genome editing enzyme found within bacterial adaptive immune pathways. Unlike CRISPR-Cas9, Cas12a uses only a single catalytic site to both cleave target double-stranded DNA (dsDNA) (cis-activity) and indiscriminately degrade single-stranded DNA (ssDNA) (trans-activity).”

    According to the study, “A DNA loading buffer of 45% formamide and 15 mM EDTA, with a trace amount of xylene cyanol and bromophenol blue…” is used to transfect the human genome.

    So, EDTA is a transfection agent used with CRISPR-Cas9 to edit the human genome. Does EDTA actually dissolve graphene, as Ana Maria claims? The answer is NO! EDTA oxidant is used to reduce graphene to Reduced Graphene Oxide (RGO) form. Graphene is reduced by oxidation. Rather than dissolving graphene, EDTA reduces it to Graphene Oxide Nanoparticles otherwise known as Quantum Dots.

    Graphene oxide is more toxic than graphene, as I documented in my article entitled, “Graphene Oxide The Vector For Covid-19 Democide”.

    I will emphasize again that Graphene Oxide Quantum Dots cannot be seen with a dark field microscope. So Ana Maria’s claims that EDTA is detoxing graphene from the human body is unscientific.

    EDTA chelation for graphene nanocomposites

    EDTA chelation is NOT effective in removing metals from the human body. It's actually a different kind of chelation that’s used to create electrochemical sensors (biosensors) when combined with GRAPHENE!

    EDTA serves as a connecting mediator between NiHCF (Graphene Oxide Nanoparticles and Nickle) and graphene nanosheets. EDTA is used with metal nanoparticles, metal oxides, graphene, carbon nanotubes, and quantum dots to stabilize the technology for a more uniform distribution throughout the body.

    A Science Direct paper entitled, “Highly sensitive ascorbid acid sensors from EDTA chelation derived nickel hexacyanoferrate/graphene nanocomposites” reveals that EDTA is used to create Graphene/Nickel, AA sensor nanocomposites.

    “EDTA chelation stragey” is used for the “homogeneously distrubuted" NiHCF” (Nickel hexacyanoferrate composite) on graphene sheets. EDTA residue-supported pyramidal and spherical nanoparticles of NiHCF deposited on graphene sheets is used to create biosensors for the formation of Graphene/Nickel hydrogels.


    The graphene hydrogel nanocomposite sensors (Gr/NiHCF) are used as externally controlled biosensing tools. They tell us it’s used to test for ascorbic acid, but the application of this technology is for “human life” as well as for industrial use. See link here.


    Graphene oxide/Lauric acid nanoparticles are modified using EDTA. Lauric acid nanoparticles is suggested as a “prospective drug carrier” for oral nanoparticle-mediated sustained drug delivery (timed release technology) used for the removal of Pb(II) ions (lead). However, studies show there are cytotoxic results.

    Another study entitled, “Improved genome editing by an engineered CRISPR-Cas12a” demonstrates how EDTA improves transfection and modification of the human genome.

    Once Graphene is reduced to Graphene Oxide, due to its small particulate size, you can no longer identify it using a Dark Field Microscope. Ana Maria is using a dark field scope, not a spectroscopy microscope, which is the only instrument that can measure GON and Quantum Dots.

    So what is Ana Maria doing with EDTA infusions? She’s creating a metal-EDTA complex that stabilizes and strengthens the graphene-based nanotech weapon system and enables it to spread more readily throughout the body, for human transfection. She uses “light and sound healing techniques” to activate the delayed release technology before administering EDTA infusion, as she reveals in an interview here.

    EDTA is a poison acid that dissolves DNA. It's used to prime the cells’ DNA for transfection. EDTA disrupts the surface of skin cells so that other chemicals can penetrate more easily and CRISPR-Cas9 gene editing technology can work more efficiently.

    The NIH describes EDTA’s enhanced cellular transfection:

    “Flow cytometric analysis using an enhanced green fluorescent protein vector showed a significantly increased transfection efficiency of EDTA method compared to standard enzyme method. In addition, the EDTA approach maintained stable cell viability and recovery rate of hESCs after transfection.”

    Another study published in Research Gate, confirms that EDTA increases cellular transfection, along with using chloroquine.

    Graphene Oxide Quantum Dots (GOQD-HA) nanocomposite use EDTA for tissue-specific delivery of Metformin, an anti-diabetic drug otherwise known as insulin.


    Conclusion

    Beware of snakeoil salesmen! Never trust pharmaceuticals! Superior heavy metal chelation supplements exist such as ASEA redox molecules and Master Peace, sign up and order here. Medicines made from nature are always superior to pharmaceutical drugs. Finally, be sure your Naturopathic Doctor is competent!

    Schedule a health consultation with me for a customized detox protocol and complete cellular health restoration.

    https://substack.com/home/post/p-144979143
    EDTA Snakeoil! Ana Maria Mihalcea's Medical Malfeasance Exposed “I already have had.. uh.. patients die from shedding” - Ana Maria Mihalcea, M.D. Dr. Ariyana Love (ND) “My people are destroyed for lack of knowledge: because thou hast rejected knowledge, I will also reject thee, that thou shalt be no priest to me: seeing thou hast forgotten the law of thy God, I will also forget thy children.” ~ Hosea 4:6 KJV Rockefeller Medicine Around 1900, the science world was getting excited about new “petrochemicals” and the ability to create a variety of new compounds from oil. Some of the first products derived from petrochemicals were plastics. In 1908, modern medicine was established by the Rockefeller’s and dubbed “Allopathy”. The Rockefeller’s created the business of modern medicine which has always been about poisoning people, Eustice Mullen explains. This is the definition of Allopathic medicine according to the NIH: “A system in which medical doctors and other health care professionals (such as nurses, pharmacists, and therapists) treat symptoms and diseases using drugs, radiation, or surgery.” The Rockefeller Institute for Medicine, founded in 1908, marked the advent of the re-creation of synthetic versions of natural cures. Prior to 1908, every place of healing in America, Europe and the world, used only ancient traditional natural medicinal cures. Every hospital was a “Homeopathic Hospital”. Most of these magnificent buildings were converted into mental health asylums where a system of torture and electric shock was established to “cure” mental illness. John D. Rockefeller created the oil industry and used it to crush traditional medicine in order to enslave people. They also financed the Eugenics movement. One of the perks of modern medicine is depopulation. “Everyone knows that the infamous Roe v. Wade opinion legalized abortion, but almost no one knows that legal abortion was a strategy by eugenicists, as early as 1939, to “genetically improve” the population by “reducing” it.” In the book, “Rockefeller Medicine Men: Medicine and Capitalism in America”, authored by E. Richard Brown, he tells the hidden story of the financial, political, and institutional manipulations whereby a diverse and eclectic range of traditional healing modalities available to the North American public was summarily canceled and pared down to a singular style of medicine that would become the predominant medicine of the Western world and a major force in global medical culture during the 20th century. This was brought about largely by the collaboration of the American Medical Association, the philanthropies of Andrew Carnegie and John D. Rockefeller, and the development of a revolutionary curriculum by the Johns Hopkins School of Medicine. Brown documents the story of how a powerful professional elite gained virtual hegemony in the Western theatre of healing by effectively taking control of the ethos and practice of Western medicine. E. Richard Brown describes how, in 1905, the American Medical Association’s new Council on Medical Education funded by Carnegie and Rockefeller commenced serious activity. They employed the services of Abraham Flexner who proceeded to visit and “assess” every single medical school in the US and Canada. Within a short time of this development, medical schools all around the US began to collapse or consolidate. By 1910, 30 schools had merged, and 21 had closed their doors. Of the 166 medical schools operating in 1904, 133 had survived by 1910, and 104 by 1915. Fifteen years later, only 76 schools of medicine existed in the US and they all followed the same curriculum. The 1910 Flexner Report laid the foundations of the modern medical system, dubbed “Rockefeller medicine” (Allopathy). Since 1910, corporate interests have established near total control of the medical field, both though pharmacology and through their impact on medical education. In 1935, vitamin C became the first vitamin to be artificially synthesized in Switzerland. Rockefeller saw a big opportunity with the possibility that vitamins and medications could be developed from petroleum. He saw the chance to control and monopolize multiple industries at once: petroleum, chemical and medical. Petrochemicals were ideal from a business perspective because they could be patented, owned and sold for high profits. Today, the petrochemicals in plastics are causing a slew of illnesses including neurodevelopmental disorders, diabetes, chronic respiratory disease, and cancer, which have increased between 28% and 150% between 1990 and 2019. Petrochemicals in microplastics are also rapidly reducing fertility in males in particular, and polluting our environment. Please also read more here, here, and here. The first pharmaceutical drug was an arsenic named Salvarsan. That’s right, an ARSENIC! DEATH is an all-to-common side effect of pharmaceutical drugs which is only logical when you administer poisons internally. The following pages demonstrate the many deaths of people around the world, most of them children, who were fatally poisoned during the first mass medication experiments with Rockefeller’s Allopathic health. The paper is entitled, Toward Responsibility in International Health: Death following Treatment in Rockefeller Hookworm Campaigns, 1914–1934. What is EDTA? EDTA is synthesized on an industrial scale using 1, 2-diaminoethane (ethylene diamine), formaldehyde, water and sodium cyanide. Ethylene diamine induced acute and subchronic toxicity in lab animals, also allergic hypersensitivity. The liver and kidneys are target organs of ethylenediamine, where they simply stop working. Read more: Is C60 And EDTA Safe? Clinical Review Absorption of large amounts of formaldehyde via any route can cause severe systemic toxicity, leading to metabolic acidosis, tissue and organ damage, and coma, according to the CDC. Exposure to sodium cyanide can be rapidly fatal. It has whole-body (systemic) effects, particularly affecting those organ systems most sensitive to low oxygen levels: the central nervous system (brain), the cardiovascular system (heart and blood vessels), and the pulmonary system (lungs), according to the CDC. EDTA is an industrial poison. The textile industry required a chelating agent to remove calcium during textile processing and this led to the synthesis of polyamino-carboxylic acids, one of which was EDTA. A patent was filed for EDTA in Germany in 1935, for industrial chemical use. EDTA is a synthetic acid effectively used to clean boiler rooms in nuclear power plants. In 1945, Franz Munz obtained a US EDTA patent in 1945. In 1947, EDTA was approved by the US Food and Drug Administration (FDA) as a food additive in “low doses” because it’s a forever chemical and a preservative. There are two different types of EDTA approved by the U.S. FDA. In 1953, Edetate calcium disodium also known as Calcium EDTA (marketed under the trade name Calcium Disodium Versenate registered ) was approved for the treatment of lead poisoning. Three years later, in 1956, a related EDTA compound, Edetate disodium, was also approved for clinical use. This compound, also known as Disodium EDTA, has been marketed under the trade names Disotate (registered) and Endrate (registered). The essential difference between these two compounds is that Calcium EDTA's structure has an incorporated Ca super(2+) moiety while Disodium EDTA does not. The use of the latter compound, Disodium EDTA, has been associated with life-threatening and fatal hypocalcemia. EDTA trial DEATHS An EDTA trial (Sloth-Nielsen et al., 1981) on the possible antiatherogenic effect of EDTA with 6 patients, showed clinical signs of potentially lethal hypocalcemia from abnormally low calcium levels caused by EDTA. Another EDTA chelation human trial in 2003-2005 resulted in DEATHS due to hypocalcemia. A 2006 EDTA chelation trial also resulted in DEATHS due to hypocalcemia. There were several DEATHS reported from cardiac arrest due to lethal hypocalcemia in EDTA trials in 2006 and 2008 and (Brown, Willis, Omalu, & Leiker, 2006; Baxter & Krenzelok, 2008), from calcium deficiency inducing alterations in the brain, and osteoporosis, which causes the bones to become brittle. In 2008, a clinical trial with EDTA chelation on autistic children also proved fatal, resulting in DEATHS of children. A 2007 EDTA chelation study proved KIDNEY FAILURE in humans. Decades of clinical studies demonstrate that EDTA treatment is associated with severe, life-threatening adverse effects, as Science Direct explained in 2016. “It should be emphasized that EDTA treatment is associated with severe, life-threatening adverse effects. EDTA for cardiovascular disease DEBUNKED Many Allopathic specialists tried to popularize the use of EDTA for chelation, to no avail. In the 1980s, Richard Casdorph, a practicing cardiologist, claimed improvements in ejection fractions of the heart and in cerebral blood flow with EDTA chelation therapy in several articles. McDonagh, Rudolph, and Cheraskin published about 30 articles documenting various positive effects of EDTA chelation. This group wrote articles showing no problems with kidney function in patients treated with EDTA according to the published protocol. At the same time, conventional cardiologists wrote several editorials against EDTA chelation. So the American Medical Association called for studies to see if chelation worked. The American Board of Chelation Therapy in 1983 was formed to certify doctors who give the therapy. It was later called the American Board of Clinical Metal Toxicology. ACAM also certified doctors who took its workshop on chelation therapy and passed its written and oral examinations. The Great Lakes College of Clinical Medicine, later called the International College of Integrative Medicine (ICIM), was formed in 1983 to teach and do research on chelation and other integrative therapies. After complex negotiations, in the late 1980's Walter Reed Army Hospital agreed to do a randomized clinical trial on EDTA chelation therapy, but part way through the study it was suddenly discontinued for unknown reasons. However, in a paper by Seely, Wu, and Mills, (2005), a systematic review of published articles in this field was undertaken. The authors concluded that the best current available evidence did not support the therapeutic use of EDTA chelation therapy in the treatment of cardiovascular disease. Similar results have been reported in review papers by Shrihari, Roy, Prabhakaran, and Reddy (2006) and Crisponi et al. (2015). While a 2002 EDTA large randomized clinical trial “showed benefit”, smaller studies were inconsistent. In the 1990s, the Federal Trade Commission filed a complaint against ACAM for making a claim in a brochure that chelation was effective for vascular disease. ACAM submitted almost 100 articles in support of the claim, but the FTC insisted that a large randomized trial was required to make that claim. ACAM finally gave up after spending a million dollars in legal fees and signed a consent order saying they would not make such a claim anymore, based on the evidence at that time. In conclusion, our study shows that in a population of stable, largely asymptomatic coronary artery disease patients with prior myocardial infarction, use of EDTA chelation therapy did not produce a measurable change in health-related quality of life over 2 years of follow-up. A slew of other adverse events such as lacrimation, nasal congestion, mucocutaneous lesions, glycosuria, hypotension, and ECG abnormalities (DISEASE OF THE HEART AND LUNGS) have also been reported as well as allergic reactions (Wax, 2013) to EDTA. Prolonged treatment with calcium EDTA gives rise to depletion of magnesium and trace-metal depletion, the most marked being due to the excretion of zinc. Zinc depletion destroys your cells’ ability to absorb nutrients and leads to diabetes. A 2015 study entitled, Quality of Life Outcomes with a Disodium EDTA Chelation Regimen for Coronary Disease: Results from the TACT Randomized Trial concluded with this statement: “In conclusion, our study shows that in a population of stable, largely asymptomatic coronary artery disease patients with prior myocardial infarction, use of EDTA chelation therapy did not produce a measurable change in health-related quality of life over 2 years of follow-up.” Severe kidney damage from EDTA chelation therapy was reported in a (Nissel 1986) trial. In a very short period of time, EDTA causes kidneys to shut down in complete failure. A study from 2015 suggests EDTA chelation for myocardial infarction with “modest” benefits to cardio health. However, I would suggest that the moderate benefits of this study were due to the high doses of vitamin C administered. A 2017 study on EDTA chelation for atherosclerosis and Miocardial Infraction concluded: “Unsubstantiated claims of chelation therapy as an effective treatment of atherosclerosis should be avoided and patients made aware of the inadequate evidence for efficacy and potential adverse effects, especially the harm that can occur if used as a substitute for proven therapies.” In a 2018 EDTA trial it was concluded: “These results… are not sufficient to support the routine use of chelation therapy for treatment of patients who have had an MI (Miocardial Infraction)”. A study from 2023 entitled, Chelation Therapy Associated with Antioxidant Supplementation Can Decrease Oxidative Stress and Inflammation in Multiple Sclerosis: Preliminary Results proved a flop with two participants discontinuing their trial participation. EDTA for lead poisoning DEBUNKED EDTA has also been touted as a treatment for lead poisoning. Because of its adverse effects, calcium EDTA was replaced by DMSA in the treatment of lead poisoning (Aposhian et al., 1995) in 1995. CaEDTA has also been used for the treatment of cases with manganese toxicity, but the result was neurotoxic symptoms resembling PARKINSONISM (Andersen, 1999). A 2004 trial showed that EDTA actually REDISTRIBUTES LEAD TO THE BRAIN after acute or chronic lead exposure (Andersen, 2004). Another trial proved adverse effects in 5 patients receiving EDTA at an outpatient chelation clinic in 2002, and all patients experienced gastrointestinal and musculoskeletal symptoms. Oral exposure to EDTA (2002) had produced adverse reproductive and developmental effects in animals. EDTA did not make it past the animal or human trials, so why are medical doctors using it in humans? A 2002 EDTA trial was performed on humans as a test for “chelation” therapy by a chelation clinic, demonstrating adverse events in 5 out of 5 patients. Additionally, EDTA is a persistent organic pollutant (POP). In that case, each intake would only be partially excreted, while the remaining chemicals build up in the body and produce cell death. And long-term exposure to calcium disodium EDTA creates toxicity and kidney damage. EDTA Snakeoil Salesmen In March 2023, Ana Maria Mihalcea interviewed Dr. Michael Roth who claims that EDTA is a “synthetic amino acid related to vinegar.” Together they make a slew of medical claims that are not scientifically proven, such as that EDTA “detoxifies covid vaccine, heavy metals, graphene oxide, parasites, hydrogels, and nanoparticles”. The only scientific tool Ana Maria uses to back her claims is dark field microscopy. You cannot see nanoparticles with a dark field microscope. It takes a spectroscopy microscope to identify nanoparticles. Her medical claims are simply fabricated and unscientific lies. Ana Maria and Dr. Ross made additional unproven medical statements that “EDTA removes the effects of a heart attack, can bring back the elderly from senility and Alzheimer’s, reduces blood pressure, detoxifies several snake and spider venoms, lowers insulin, smooths skin and wrinkles, ” and a host of other laughable health claims that aren’t backed by anything. Incidentally, Dr. Ross is now dead. “Dr. Roth sadly passed away on March 11/2023” My sources informed me that Dr. Rashid Buttar was using EDTA. Given that he was already severely poisoned as Stew Peter’s reported, using EDTA Acid would have been enough to tip him over the edge and kill him. EDTA is not an approved pharmaceutical drug. It was Covid Emergency approved by the FDA under an Emergency Use Authorization (EUA), just like the modified RNA (modRNA) Covid-19 vaccine nanotechnology. The National Center for Complementary and Integrative Health (.gov) makes it clear that the use of EDTA chelation for heart disease has not been approved by the FDA. Ana Maria has been touting EDTA as an “antioxidant” when it is not. She even published to her Substack that EDTA is an “Antioxidant” when in fact it’s an acid poison and an oxidant. Many people saw it on her Substack before she removed it. I’ve had over a dozen clients come to me extremely sick from EDTA pills and EDTA IV infusion. Some told me they thought it was a natural substance due to Ana Maria’s false advertising and medical malfeasance. A Medical Doctor is licensed to know wether EDTA Acid is an oxidant poison or an antioxidant. Not knowing this and inducing the death of a patient is not an acceptable excuse. Ana Maria is criminally liable. EDTA is an oxidant when used internally. The studies that refer to EDTA as an “antioxidant” are in vitro lab studies, not in vivo (inside the body). EDTA is used to preserve cell specimens for chemistry lab work because it prevents blood coagulation and oxidation of cells in a petri dish where it’s used for diagnostic purposes. This is the kind of “antioxidant” the studies are referring to. But when you infuse EDTA Acid into the human body, it acts as an oxidant poison. EDTA also will not decoagulate the blood in vivo (inside the body). But I can see how people who cannot read peer-reviewed literature could be deceived and manipulated by snake oil salesmen. For example, a study entitled, “Comparative study of the antioxidant capability of EDTA and Irganox”. EDTA is a preservative used in laboratories to preserve cells for scientific lab research. EDTA prevents the oxidation of cells in a petri dish. Oxygen causes cells to deteriorate, but labs need them to last longer for research purposes. When used inside the human body (in vivo), it’s a different story. Then EDTA acts as an oxidant poison, not an antioxidant. So this has a very different meaning. One of the well documented and widely known adverse events from EDTA “chelation” is DEATH, according to Mount Sinai. Other serious side effects that have been reported include low blood sugar, diminished calcium levels, headache, nausea, dangerously low blood pressure, kidney failure, organ damage, irregular heartbeat, seizures, or even death. I have to wonder if Ana Maria Mihalcea is informing her patients that death is a potential adverse event to EDTA chelation? In a March 24, 2024, broadcast that Ana Maria released, at the 53:24 minute mark, she makes a chilling confession: “I already have had… uh… patients die from the shedding” How many of Ana Maria Mihalcea’s patients have been killed by her EDTA infusion protocol? I was horrified when I heard Ana Maria’s confession because I haven’t had any clients die from shedding! I’ve treated many people who were extremely sick from shedding, and I helped them all to detox effectively. Some clients came to me after several hospitalizations from extreme shedding but none of them died in my care! Nobody needs to die from shedding if they use an effective detox protocol. Between 1-2 years, Ana Maria has been claiming that EDTA detoxes graphene, dissolves graphene and chelates heavy metals, but experts such as Dr. Robert Young and Dr. Judy Mikovitz told me this is impossible. Ana Maria has gone so far as to produce a medical study with unscientific claims right in the title, “EDTA Chelation Dissolves the Artificial Intelligence Magnetic Hydrogel Weapon”. The study was also promoted by Health Canada. In her study, Ana Maria claims that EDTA can “detoxify the body even from Graphene”. EDTA is not a detox agent! Again, it’s an oxidant that degrades cells whereas genuine antioxidants repair cells. Ana Maria does in fact know about oxidant poisons. In an interview from December 2022, she referred to graphene as an oxidant. At least she’s correct about something. Saul Green, Ph.D., and Wallace I. Sampson, M.D. wrote in great detail about the Implausibility of EDTA Chelation Therapy, stating: “EDTA chelation effectiveness is implausible; (2) the preponderance of evidence shows ineffectiveness; and (3) EDTA augments oxidative reactions involving iron instead of inhibiting them, resulting in increased likelihood of production of oxygen free radicals rather than neutralization of them, as claimed.” EDTA a precurser to cellular transfection The Rockefeller Institue of Medicine has done clinical research on EDTA. One particular study entitled, Studies of Cell Deformity from 1967, shows that cells will degrade from EDTA exposure, which also induces “deformation” on their surfaces. The trial demonstrated that EDTA stops cellular synthesis of calcium. They learned that calcium is bound to anionic sites at the cell periphery, some of which are located at the cellular electrokinetic surface. Due to Rockefeller’s research, EDTA is now used in electrophoresis which is a laboratory technique used to separate DNA, RNA or protein molecules based on their size and electrical charge. An electric current is used to move the molecules through a gel or other matrix, according to the National Human Genome Research Institute. In agarose gel electrophoresis, EDTA is added for chelating the magnesium ions which are cofactors for DNA nucleases. Hence, activity of DNA nucleases that may be present is inhibited, and “DNA is protected from degrading”. This is why EDTA is an effective transfection agent because it dissolves parts of your DNA, preserving cells for lab research in vitro. Gel electrophoresis using EDTA is routinely used for detection and size analysis of proteins and nucleic acid. DMSO is used with EDTA in this process. This destruction of cells makes transfection (gene editing) of cells easier using CRISPR-Cas9 which splices and dices the genome in vivo, as this study explains entitled, “Inhibition of CRISPR-Cas9 ribonucleoprotein complex assembly by anti-CRISPR AcrIIC2”. EDTA was found to be genotoxic in laboratory animals. A study from 1983 demonstrates that EDTA induces gene mutations and chromosomal breakage, meaning that genetic mutations will be passed on your offspring, affecting generations to come, according to this Genetic Toxicology of EDTA study from 1983. Calcium chelate of EDTA (CaEDTA) “chelation” has shown teratogenic effects (Catsch & Harmuth-Hoene, 1976), which are central nervous system depression and peripheral neuropathy. EDTA produced abnormalities in pups of rats removed by cesarian section on day 21 of the study. Increases in several abnormalities (cleft palate, adactyly or syndactyly, abnormal rib or abnormal vertebrae) were observed with increased doses of CaEDTA. EDTA improves transfection of embryonic stem cells lines (hESC) in cells, according to the NIH. According to a peer reviewed paper from the NIH, EDTA is a precursor to cellular transfection. “We found that chemically abrading the differentiated CACO-2 human intestinal epithelial cell layer by a trypsin and EDTA pretreatment (before the use of detergent-like transfection reagents) dramatically improved transfection efficiency in this polar, differentiated model. Although this treatment did improve the transfection efficiency, it also induced leakiness in the epithelial barrier by both opening tight junctional complexes and by creating holes in the cell layer because of low-level cell death and detachment. Thus, this approach to enhance the transfection efficiency of polar, differentiated cells will be useful for assessment of the effect of the transfected/expressed protein on (re)formation of an epithelial barrier..." Thermo Fisher Scientific Inc. Fetal Bovine Serum for human transfection also uses EDTA. An NIH study entitled, “Kinetic Basis for DNA Target Specificity of CRISPR-Cas12a” reveals that EDTA enables rapid binding to DNA during gene editing (transfection). Another study entitled, “Improved genome editing by an engineered CRISPR-Cas12a” explains: “CAS12a is an RNA-guided, programmable genome editing enzyme found within bacterial adaptive immune pathways. Unlike CRISPR-Cas9, Cas12a uses only a single catalytic site to both cleave target double-stranded DNA (dsDNA) (cis-activity) and indiscriminately degrade single-stranded DNA (ssDNA) (trans-activity).” According to the study, “A DNA loading buffer of 45% formamide and 15 mM EDTA, with a trace amount of xylene cyanol and bromophenol blue…” is used to transfect the human genome. So, EDTA is a transfection agent used with CRISPR-Cas9 to edit the human genome. Does EDTA actually dissolve graphene, as Ana Maria claims? The answer is NO! EDTA oxidant is used to reduce graphene to Reduced Graphene Oxide (RGO) form. Graphene is reduced by oxidation. Rather than dissolving graphene, EDTA reduces it to Graphene Oxide Nanoparticles otherwise known as Quantum Dots. Graphene oxide is more toxic than graphene, as I documented in my article entitled, “Graphene Oxide The Vector For Covid-19 Democide”. I will emphasize again that Graphene Oxide Quantum Dots cannot be seen with a dark field microscope. So Ana Maria’s claims that EDTA is detoxing graphene from the human body is unscientific. EDTA chelation for graphene nanocomposites EDTA chelation is NOT effective in removing metals from the human body. It's actually a different kind of chelation that’s used to create electrochemical sensors (biosensors) when combined with GRAPHENE! EDTA serves as a connecting mediator between NiHCF (Graphene Oxide Nanoparticles and Nickle) and graphene nanosheets. EDTA is used with metal nanoparticles, metal oxides, graphene, carbon nanotubes, and quantum dots to stabilize the technology for a more uniform distribution throughout the body. A Science Direct paper entitled, “Highly sensitive ascorbid acid sensors from EDTA chelation derived nickel hexacyanoferrate/graphene nanocomposites” reveals that EDTA is used to create Graphene/Nickel, AA sensor nanocomposites. “EDTA chelation stragey” is used for the “homogeneously distrubuted" NiHCF” (Nickel hexacyanoferrate composite) on graphene sheets. EDTA residue-supported pyramidal and spherical nanoparticles of NiHCF deposited on graphene sheets is used to create biosensors for the formation of Graphene/Nickel hydrogels. The graphene hydrogel nanocomposite sensors (Gr/NiHCF) are used as externally controlled biosensing tools. They tell us it’s used to test for ascorbic acid, but the application of this technology is for “human life” as well as for industrial use. See link here. Graphene oxide/Lauric acid nanoparticles are modified using EDTA. Lauric acid nanoparticles is suggested as a “prospective drug carrier” for oral nanoparticle-mediated sustained drug delivery (timed release technology) used for the removal of Pb(II) ions (lead). However, studies show there are cytotoxic results. Another study entitled, “Improved genome editing by an engineered CRISPR-Cas12a” demonstrates how EDTA improves transfection and modification of the human genome. Once Graphene is reduced to Graphene Oxide, due to its small particulate size, you can no longer identify it using a Dark Field Microscope. Ana Maria is using a dark field scope, not a spectroscopy microscope, which is the only instrument that can measure GON and Quantum Dots. So what is Ana Maria doing with EDTA infusions? She’s creating a metal-EDTA complex that stabilizes and strengthens the graphene-based nanotech weapon system and enables it to spread more readily throughout the body, for human transfection. She uses “light and sound healing techniques” to activate the delayed release technology before administering EDTA infusion, as she reveals in an interview here. EDTA is a poison acid that dissolves DNA. It's used to prime the cells’ DNA for transfection. EDTA disrupts the surface of skin cells so that other chemicals can penetrate more easily and CRISPR-Cas9 gene editing technology can work more efficiently. The NIH describes EDTA’s enhanced cellular transfection: “Flow cytometric analysis using an enhanced green fluorescent protein vector showed a significantly increased transfection efficiency of EDTA method compared to standard enzyme method. In addition, the EDTA approach maintained stable cell viability and recovery rate of hESCs after transfection.” Another study published in Research Gate, confirms that EDTA increases cellular transfection, along with using chloroquine. Graphene Oxide Quantum Dots (GOQD-HA) nanocomposite use EDTA for tissue-specific delivery of Metformin, an anti-diabetic drug otherwise known as insulin. Conclusion Beware of snakeoil salesmen! Never trust pharmaceuticals! Superior heavy metal chelation supplements exist such as ASEA redox molecules and Master Peace, sign up and order here. Medicines made from nature are always superior to pharmaceutical drugs. Finally, be sure your Naturopathic Doctor is competent! Schedule a health consultation with me for a customized detox protocol and complete cellular health restoration. https://substack.com/home/post/p-144979143
    SUBSTACK.COM
    EDTA Snakeoil! Ana Maria Mihalcea's Medical Malfeasance Exposed
    “I already have had.. uh.. patients die from shedding” - Ana Maria Mihalcea, M.D.
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  • Massimo Luciani - Structures found in the Great Red Spot area on Jupiter:

    https://english.tachyonbeam.com/2024/06/26/structures-found-in-the-great-red-spot-area-on-jupiter/

    #GreatRedSpot #Jupiter #JamesWebb #SpaceTelescope #JWST #Infrared #Spectroscopy #NIRSpec #SolarSystemScience #PlanetaryScience #AtmosphericPhysics #Physics #Astronomy
    Massimo Luciani - Structures found in the Great Red Spot area on Jupiter: https://english.tachyonbeam.com/2024/06/26/structures-found-in-the-great-red-spot-area-on-jupiter/ #GreatRedSpot #Jupiter #JamesWebb #SpaceTelescope #JWST #Infrared #Spectroscopy #NIRSpec #SolarSystemScience #PlanetaryScience #AtmosphericPhysics #Physics #Astronomy
    ENGLISH.TACHYONBEAM.COM
    Structures found in the Great Red Spot area on Jupiter
    An article published in the journal 'Nature Astronomy' reports the identification of structures in the planet Jupiter's upper atmosphere above the Great Red...
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  • Clare Sansom - Probing neptunium's atomic structure with laser spectroscopy:

    https://phys.org/news/2024-05-probing-neptunium-atomic-laser-spectroscopy.html

    #Neptunium237 #Neptunium #Isotope #ActinideMetal #LaserSpectroscopy #Spectroscopy #IonizationPotential #Ionization #RadioactiveWaste #AtomicPhysics #Physics
    Clare Sansom - Probing neptunium's atomic structure with laser spectroscopy: https://phys.org/news/2024-05-probing-neptunium-atomic-laser-spectroscopy.html #Neptunium237 #Neptunium #Isotope #ActinideMetal #LaserSpectroscopy #Spectroscopy #IonizationPotential #Ionization #RadioactiveWaste #AtomicPhysics #Physics
    PHYS.ORG
    Probing neptunium's atomic structure with laser spectroscopy
    A new technique developed by researchers in Germany can measure ionization states of this element more precisely than before, with implications for its detection and remediation in radioactive waste.
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  • Simon Kelly & Emma Midgley - Combating Olive Oil Fraud with Nuclear Innovations:

    https://www.iaea.org/newscenter/news/combating-olive-oil-fraud-with-nuclear-innovations

    #OliveOil #Authenticity #NearInfrared #Infrared #Spectroscopy #FourierTransform #GasChromatography #Chromatography #Atoms4Food #IAEA #Agriculture #Physics
    Simon Kelly & Emma Midgley - Combating Olive Oil Fraud with Nuclear Innovations: https://www.iaea.org/newscenter/news/combating-olive-oil-fraud-with-nuclear-innovations #OliveOil #Authenticity #NearInfrared #Infrared #Spectroscopy #FourierTransform #GasChromatography #Chromatography #Atoms4Food #IAEA #Agriculture #Physics
    WWW.IAEA.ORG
    Combating Olive Oil Fraud with Nuclear Innovations
    The International Atomic Energy Agency (IAEA) is developing new and rapid methods to rapidly screen and authenticate the origin of foods like extra virgin olive oil.
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  • Hydrogels in COVID Vaccine as Programmable Human Interface

    From Ana Maria Mihalcea’s "Hydrogel Platform Enables Versatile Data Encryption And Decryption"

    Greg ReeseFeb 16
    The following report is from Doctor Ana Maria Mihalcea’s recent article entitled, "Hydrogel Platform Enables Versatile Data Encryption And Decryption"

    The building blocks of Hydrogels are being found in the COVID vaccine, and Hydrogels are being found in the blood of both the vaccinated and the unvaccinated. They are the so-called blood clots that are being found around the world. And these Hydrogels can now be programmed, encrypted and decrypted. According to Mihalcea, they are the substrate of the brain computer interface and the primary method of fusing humans with machines as she described by referencing MIT research in the article, “Hydrogel Interfaces for Merging Humans and Machines”

    Elements which Mihalcea and Clifford Carnicom found with Near Infrared spectroscopy in the blood of the unvaccinated exposed to shedding and environmental contamination include hydrogel plastics such as polyenes, vinyl, nylon, kevlar, and spider silk proteins. As well as other nanotechnology signatures such as silicone and sulfur. This technology hijacks methyl groups, which are needed to detoxify and create Glutathione in the body. Hydrogels used for the encrypted programmable technology include polyvinyl alcohol and polycaprolacton. Both of these Hydrogels are listed as stealth nanoparticles in the Moderna patent for lipid nanoparticle composition. This suggests that not only those who received the shot have this hydrogel encryption technology in their bodies, but also those who have experienced shedding and environmental contamination. Which is just about everyone.

    These hydrogels are known to be programmable and encrypted. This technology can behave as brain storage. It can store memories and visual information in an individual’s brain. And it can be chemical-induced to be securely encrypted and decrypted allowing for the secure recording and storage of confidential visual information. This provides a platform for secure financial transactions, which is a requirement for a digital ID.

    MIT researchers have discussed how this very same technology can be used to fuse humans with machines. And while they’ve had problems working it out in the past, a recent paper has announced they’ve found success using the very same elements found in both the blood of the vaccinated and unvaccinated by Mihalcea and Carnicom.

    In a lecture by Professor Sakhrat Khizroev at the University of Miami, it is discussed how advanced materials can be used for interfacing machines and the human brain. He references a research project funded by DARPA wherein magnetic nanoparticles are key to this technology. Mihalcea has published research that shows how the COVID shots alter torsion fields in the body and produce magnetism. A review by the Rand Corporation, “Brain Computer Interfaces: US Military Applications and Implications” discusses the convergence of human with machine.

    In an interview with Big Pharma whistleblower, Karen Kingston, Kingston discusses this self assembly nanotechnology and how the spike protein is an engineered device, triggered by electromagnetic frequency, and how the Quantum Dots are gene editing technology. This nanotechnology appears to be distributed via Chemtrails, the food and water supply, medications, and in all of the scheduled vaccines for children. It has been found by multiple scientists in the blood of both the vaccinated and the unvaccinated. And the fact that this widespread technology is being ignored while the topic of mRNA is being pushed into the mainstream, is of great concern.

    Mihalcea has shown that the new protocols being sold to the public as a way of reversing the negative effects of the COVID shots, have no effect on these Hydrogels. And it would seem that well over a billion people are infected with them.

    While many are talking about an archaic implanted computer chip, it seems that the latest breakthrough technology has already been deployed without anyone’s consent.

    The situation almost seems hopeless, but where there is a will there is a way. And now is not the time to hide our head in the sand. The human body is miraculous and our potential is endless. The more people addressing this dire situation, the better chances we have of finding a remedy.

    https://rumble.com/v4dqd6t-hydrogels-in-covid-vaccine-as-programmable-human-interface.html
    Hydrogels in COVID Vaccine as Programmable Human Interface From Ana Maria Mihalcea’s "Hydrogel Platform Enables Versatile Data Encryption And Decryption" Greg ReeseFeb 16 The following report is from Doctor Ana Maria Mihalcea’s recent article entitled, "Hydrogel Platform Enables Versatile Data Encryption And Decryption" The building blocks of Hydrogels are being found in the COVID vaccine, and Hydrogels are being found in the blood of both the vaccinated and the unvaccinated. They are the so-called blood clots that are being found around the world. And these Hydrogels can now be programmed, encrypted and decrypted. According to Mihalcea, they are the substrate of the brain computer interface and the primary method of fusing humans with machines as she described by referencing MIT research in the article, “Hydrogel Interfaces for Merging Humans and Machines” Elements which Mihalcea and Clifford Carnicom found with Near Infrared spectroscopy in the blood of the unvaccinated exposed to shedding and environmental contamination include hydrogel plastics such as polyenes, vinyl, nylon, kevlar, and spider silk proteins. As well as other nanotechnology signatures such as silicone and sulfur. This technology hijacks methyl groups, which are needed to detoxify and create Glutathione in the body. Hydrogels used for the encrypted programmable technology include polyvinyl alcohol and polycaprolacton. Both of these Hydrogels are listed as stealth nanoparticles in the Moderna patent for lipid nanoparticle composition. This suggests that not only those who received the shot have this hydrogel encryption technology in their bodies, but also those who have experienced shedding and environmental contamination. Which is just about everyone. These hydrogels are known to be programmable and encrypted. This technology can behave as brain storage. It can store memories and visual information in an individual’s brain. And it can be chemical-induced to be securely encrypted and decrypted allowing for the secure recording and storage of confidential visual information. This provides a platform for secure financial transactions, which is a requirement for a digital ID. MIT researchers have discussed how this very same technology can be used to fuse humans with machines. And while they’ve had problems working it out in the past, a recent paper has announced they’ve found success using the very same elements found in both the blood of the vaccinated and unvaccinated by Mihalcea and Carnicom. In a lecture by Professor Sakhrat Khizroev at the University of Miami, it is discussed how advanced materials can be used for interfacing machines and the human brain. He references a research project funded by DARPA wherein magnetic nanoparticles are key to this technology. Mihalcea has published research that shows how the COVID shots alter torsion fields in the body and produce magnetism. A review by the Rand Corporation, “Brain Computer Interfaces: US Military Applications and Implications” discusses the convergence of human with machine. In an interview with Big Pharma whistleblower, Karen Kingston, Kingston discusses this self assembly nanotechnology and how the spike protein is an engineered device, triggered by electromagnetic frequency, and how the Quantum Dots are gene editing technology. This nanotechnology appears to be distributed via Chemtrails, the food and water supply, medications, and in all of the scheduled vaccines for children. It has been found by multiple scientists in the blood of both the vaccinated and the unvaccinated. And the fact that this widespread technology is being ignored while the topic of mRNA is being pushed into the mainstream, is of great concern. Mihalcea has shown that the new protocols being sold to the public as a way of reversing the negative effects of the COVID shots, have no effect on these Hydrogels. And it would seem that well over a billion people are infected with them. While many are talking about an archaic implanted computer chip, it seems that the latest breakthrough technology has already been deployed without anyone’s consent. The situation almost seems hopeless, but where there is a will there is a way. And now is not the time to hide our head in the sand. The human body is miraculous and our potential is endless. The more people addressing this dire situation, the better chances we have of finding a remedy. https://rumble.com/v4dqd6t-hydrogels-in-covid-vaccine-as-programmable-human-interface.html
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  • Rubbery Clot Development Observations In C19 Unvaccinated Blood With Different Anti Oxidant Compounds - Comparison with Clifford Carnicoms CDB/Morgellons Historical Culture Work
    Ana Maria Mihalcea, MD, PhD

    Image: C19 unvaccinated blood from 2 different individuals. First 4 syringes contain Alpha lipoic Acid, Glutathione, Plaquex and Control sample. Second Set contain Methylene Blue and Glutathione and a Control Sample.

    I had previously posted experiments with C19 unvaccinated blood and different compounds that could inhibit the production of the rubbery clot material that Clifford Carnicom and I have shown to be Cross Domain Bacteria ( CDB) or Morgellon’s like - a polymerized protein that creates the rubbery clots. My most successful clot inhibition was with EDTA and Vitamin C. I have written multiple substacks regarding this research of the rubbery clot formation:

    Rubbery Clot Development In C19 Unvaccinated Individual With Previous Deep Vein Thrombosis and Massive Pulmonary Emboli - While On Eliquis, Nattokinase, Lumbrokinase and Serreptase

    Correlation Of Severity Of Live Blood Contamination Seen On Darkfield Microscopy With Visible Clotting In C19 Unvaccinated Individual

    C19 Unvaccinated Have Same Blood Clotting Problem As C19 Vaccinated - EDTA And Vitamin C Prevents Blood Clotting In C19 Unvaccinated

    What Happens To A Human When There Is More Hydrogel, Nanotechnology And Synthetic Biology Then Blood? And A HAARP Warning BY Cathy O'Brien From 1990's - Is 4Hz Accelerating This Process?

    Blood Clot Analysis From Living & Deceased Individuals Shows Consistent Findings: A Rubber Like Polymerized Protein - Microscopy Shows Filaments. Part 1 of 3 - Dr. Ana Mihalcea With Clifford Carnicom

    Blood Clot Analysis From Living And Deceased Individuals Near Infrared Spectroscopy Shows Multiple Hydrogel Polymer Components - Part 2 of 3 - Dr. Ana Mihalcea With Clifford Carnicom

    Blood Clot Analysis From Living And Deceased Individuals - Preliminary Chemical Solubility Testing - Part 3 of 3 - Dr. Ana Mihalcea With Clifford Carnicom

    The original research by Clifford Carnicom has similar results. Vitamin C had a very strong inhibition of replication of the CDB/ Morgellons which we have correlated to the rubbery clot development in the studies outlined above. NAC was also effective with Glutathione having some effects compared to no treatment but being less effective than the other two. Here are Cliffords historical articles:

    Growth Inhibition Achieved - Original article on Vitamin C, NAC, Glutathione testing

    Morgellons : A Working Hypothesis – PART III POTENTIAL MITIGATING STRATEGIES (RESEARCH BASED)


    Image: CDB cultures and inhibitory effects of Vitamin C, NAC, Glutathione by Carnicom Institute

    In the first image above, I show blood drawn from two C19 unvaccinated individuals mixed with different compounds - ages 40’s and 50’s. The blood was left to sit overnight before the syringes were examined. Both patients have been on detoxification strategies. This is the first set of C19 unvaccinated control blood, a rubbery clot clearly developed. I want to reiterate how abnormal this is and absolutely catastrophic for the human species. If you count medical school, I have been in the medical field now for 30 years. I have never ever seen blood turn into rubber until this past year, when I started looking at this nanotechnology and synthetic biology phenomenon - after the C19 bioweapon roll out. I was just part of a court hearing and will be part of the upcoming trial as a witness. Is there someone that comprehends the catastrophic nature of this single finding in clinical practice? Someone who can look at this and via sheer logic understand the ramifications of what this means - that unvaccinated people are developing the same rubbery clots as the C19 injected due to shedding?


    Image - courtesy Karen Kingston, FDA guidance on shedding

    Still, most people ignore these findings and think they are safe, even though more and more people, including the unvaccinated are developing turbo cancers and are dying suddenly. I believe the reason for this development can be found in the blood, and if not mitigated or ignored, can have detrimental health effects.


    Image: C19 Unvaccinated blood control shows yellow rubbery hydrogel development

    In the video below you see the sample of 30 ml of C19 unvaccinated blood mixed with 1 cc Glutathione 200mg/ml concentration:

    Here is Methylene Blue, a molecule used for anti aging purposes, a precursor for Hydroxychloroquine. I use Methylene Blue a lot due to its ability as a direct electron donor bypassing mitochondrial dysfunction and its capacity to increase oxygen delivery between 30-70 %. You can see that the hydrogel development was inhibited, while the blood clot part was still rubbery. Normally you should be able to break apart a clot with your hands and I am not able to do anything to this rubber.

    This is C19 unvaccinated blood from a second person - this time mixed with Alpha Lipoic Acid 1 ml - Concentration 200mg/ ml. No inhibition of hydrogel seen.

    Here is it mixed with Plaquex, a patented form of Phosphatidylcholine that reverses Atherosclerosis. While these molecules do not inhibit growth after blood is drawn, I still highly recommend them for other functions. Plaquex has been shown to work amazing in reversing oxidative stress affecting the cell membranes of red blood cells and appears to make them more resistant to the assault of the CBD/ microbots. I have shown this in previous live blood analysis.

    This is the control sample without anything in it except C19 unvaccinated blood. Huge hydrogel rubbery clot developed that sticks to the syringe.

    I tested Glutathione again, this is actually my third time and it does not inhibit the hydrogel/ CDB growth.

    Summary:

    I am still exploring mitigation strategies and test molecules that I have been using already for my detoxification protocol to help support the body. In my clinic, I have seen that oral supplements must be supported with iv therapy - if you take supplements my mouth only, even EDTA - it is simply not enough anymore. A maintenance with oral EDTA/ Minerals and regular IV therapy at this time of high contamination delivers best results. Everything and everyone is so contaminated, that the best strategy is to detox with EDTA and Vitamin C while using all the other supplements to enhance immune function. I still use Nattokinase, but you have seen in my article above, that does not prevent the hydrogel rubbery clots. The two individuals who’s blood I tested here were both on 20.000 Units of Nattokinase daily. I use Methylene Blue at a dose of 50mg to 100mg daily depending on the person - from compounding pharmacies if no contraindications exist. You can see from the blood results, that Methylene Blue is a significant contender in helping us against these rubbery clots.

    I wanted to mention that persistence, determination and a fighting spirit is absolutely necessary to maintain your health. Many people do not even fight for their life, they just ignore the threat. Some people give up at first defeat, because it is too hard and inconvenient. What is still coming in illness in death will be unfathomable for most people’s comprehension. People do not want to hear that because it is too uncomfortable. I suggest you start fighting for your life and rearranging priorities. I have seen many people crushed who just wanted to keep ignoring shedding and partying on - until they got their very advanced cancer diagnosis or their blood clotting event. Its everywhere, in all age groups. And those cancers grow fast and furious. I have already had many unvaccinated patients die from shedding. I know because their cancer came after excessive exposure to vaccinated people. Open your eyes and see it. And then do what you can to save your own life and clean your own blood.

    In our meeting with the attorney today we were discussing the timeline of getting a verdict for the main trial. It was estimated at a year.

    I tell you, many people may not have a year with this in their blood and without mitigation strategies. That is not science fiction or fear mongering on my part, as much as my colleagues deny my findings. Look at the rubber clots and contemplate the potential outcome on a human of any age with this in their body. Despite the C19 bioweapon uptake going down, the blood contamination of people is going up, indicating persistent replication of synthetic biology and nanotechnology. I find this CATASTROPHIC in what it suggests for the future of humanity.

    Decontaminating The Blood From Synthetic Biology Hydrogel With EDTA Chelation - Live Blood Documentation

    THERE IS HOPE - EDTA CHELATION WORKS and What Really IS COVID???

    Hope Wins: Before And After Intravenous EDTA Chelation + Vitamin C - Dark Field Live Blood Analysis - A Case Report


    Med Five Patented EDTA
    Rubbery Clot Development Observations In C19 Unvaccinated Blood With Different Anti Oxidant Compounds - Comparison with Clifford Carnicoms CDB/Morgellons Historical Culture Work Ana Maria Mihalcea, MD, PhD Image: C19 unvaccinated blood from 2 different individuals. First 4 syringes contain Alpha lipoic Acid, Glutathione, Plaquex and Control sample. Second Set contain Methylene Blue and Glutathione and a Control Sample. I had previously posted experiments with C19 unvaccinated blood and different compounds that could inhibit the production of the rubbery clot material that Clifford Carnicom and I have shown to be Cross Domain Bacteria ( CDB) or Morgellon’s like - a polymerized protein that creates the rubbery clots. My most successful clot inhibition was with EDTA and Vitamin C. I have written multiple substacks regarding this research of the rubbery clot formation: Rubbery Clot Development In C19 Unvaccinated Individual With Previous Deep Vein Thrombosis and Massive Pulmonary Emboli - While On Eliquis, Nattokinase, Lumbrokinase and Serreptase Correlation Of Severity Of Live Blood Contamination Seen On Darkfield Microscopy With Visible Clotting In C19 Unvaccinated Individual C19 Unvaccinated Have Same Blood Clotting Problem As C19 Vaccinated - EDTA And Vitamin C Prevents Blood Clotting In C19 Unvaccinated What Happens To A Human When There Is More Hydrogel, Nanotechnology And Synthetic Biology Then Blood? And A HAARP Warning BY Cathy O'Brien From 1990's - Is 4Hz Accelerating This Process? Blood Clot Analysis From Living & Deceased Individuals Shows Consistent Findings: A Rubber Like Polymerized Protein - Microscopy Shows Filaments. Part 1 of 3 - Dr. Ana Mihalcea With Clifford Carnicom Blood Clot Analysis From Living And Deceased Individuals Near Infrared Spectroscopy Shows Multiple Hydrogel Polymer Components - Part 2 of 3 - Dr. Ana Mihalcea With Clifford Carnicom Blood Clot Analysis From Living And Deceased Individuals - Preliminary Chemical Solubility Testing - Part 3 of 3 - Dr. Ana Mihalcea With Clifford Carnicom The original research by Clifford Carnicom has similar results. Vitamin C had a very strong inhibition of replication of the CDB/ Morgellons which we have correlated to the rubbery clot development in the studies outlined above. NAC was also effective with Glutathione having some effects compared to no treatment but being less effective than the other two. Here are Cliffords historical articles: Growth Inhibition Achieved - Original article on Vitamin C, NAC, Glutathione testing Morgellons : A Working Hypothesis – PART III POTENTIAL MITIGATING STRATEGIES (RESEARCH BASED) Image: CDB cultures and inhibitory effects of Vitamin C, NAC, Glutathione by Carnicom Institute In the first image above, I show blood drawn from two C19 unvaccinated individuals mixed with different compounds - ages 40’s and 50’s. The blood was left to sit overnight before the syringes were examined. Both patients have been on detoxification strategies. This is the first set of C19 unvaccinated control blood, a rubbery clot clearly developed. I want to reiterate how abnormal this is and absolutely catastrophic for the human species. If you count medical school, I have been in the medical field now for 30 years. I have never ever seen blood turn into rubber until this past year, when I started looking at this nanotechnology and synthetic biology phenomenon - after the C19 bioweapon roll out. I was just part of a court hearing and will be part of the upcoming trial as a witness. Is there someone that comprehends the catastrophic nature of this single finding in clinical practice? Someone who can look at this and via sheer logic understand the ramifications of what this means - that unvaccinated people are developing the same rubbery clots as the C19 injected due to shedding? Image - courtesy Karen Kingston, FDA guidance on shedding Still, most people ignore these findings and think they are safe, even though more and more people, including the unvaccinated are developing turbo cancers and are dying suddenly. I believe the reason for this development can be found in the blood, and if not mitigated or ignored, can have detrimental health effects. Image: C19 Unvaccinated blood control shows yellow rubbery hydrogel development In the video below you see the sample of 30 ml of C19 unvaccinated blood mixed with 1 cc Glutathione 200mg/ml concentration: Here is Methylene Blue, a molecule used for anti aging purposes, a precursor for Hydroxychloroquine. I use Methylene Blue a lot due to its ability as a direct electron donor bypassing mitochondrial dysfunction and its capacity to increase oxygen delivery between 30-70 %. You can see that the hydrogel development was inhibited, while the blood clot part was still rubbery. Normally you should be able to break apart a clot with your hands and I am not able to do anything to this rubber. This is C19 unvaccinated blood from a second person - this time mixed with Alpha Lipoic Acid 1 ml - Concentration 200mg/ ml. No inhibition of hydrogel seen. Here is it mixed with Plaquex, a patented form of Phosphatidylcholine that reverses Atherosclerosis. While these molecules do not inhibit growth after blood is drawn, I still highly recommend them for other functions. Plaquex has been shown to work amazing in reversing oxidative stress affecting the cell membranes of red blood cells and appears to make them more resistant to the assault of the CBD/ microbots. I have shown this in previous live blood analysis. This is the control sample without anything in it except C19 unvaccinated blood. Huge hydrogel rubbery clot developed that sticks to the syringe. I tested Glutathione again, this is actually my third time and it does not inhibit the hydrogel/ CDB growth. Summary: I am still exploring mitigation strategies and test molecules that I have been using already for my detoxification protocol to help support the body. In my clinic, I have seen that oral supplements must be supported with iv therapy - if you take supplements my mouth only, even EDTA - it is simply not enough anymore. A maintenance with oral EDTA/ Minerals and regular IV therapy at this time of high contamination delivers best results. Everything and everyone is so contaminated, that the best strategy is to detox with EDTA and Vitamin C while using all the other supplements to enhance immune function. I still use Nattokinase, but you have seen in my article above, that does not prevent the hydrogel rubbery clots. The two individuals who’s blood I tested here were both on 20.000 Units of Nattokinase daily. I use Methylene Blue at a dose of 50mg to 100mg daily depending on the person - from compounding pharmacies if no contraindications exist. You can see from the blood results, that Methylene Blue is a significant contender in helping us against these rubbery clots. I wanted to mention that persistence, determination and a fighting spirit is absolutely necessary to maintain your health. Many people do not even fight for their life, they just ignore the threat. Some people give up at first defeat, because it is too hard and inconvenient. What is still coming in illness in death will be unfathomable for most people’s comprehension. People do not want to hear that because it is too uncomfortable. I suggest you start fighting for your life and rearranging priorities. I have seen many people crushed who just wanted to keep ignoring shedding and partying on - until they got their very advanced cancer diagnosis or their blood clotting event. Its everywhere, in all age groups. And those cancers grow fast and furious. I have already had many unvaccinated patients die from shedding. I know because their cancer came after excessive exposure to vaccinated people. Open your eyes and see it. And then do what you can to save your own life and clean your own blood. In our meeting with the attorney today we were discussing the timeline of getting a verdict for the main trial. It was estimated at a year. I tell you, many people may not have a year with this in their blood and without mitigation strategies. That is not science fiction or fear mongering on my part, as much as my colleagues deny my findings. Look at the rubber clots and contemplate the potential outcome on a human of any age with this in their body. Despite the C19 bioweapon uptake going down, the blood contamination of people is going up, indicating persistent replication of synthetic biology and nanotechnology. I find this CATASTROPHIC in what it suggests for the future of humanity. Decontaminating The Blood From Synthetic Biology Hydrogel With EDTA Chelation - Live Blood Documentation THERE IS HOPE - EDTA CHELATION WORKS and What Really IS COVID??? Hope Wins: Before And After Intravenous EDTA Chelation + Vitamin C - Dark Field Live Blood Analysis - A Case Report Med Five Patented EDTA
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  • W. M. Keck Observatory - A Strange, Solitary Life For Young Stars At The Milky Way’s Center:

    https://keckobservatory.org/s-stars/

    #SagittariusA #SStars #LonelyStars #Stars #BlackHole #MilkyWay #GalacticCenter #KeckObservatory #Spectrograph #Spectroscopy #InfraredAstronomy #Infrared #Astronomy #Astrophysics
    W. M. Keck Observatory - A Strange, Solitary Life For Young Stars At The Milky Way’s Center: https://keckobservatory.org/s-stars/ #SagittariusA #SStars #LonelyStars #Stars #BlackHole #MilkyWay #GalacticCenter #KeckObservatory #Spectrograph #Spectroscopy #InfraredAstronomy #Infrared #Astronomy #Astrophysics
    KECKOBSERVATORY.ORG
    A Strange, Solitary Life for Young Stars at the Milky Way’s Center
    The Keck Observatory telescopes on Maunakea in Hawaii, are the world’s largest optical and infrared telescopes. Keck Observatory's vision is to advance the frontiers of astronomy and share our discoveries with the world.
    0 Comments 0 Shares 9545 Views
  • Ingrid Fadelli - A highly precise terahertz molecular clock:

    https://phys.org/news/2023-04-highly-precise-terahertz-molecular-clock.html

    #AtomicClock #MolecularClock #Clock #Strontium #Sr2 #Terahertz #VibrationalModes #LASERs #Supercooling #Spectroscopy #Physics
    Ingrid Fadelli - A highly precise terahertz molecular clock: https://phys.org/news/2023-04-highly-precise-terahertz-molecular-clock.html #AtomicClock #MolecularClock #Clock #Strontium #Sr2 #Terahertz #VibrationalModes #LASERs #Supercooling #Spectroscopy #Physics
    PHYS.ORG
    A highly precise terahertz molecular clock
    In recent years, many physicists worldwide have introduced atomic clocks, systems to measure the passing of time that are based on quantum states of atoms. These clocks can have numerous valuable applications, for instance in the development of satellite and navigation systems.
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  • Li Yuan - Novel probe helps to detect deep sea biological macromolecules:

    https://phys.org/news/2023-03-probe-deep-sea-biological-macromolecules.html

    #RamanScattering #InsertionProbe #RiPSERS #AcetylCoA #βCarotene #AminoAcids #BiologicalMacromolecules #CAS #Spectroscopy #DeepSea #SeepVents #Biomolecules #Biology #Oceanology
    Li Yuan - Novel probe helps to detect deep sea biological macromolecules: https://phys.org/news/2023-03-probe-deep-sea-biological-macromolecules.html #RamanScattering #InsertionProbe #RiPSERS #AcetylCoA #βCarotene #AminoAcids #BiologicalMacromolecules #CAS #Spectroscopy #DeepSea #SeepVents #Biomolecules #Biology #Oceanology
    PHYS.ORG
    Novel probe helps to detect deep sea biological macromolecules
    The phenomenon of chemically synthesized life in extreme deep-sea environment is an international research hotspot in deep-sea science and life science. However, due to the extremely low concentration of organic macromolecules such as extracellular metabolites synthesized by deep-sea chemicals and the complex surrounding environment, there is no in-situ detection technology so far.
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