The Many Ways in Which COVID Vaccines May Harm Your Health

COVID-19 vaccines are capable of causing damage in a number of different ways leading to lung damage and heart and brain diseases.

In this interview, Stephanie Seneff, Ph.D., and Judy Mikovits, Ph.D., a dream-team in terms of deep insights into the scientific details, explain the problems they see with gene-based COVID-19 vaccines. There is a load of highly useful technical information that you can use to defend your opposition to these dangerous vaccines.

However, unless you have deeply studied molecular biology and genetics, it would be wise to view the video two or three times, as with each review, you will learn more and understand just how dangerous these vaccines are. I recently interviewed Seneff about the excellent paper[1] she published on this topic. That interview was featured in “COVID Vaccines May Bring Avalanche of Neurological Disease.”

In May 2020, I also interviewed Mikovits about the possibility of these vaccines causing reproductive harm and other health problems. At the time, Mikovits warned that fertility rates may drop thanks to the SARS-CoV-2 spike protein creating antibodies that attack syncytium, and indeed, we’re now starting to see that.

Still, the U.S. Centers for Disease Control and Prevention are recommending pregnant women get these vaccines, as well as children, which is unconscionable, considering the potential lifelong risks and impairment of fertility.

The Spike Protein Is the ‘Bioweapon’

As noted by Mikovits, we now know that the worst symptoms of COVID-19 are created by the SARS-CoV-2 spike protein, and that is the very thing these gene-based vaccines are instructing your body to make. But it’s far worse, as the vaccines do not cause your body to make the same spike protein as SARS-CoV-2 but one that has been genetically modified, making it far more toxic. So, it’s no wonder things are going wrong.

“The SARS-CoV-2 infection never was what they said it was,” Mikovits says. “There was no infection asymptomatically, but the spike protein is clearly [causing] the disease.

So, you just injected the envelope of HIV … a syncytin gammaretrovirus envelope, and a SARS S2 receptor binding domain. That’s not a vaccine. It is the disease-causing agent. So now your cells are all producing that ‘bioweapon’ and you’re going to take out the innate immunity, NK [natural killer] cells and dendritic cells …

You’re going to disrupt your white blood cells, your immune response. You’re going to turn on an anti-inflammatory cytokine signature in every cell of your body. It exhausts your NK cells’ ability to determine infected cells. It’s the nightmare we predicted.”

The Spike Protein Produced in Your Body Is Highly Unnatural

In her paper, “Worse Than The Disease: Reviewing Some Possible Unintended Consequences of mRNA Vaccines Against COVID-19,” published in the International Journal of Vaccine Theory, Practice and Research in collaboration with Dr. Greg Nigh,[2] Seneff explains that a significant part of the problem is that while the natural spike protein is bad, the spike protein your body produces in response to the vaccine is even worse.

The reason for this is because the synthetic RNA has been manipulated in such a way as to create a very unnatural spike protein that result in it not collapsing on itself into the cell once it attaches to the ACE2 receptor, as it normally does. Instead it stays open and attached to the ACE2 receptor, disabling it and causing a host of problems leading to heart, lung, and immune impairment. As explained by Seneff:

“They modified the RNA to make it really sturdy so the enzymes can’t break it down … Normally, enzymes that are in your system would just break down that RNA. RNA is very fragile, but they’ve made it sturdy by putting in PEG [polyethylene glycol], by adding this lipid membrane, and the lipid is positively charged, which causes the cell to be very upset when that goes into the membrane of the cell.

But I think maybe the most disturbing thing is they actually modified the [RNA] code so that it doesn’t produce a normal version of the spike protein. It produces a version that has a couple of prolines in it, side by side at the critical place where this spike protein normally would fuse with the cell that it’s infecting.

So, the spike protein binds to the ACE2 receptor once it’s produced by the human cell … but it’s a modified version of the spike protein. It has these two prolines that make it very stiff so that it can’t reshape. Normally it would bind to the ACE2 receptor and then it would reshape and go straight into the membrane like a spear.

Because of this redesign, it can’t do that, so it sits there on the ACE receptor, exposed … That allows the immune cells to produce antibodies specific to that place where it should be fusing with the cell, the fusion domain. It messes up the fusion domain, keeps the protein open, and prevents the protein from getting in, which means the protein will just stick there on the ACE2 receptor, disabling it.

When you disable ACE2 receptors in the heart, you get heart failure. When you disable them in the lungs, you get pulmonary hypertension. When you do it in the brain, you get stroke. Lots of nasty things happen when you disable ACE2 receptors …

The other thing they’ve done with the RNA is they’ve stuck in a lot of extra Gs (guanine) and Cs (cytosine), which makes it much better at making proteins. It’s turned up the gain on the natural virus 1,000-fold, making the RNA much more willing to make a protein. So, it’ll make a lot more spike protein than you would’ve had from a natural RNA virus.”

Reality Is Exponentially Worse Than Predicted

With the added information provided by Seneff, Mikovits now believes the reality of these vaccines may be exponentially worse than she initially predicted a year ago. Not only is the lipid nanoparticle a serious hazard, as we’ve seen with Gardasil and some of the newer hepatitis B vaccines, but we now also have the added issue of unnatural mRNA, made more robust so as to evade its natural breakdown.

As explained by Mikovits, free RNA acts as a danger signal inside your body, so now your system is on red alert for however long the RNA remains viable. Now, by manipulating the RNA code to be enriched in G and C, and configured as if it’s a human messenger RNA molecule ready to make protein by adding a polyA tail, the spike protein’s RNA sequence in the vaccine looks as if it is part bacteria,[3] part human[4] and part viral at the same time.

“We use poly(I:C) [a toll-like receptor 3 agonist] to signal the cell to turn on the type I interferon pathway,” Mikovits explains, “and because this is an unnatural synthetic envelope, you’re not seeing poly(I:C), and you’re not [activating] the Type I interferon pathway.

You’ve bypassed the plasmacytoid dendritic cell, which combined with IL-10, by talking to the regulatory B cells, decides what subclasses of antibodies to put out. So, you’ve bypassed the communication between the innate and adaptive immune response. You now miss the signaling of the endocannabinoid receptors …

A large part of Dr. [Francis] Ruscetti’s and my work over the last 30 years has been to show you don’t need an infectious transmissible virus — just pieces and parts of these viruses are worse, because they also turn on danger signals. They act like danger signals and pathogen-associated molecular patterns.

So, it synergistically leaves that inflammatory cytokine signature on that spins your innate immune response out of control. It just cannot keep up with the myelopoiesis [the production of cells in your bone marrow]. Hence you see a skew-away from the mesenchymal stem cell towards TGF-beta regulated hematopoietic stem cells.

This means you could see bleeding disorders on both ends. You can’t make enough firetrucks to send to the fire. Your innate immune response can’t get there, and then you’ve just got a total train wreck of your immune system.”

With respect to Mikovits’ comment that pieces and parts of the virus are actually worse than the whole virus, that is precisely what we have with the COVID vaccines. In last week’s interview with Seneff, she explained how the manufacturing process leaves fragmented genetically modified RNA in the vaccine. They are not filtered out and assumed to be harmless, but as Mikovits states, this is not the case. This is being completely missed as one reason why this vaccine is so dangerous.

Latent Viruses May Flare if You Receive the COVID Vaccine

As noted by Seneff, her and Mikovits’ findings mesh well to explain many of the problems we’re now seeing from these gene-therapies. For example, vaccinated patients are reporting herpes and shingles infection following COVID-19 vaccination, which you’d expect if your Type I interferon pathway is disabled.

“Basically, you’ve got these latent viruses that are not bothering you at all until your immune system gets completely distracted by this crazy thing going on in the spleen with all this messenger RNA and all these spike proteins,” Seneff says.

“Immune cells are distracted from their other job of keeping these viruses in check. So, you get these other conditions showing up, and there are several. There’s Bell’s palsy (facial palsy), for example. There are over 1,200 cases of Bell’s palsy reported after the vaccine in the Vaccine Adverse Event Reporting System (VAERS).

And when you look at the research of what causes that, they really point to the herpes virus and the varicella virus as being the source of Bell’s palsy. The Type I interferon system is what you need to keep these guys in check, and so those viruses are getting enabled and they’re causing symptoms.

That is actually a very bad sign. If a woman who’s pregnant has a herpes flare-up during pregnancy, she has a twofold increased risk of producing an autistic son.

Also, in a study on 200 Parkinson’s patients, compared to 200 age- and gender-matched controls, six of those Parkinson’s patients had at least one episode of Bell’s palsy in the past, whereas none of the controls had. So, it looks to me like the Bell’s palsy is an indicator of a future risk of Parkinson’s disease.”

To summarize, it looks as though pregnant women who are getting the COVID-19 vaccine are at increased risk not only for miscarriage but also for future infertility and having an autistic child. So, please, be careful out there and spread the word.

The best way to treat any disease is to prevent it. These vaccines simply are not decreasing COVID-19 but radically decreasing the health of those who receive it, especially pregnant women that the CDC merely a month ago encouraged to get vaccinated without a shred of safety evidence.

The Importance of Type I Interferon

Mikovits has done a great deal of research on interferon for the last 40 years. Innate immune interferon makes up your entire frontline defense. People with HIV/AIDS have dysregulated Type I interferon, which allows parasites to gain a solid foothold. Interestingly enough, antiparasitic drugs such as hydroxychloroquine and ivermectin have been shown to be effective against COVID-19, both prophylactically and in treatment.

Mikovits cites a research paper[5] titled “War and Peace Between Microbes,” which details how HIV-1 interacts with coinfecting viruses, thereby accelerating the disease. Herpes viruses in particular have been implicated as a cause of AIDS. Human herpesvirus 6 (HHVS-6) has also been implicated in myalgic encephalomyelitis or chronic fatigue syndrome (ME-CFS).

In short, these diseases, AIDS and ME-CFS, don’t appear until viruses from different families partner up and retroviruses take out the Type 1 interferon pathway.

In short, the COVID-19 vaccines are capable of causing damage in a number of different ways. Disturbingly, all these different mechanisms of harm have synergistic effects when it comes to dysregulating your innate and adaptive immune systems and activating latent viruses. “It’s just an explosion of a nightmare of crippling every area of your immune response,” Mikovits says.

How mRNA Can Alter Your DNA

In her paper, Seneff also describes how mRNA can, in fact, alter your DNA, essentially integrating the instructions to make spike proteins into your genome. Typically, mRNA cannot be integrated directly into your genes because you need reverse transcriptase.

Reverse transcriptase converts RNA back into DNA (reverse transcription). However, there’s a wide variety of reverse transcriptase systems already embedded in our DNA, which makes this possible. This is an area that Mikovits has studied for decades, so, commenting on Seneff’s findings, she says:

“When you activate latent and defective viruses, you turn on reverse transcriptase; you turn on the virome. But you also need an integrase gene. So how are retroviruses silenced? [Through] DNA methylation. [When] you throw in a lot of GC-rich regions — you’ve got that synthetic viral particle [i.e., the vaccine-induced spike protein RNA] — now you’ve woken up your herpes viruses.

[Latent viruses] are silenced [through] DNA methylation, but as our soil is depleted in minerals, we have people with methylation defects. This is why I said the first people who are going to die are people with inflammatory conditions and cancer.”

SARS-CoV-2 Spike Protein May Be a Prion

In her paper, Seneff also discusses evidence suggesting the SARS-CoV-2 spike protein may be a prion, which is yet another piece of really bad news. “It’s absolutely terrifying to me,” she says, adding:

“I’m now thinking that may be the worst aspect of these mRNA vaccines, because they’re producing this abnormal spike protein that doesn’t want to go into the membrane. Prion proteins are known to be membrane proteins. They’re alpha-helices in the membrane and then they misfold, becoming beta-sheets in the cytoplasm, and that’s what leads to the prion problem.

They form a crystal that draws in other proteins and makes this big mess and builds fibrils and Alzheimer’s plaque. The main prion protein is PrP, which is in Creutzfeldt-Jakob disease, the human form of mad cow disease. It’s a sort of protein-source infection. It’s quite wild because there’s no DNA involved, no RNA involved, just protein.

But the thing is, when you have produced a version of mRNA that knows how to spew out tons of a prion protein, the prion proteins become problematic when there’s too many of them and the concentration is too high in the cytoplasm.

And the spike proteins that these mRNA vaccines are producing … isn’t able to go into the membrane, which I think is going to encourage it to become a problematic prion protein. Then, when you have inflammation, it upregulates alpha-synuclein [a neuronal protein that regulates synaptic traffic and neurotransmitter release].

So, you’re going to get alpha-synuclein drawn into misfolded spike proteins, turning into a mess inside the dendritic cells in the germinal centers in the spleen. And they’re going to package up all this crud into exosomes and release them. They’re then going to travel along the vagus nerve to the brainstem and cause things like Parkinson’s disease.

So, I think this is a complete setup for Parkinson’s disease. What may happen is that because they got this vaccine, they get Parkinson’s disease five years earlier than they would have gotten it otherwise. It’s going to push forward the date at which someone who has a propensity towards Parkinson’s is going to get it.

And it’s probably going to cause people to get Parkinson’s who never would have gotten it in the first place — especially if they keep getting the vaccine every year. Every year you do a booster, you bring the date that you’re going to get Parkinson’s ever closer.”

This is taken from a long document. Read the rest here: theepochtimes.com

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Comments (17)

    • Avatar

      Alcheminister

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      Why covid injections are not vaccines?

      Please explain. Every vaccine ever has no potential benefit, is toxic, for the purpose of causing disease and based on fraud. Now, you could argue covid vaccines are “more advanced”, but like every other vaccine, it’s BS.

      Would you like to perhaps tell me which vaccines YOU think are worth using?

      Reply

      • Avatar

        Alcheminister

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        Do people actually understand how many toxic factors change their genetic material (including every vaccine ever)?

        Reply

        • Avatar

          Alcheminister

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          Oh and anyone trying to harp on about the importance of “viruses” as causative is a charlatan, a piece of shit or an idiot and not worth considering.

          Reply

          • Avatar

            Mark Tapley

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            Viruses and pathogenic transmission are the sacred dogma of germ theory allopathic medicine. And a big factor for controlling the herd in the digital prison where we are all Palestinians of Gaza. Read the real history of “vaccines” in Suzanne Humphries MD “Dissolving Illusions.” Also on the fake Polio, Maready’s “The Moth In The iron Lung.”

          • Avatar

            Alcheminister

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            Mark, to me it’s simple. There is simply no evidence for contagion or the supposed virus functionality. Even by their descriptions, they cannot exist or function as claimed.

            People ignore that the supposed “diagnostics” are massively flawed, alter material (which happens to be nowhere near indicative of health status) deviate to the point of irrelevance, they ignore thousands of factors known to be causative in disease. They use religious reductionist reasoning and jump to conclusions based on whatever cultist zealotry they’ve been indoctrinated with through say, fearmongering (much like you’d find in abrahamism, which essentially a template) or institutional “credentials” (certification of being souled out).

            I made some TMV (hint, it involves phosphorus, anthocyanin, heat, energy, metabolic deficiencies and imbalances) the previous winter ffs, WHILE simultaneously disproving contagion.

            I’ve never caught a disease from anyone ever and I’ve been around a lot of sick people and since I was a toddler was heavily involved with medical institution (which is related to how I noticed everything pharma is BS).

            By their idiot reasoning, if you even walk past a hospital or a clinic, you should have like 500 new diseases (just keep on ignoring 80 years of actual tons of physical inputs and toxins), every doctor and nurse should be dead.

          • Avatar

            Alcheminister

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            And none of them even want to consider that you cannot be immune to deficiencies or excessive toxicity. Which is for instance, associated with recurring disease, regardless of things like vaccines, antibodies (btw, high antibody counts are associated with severe toxicity). You know, like how people get RTIs in winters, never developing immunity, or recurring symptomatic issues from not addressing those causative factors.

      • Avatar

        Mark Tapley

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        Yes Alcheminister, Pasteur never transmitted anything but the injection of toxins (usually arsenic or mercury). He even admitted it on his deathbed, “The germ is nothing. The terrain is everything.” His medical diary that was not to ever be published has finally revealed his 40 years of deception.

        Reply

    • Avatar

      Alcheminister

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      Oh also, the 5G shit. See, if there is graphene in the vaccines, graphene collapses and aggregates tissues and makes a “bio-corona” (that’s what the literature before “covid” says). Now, if graphene comes into contact with red blood cells, it could conceivably collapse those red blood cells and aggregate iron oxide (magnetite, hematite sort of) structures. Aside from the implications of that regarding neutrophil, fibrin sort of issues, there’s iron and oxygen hijacking (localized anemia/lack of iron, oxygenation) and also clotting associated. Magnetite is almost ideal for EM absorption in the range of much of popularized and promoted anthropogenic EM (roughly 100mhz to 10ghz). Quite a bit of the supposed 5G happens to be around the 3G sort of frequency (tending to roughly the middle of that range I speak about). 3G happens to be associated with say, colony collapse in bees (because bees use magnetite for navigation). So around the 3G (which includes much of the 5G frequency) range, there’s around 10^(18-20) more EM than natural. In America, I recently read there’s almost 6w/m2 on average these days, that’s a fuckload and it WILL cause issues because no natural systems are adapted to that. Also, IBM has iron oxide storage at a few atoms per bit, they’re heavily invested in a “vaccinated world” and have done security and data management related shit for vax manufacturers apparently. AND there’s quite a lot of “literature” about say, PEG, neutrophil, fibrin, graphene sort of BS for things like crossing the BBB regarding to pharma toxification and/or influence.

      So yeah, don’t underestimate 3G sort of frequencies, it’s typically, far more pervasive than 5G.

      Reply

      • Avatar

        Alcheminister

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        At least, the sort of 5G frequencies that is often mentioned (like near 60ghz). That sort of 5G is very limited (not only in terms of range), easily blocked and likely not in use much.

        The typical 3G/WIFI sort of frequencies by virtue of interfering with things like iron oxide, hydrogen, hydrides happens to affect oxygen by virtue of things interacting and I mean, say, h2o (not like there’s any water in your body, right?).

        So yeah, minimize EM exposure if you can (sunlight helps, melatonin and in general mitochondrial suppor factors), and stay the fuck away from areas with high EM tower, base station density.

        Reply

    • Avatar

      Mark Tapley

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      Hello Chris:
      There is no proof of the successful application of mRNA spike protein technology. If there were there would be a mountain of data on it. T here are none. The only information are the phony microscopy photos of contaminated tissue samples, identical to what Enders provided in 1953 for the fake Polio vaccines. There is no evidence of any genetic modification but only a new and more deadly blood toxin packaged in the facade of a fake vaccine for a fake virus.

      Reply

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        Alcheminister

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        But Mark, toxins, deficiencies…excessive stressors, that’s genetic modification.

        Reply

        • Avatar

          Alcheminister

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          Pretty much anything you experience alters you, so…

          Reply

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          Mar Tapley

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          Hello Alcheminester:
          Yes technically those would also alter the body’s function and so they could result in devastating modifications, not only deficiencies but cancer and even epigenetic traits passed on to the next generation as shown by Pottenger’s cats. Of course that has always been the aim of the eugenicists in their desire to achieve a more efficient and manageable herd size.

          Reply

  • Avatar

    VOWG

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    The word “may” harm people is used in the headline. There is no freaking may6 about it. No studies are needed. The vaxxes are killing millions while words are being to obscure that fact. Stupid has become the order of the day and unless we stop asking for definitive proof that will never be seen, we will kill tens of millions more. Stop the insanity, there was never anything such thing as covid.

    Reply

    • Avatar

      Alcheminister

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      Russ, the “immune system” is an abstracted construct derived from health status (which is what matters). It’s used by pharma to avoid addressing health status. Every “immune response” they speak of is a measure of damage. They use those concepts (“immune system” and “immune response”) to peddle toxic BS. Antibody responses for instance, are elicited with toxicity, 1:1 neutralizing intermediaries (within the body’s capacity).

      My sister (“geneticist”) and others (being naive and indoctrinated), when working on TB and HIV vaccine shit (funded by b&m gates and such) tried REALLY hard to elicit t-cell responses (because that’s a result of/response to SEVERE toxicity). She apparently did manage to elicit t-cell responses relating to supposed HIV in GMO “humanized” mice and her work was “disappeared”. But what elicited those responses was super toxic.

      Reply

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