COVID-19 RNA Based Vaccines and the Risk of Prion Disease

 

Vaccines have been found to cause a host of chronic, late developing adverse events. Some adverse events like type 1 diabetes may not occur until 3-4 years after a vaccine is administered [1]. In the example of type 1 diabetes the frequency of cases of adverse events may surpass the frequency of cases of severe infectious disease the vaccine was designed to prevent.

Given that type 1 diabetes is only one of many immune mediated diseases potentially caused by vaccines, chronic late occurring adverse events are a serious public health issue. The advent of new vaccine technology creates new potential mechanisms of vaccine adverse events. For example, the first
killed polio vaccine actually caused polio in recipients because the up scaled manufacturing process did not effectively kill the polio virus before it was injected into patients. RNA based
vaccines offers special risks of inducing specific adverse events.

One such potential adverse event is prion based diseases caused by activation of intrinsic proteins to form prions. A wealth of knowledge has been published on a class of RNA binding proteins shown to participating in causing a number of neurological diseases including Alzheimer’s disease and ALS. TDP-43 and FUS are among the best studied of these proteins [2].

The Pfizer RNA based COVID-19 vaccine was approved by the US FDA under an emergency use authorization without long term safety data. Because of concerns about the safety of this vaccine a
study was performed to determine if the vaccine could potentially induce prion based disease.

Discussion

There is an old saying in medicine that “the cure may be worse than the disease.” The phrase can be applied to vaccines. In the current paper the concern is raised that the RNA based COVID vaccines have the potential to cause more disease than the epidemic of COVID-19.

This paper focuses on a novel potential adverse event mechanism causing prion disease which could be even more common and debilitating than the viral infection the vaccine is designed to prevent. While this paper focuses on one potential adverse event there are multiple other potential fatal adverse events as discussed below.

Over the last two decades there has been a concern among certain scientists that prions could be used as bioweapons. More recently there has been a concern that ubiquitous intracellular molecules could be activated to cause prion disease including Alzheimer’s disease, ALS and other neurodegenerative diseases.

This concern originates due to potential for misuse of research data on the mechanisms by which certain RNA binding proteins like TDP-43, FUS and others can be activated to form disease causing prions. The fact that this research, which could be used for bioweapons development, is funded by private organizations including the Bill and Melinda Gates Foundation, and Ellison Medical Foundation [2] without national/international oversight is also a concern.

In the past, for example, there were prohibitions for publishing information pertaining to construction of nuclear bombs.

Published data has shown that there are several different factors that can contribute to the conversion of certain RNA binding proteins including TDP-43, FUS and related molecules to their pathologic states. These RNA binding proteins have many functions and are found in both the nucleus and the cytoplasm.

These binding proteins have amino acid regions, binding motifs that bind specific RNA sequences. Binding to certain RNA sequences when the proteins are in the cytoplasm is believed to causes the molecules to fold in certain ways leading to pathologic aggregation and prion formation in the cytoplasm [2]. The current analysis indicates Pfizer’s RNA based COVID-19 vaccine contains many of these RNA sequences that have been shown to have high affinity for TDP-43 or FUS and have the potential to induce chronic degenerative neurological diseases.

Zinc binding to the RNA recognition motif of TDP-43 is another mechanism leading to formation of amyloid like aggregations [9]. The viral spike protein, coded by the vaccine RNA sequence, binds ACE2 an enzyme containing zinc molecules [8]. This interaction has the potential to increase intracellular zinc levels leading to prion disease. The initial binding could be between spike proteins on the surface of the cell transfected by the vaccine and ACE2 on the surface of an adjacent cell. The resulting complex may become internalized.

Alternatively, the interaction could initially take place in the cytoplasm of a cell that makes ACE2 and has been transfected with the vaccine RNA coding for the spike protein. The interaction is quite concerning given the belief that the virus causing COVID-19, SARS-CoV-2, is a bioweapon [10,11] and it is possible that the viral spike protein may have been designed to cause prion disease. Another related concern is that the Pfizer vaccine uses a unique RNA nucleoside 1-methyl-3′-pseudouridylyl (Ψ). According to FDA briefing documents, this nucleoside was chosen to reduce activation of the innate immune system [12].

RNA molecules containing this nucleoside will undoubtedly have altered binding [13]. Unfortunately, the effect on TDP-43, FUS and other RNA binding proteins is not published. The use of this nucleoside in a vaccine can potentially enhance the binding affinity of RNA sequences capable of causing TDP-43 and FUS to assume toxic configurations. There are many other potential adverse events that can be induced by the novel RNA based vaccines against COVID-19. The vaccine places a novel molecule, spike protein, in/on the surface of host cells.

This spike protein is a potential receptor for another possibly novel infectious agent. If those who argue that the COVID-19 is actually a bioweapon are correct, then a second potentially more dangerous virus may be released that binds spike protein found on the host cells of vaccine recipients.

Download the full paper at www.nutritruth.org

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Comments (6)

  • Avatar

    Tom

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    This explanation is a bit technical. Based on the potential to inject billions of test subjects many times in the coming years, the revenue streams for pharma companies is too great to ignore no matter how many millions might get some sort of disease in the future as the result of these gene scrambling therapies. The FDA and the CDC are far too weak to stop the pharma gravy train as they seek to inject the entire planet with these poisons that have never been proven safe. And why is there well over 100 other types of therapies (fake vaccines) being created and tested by dozens of drug makers?

    Reply

  • Avatar

    Wisenox

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    If the ACE2 is bound, doesn’t that mean it isn’t available to break down angiotensin 2? Angiotensin 2 has harmful effects in the body.
    High levels of Ang II are often related to hypertension, renal failure, and cardiac fibrosis.
    https://www.sciencedirect.com/topics/neuroscience/angiotensin-ii
    Angiotensin 2 is also linked to degenerative neurological diseases. Hopefully, I’m just misinterpreting the use of the term binding .

    Reply

  • Avatar

    Ken Hughes

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    Let’s face it, they’re going to try and kill most of us and our only defense is to not cooperate.

    Reply

  • Avatar

    Epicurious

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    Ken is sooooooooo right.

    Reply

  • Avatar

    Pete

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    Too technical for me,but I have always been against using vaccines and chosen to avoid them,simply because of the mechanism by which they work,the substances contained in them and the potential for initial reactions and possible long-term effects.I don’t want to get into conspiracy theory,but the motivation is clearly there and the profit potential goes without saying.I lost my father to ALZ and he was a committed vaccine user and my mum recently received the rna-based covid vaccine(moderna) and I’m concerned about that.Honestly,I would prefer the risk of not taking it than taking it.And the reality is that these vaccines often don’t provide the recipient with any immunity at all as they are implied to.

    Reply

  • Avatar

    Mark Tapley

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    Almost all of this stuff is theoretical. The existence of viruses has not even been proven much less the imaginary spike protein. We know that big Pharma has constructed a medical facade using a fake virus and cobbling together an Insilco (imaginary computer gene sequence) model and the fake PCR test, with the CDC -WHO fake numbers in the MSM controlled operative standard Zionist false flag operation.

    The only thing we know for sure is that this fake virus is a continuation of the toxic blood “vaccine” program started by Rockefeller’s (founders of the CDC) over a hundred years ago in order to condition the goyim to accept and follow big Pharma “guidance” as the herd is slowly weakened, sterilized and culled. Money is only a side benefit. The real agenda is total control. See videos and books by Forrest Maready and read the real history of “vaccines” in Suzanne Humphries MD “Dissolving Illusions.”

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