Blog: COVID & mRNA Vaccine News

23/Dec/22
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Appearing on “Ask Dr. Drew” the other day for an interview about Wuhan coronavirus (Covid-19) “vaccines,” pathologist and virology expert Dr. Ryan Cole, whose name you will probably recognize from our earlier jab coverage, revealed that the spike proteins in the injections cause prolific damage to the circulatory system.

The two started out discussing where spike proteins tend to lodge throughout the body. In Cole’s estimation, they go anywhere and everywhere they choose, including in the brain.

“It’s in the brain tissue,” Cole explained during the segment – watch below:

“Dr. Drew had a great question: ‘Is it in the brain matter, is it in the white matter, where in the brain?’ Wherever the lipid nanoparticle distributes – and it does get through the blood-brain barrier, and we know S1, the spike protein, gets through as well.”

Cole went on to explain that covid jab spike proteins “follow the small capillaries and leak into whatever tissue it wants to.”

Where the conversation really got interesting is when Cole showed slides depicting the inflammatory effects of spike proteins as they interact with lymphocytes.

“That spike protein causes the lymphocytes to chew a hole in the aorta,” Cole said.

“This is the biggest blood vessel in your body coming off your heart. When that ruptures, you’re gone in minutes. So that’s just another example of what deposited spike protein and the induced inflammation can do.” (Related: Last fall, Cole warned that cancer rates had spiked 20-fold among the fully jabbed.)

Covid jab spike proteins responsible for “clotting disease”
Cole, by the way, was among the first to explain the why behind the infamous clots that form following injection.

The spike proteins cause what Cole described as “clotting disease,” or the formation of those mysterious non-blood clots that some embalmers say they are pulling out of corpses.

Cole has also repeatedly addressed the fact that not all doctors and medical professionals are in agreement that the jabs are safe and effective. The only reason it seems that way is because the ones who disagree, including Cole, are systematically censored.

Covid jab disease can be summed up overall as endotheliitis, which is demarcated by inflammation of the lining of the blood vessels. Taking nattokinase can help alleviate it, an added benefit being that nattokinase is widely used throughout Japan to prevent Parkinson’s and Alzheimer’s disease.

One of the most concerning things about covid jabs, in Cole’s estimate, is the fact that their spike proteins are persistent. It takes the body a very long time to get rid of them – if it ever even does fully get rid of them.

The general population was never warned about any of these risks, which means informed consent was never part of the equation. Had it been, how many people still would have agreed to get shot?

“The history of covid is they fooled a majority of the people and inflicted great societal and medical harm by using the control they had over the CDC and FDA to mandate plausible and profitable mRNA vaccinations,” reads a tweet responding to the video above.

“Then they lied about the safety and effectiveness of the alternative early treatments in general, and ivermectin in particular. And they thought they could get away with it because they had control over more big governments, big tech corporations, and big media.”

Citation
(Huff, 2022). Covid jab spike proteins cause lymphocytes to “chew a hole in the aorta,” warns Dr. Cole. Retrieved on 12/22/22 online from https://chemicalviolence.com/2022-12-12-covid-jab-spike-proteins-lymphocytes-hole-aorta.html


22/Dec/22
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POPULAR ARTICLES

18/Dec/22
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RESEARCH PAPER

N-acetylcysteine (NAC) — Encourages glutathione production, thins mucus, lowers your chances of influenza infection, and reduces your risk of developing severe bronchitis.

Selenium — “Since selenium is an essential cofactor for certain peroxidases, and selenium deficiency has been endemic in certain regions of China and other parts of the world, insuring adequacy of selenium nutrition might also be appropriate in this context,” McCarty and DiNicolantonio note, adding:30

“Selenium deficiency also increases the rate at which viruses can mutate, promoting the evolution of strains that are more pathogenic and capable of evading immune surveillance.”

Zinc — Supports “effective function and proliferation of various immune cells,” lowering mortality in the elderly by 27%

Alpha Lipoic Acid — Helps boost type 1 interferon response. As explained in a 2014 paper:31

“Type I interferons (IFNs) activate intracellular antimicrobial programs and influence the development of innate and adaptive immune responses … (IFNs) are polypeptides that are secreted by infected cells and have three major functions.

  1. First, they induce cell-intrinsic antimicrobial states in infected and neighboring cells that limit the spread of infectious agents, particularly viral pathogens.
  2. Second, they modulate innate immune responses in a balanced manner that promotes antigen presentation and natural killer cell functions while restraining pro-inflammatory pathways and cytokine production.
  3. Third, they activate the adaptive immune system, thus promoting the development of high-affinity antigen-specific T and B cell responses and immunological memory. Type I IFNs are protective in acute viral infections but can have either protective or deleterious roles in bacterial infections and autoimmune diseases.”

Sulforaphane — Helps boost type 1 interferon response

 

PRODUCTS

AcuteShield Vanquish®
“Supports Vaccinated Health®
The nutraceutical composition of AcuteShield Vanquish® wherein the composition comprises Vitamin D3, Vitamin K2, Quercetin, Bromelain, Nigellin Sativa/Thymoquinone, Magnesium, Sulforaphane, N-acetylcysteine, Glutathione, Zinc, Piperine, Curcumin, Astaxanthin, and Pyrroloquinoline Quinone (PQQ).

AcuteShield Heart & Soul®
“Masters of Energy & Life”
The nutraceutical composition of AcuteShield Heart & Soul® wherein the composition comprises Vitamin D3, Vitamin K2, Vitamin B6, Vitamin B9, Vitamin B12, Magnesium, N-acetylcysteine, Glutathione, Alpha Lipoic Acid, Selenium, Zinc, Astaxanthin, and Pyrroloquinoline Quinone (PQQ).

AcuteShield Defcon 1®
“Cellular Level Support”
The nutraceutical composition of AcuteShield Defcon 1® wherein the composition comprises Cannabidiolic Acid (CBDa), Cannabigerolic Acid (CBGa), Cannabidiol (CBD), Cannabigerol (CBG), Vitamin D3, Vitamin K2, Magnesium, Quercetin, Zinc, Bromelain, Nigellin Sativa/Thymoquinone, Astaxanthin, and Pyrroloquinoline Quinone (PQQ). https://acuteshield.com

 

Table 1. Provisional daily dosage suggestions for nutraceuticals that might aid control of RNA viruses including influenza and coronavirus

Ferulic acid 500-1,000 mg
Alpha Lipoic Acid 1,200-1,800 mg (in place of ferulic acid)
Spirulina 15 g (or 100 mg PCB)
N-Acetylcysteine 1,200–1,800 mg
Selenium 50-100 mcg
Glucosamine 3,000 mg or more
Zinc 30-50 mg
Yeast Beta-Glucan 250-500 mg
Elderberry 600–1,500 mg

Citation

(McCarty, 2020). Science Direct: Nutraceuticals have potential for boosting the type 1 interferon response to RNA viruses including influenza and coronavirus. Retrieved on 12/18/22 online from https://www.sciencedirect.com/science/article/pii/S0033062020300372


11/Dec/22
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A study from Nature Neuroscience finds the S1 spike protein of SARS-CoV-2 crosses the blood–brain barrier in mice and can cause damage to the cardiovascular and central nervous systems. The spike protein is readily cleared from the blood and taken up by peripheral tissues. SARS-CoV-2 RNA was recovered from cerebrospinal fluid, proving it can cross the blood–brain barrier.

The study shows that these new spike proteins have been engineered to exploit angiotensin-converting enzyme 2 (ACE2), allowing for increased intake of spike proteins into the lungs and specifically to the brain. This is why a real case of SARS-CoV-2 can cause symptoms in the central nervous system, include changes to taste and smell, headaches, twitching, seizures, confusion, vision impairment, nerve pain, dizziness, impaired consciousness, nausea, hemiplegia, ataxia, stroke and cerebral hemorrhage.

So why are people going along with these new “vaccines” — if they turn their own cells into spike protein factories?

Intravenous administration of spike proteins concentrates in the brain TEN times greater than nasal exposure

The engineered SARS-CoV-2 spike protein binds to human cells using its S1 sub-unit. The researchers reveal that the S1 sub-unit was readily taken up in the parenchymal brain space, the hippocampus, the olfactory bulb, and was measured in eleven regions of the brain. When the spike proteins were administered intravenously, they concentrated in the brain TEN TIMES greater than when administered intranasally!

These are the same spike proteins that human cells are forced to translate, synthesize and replicate using the genetic instructions provided by new mRNA vaccines and adenovirus-vectored vaccines. The lab-engineered spike protein that is being mass produced in human cells is not only subverting the natural genetic template of protein synthesis, but it is also inundating the brain with foreign TOXINS.

The research finds that spike proteins readily cross the blood-brain barrier through a process called adsorptive transcytosis. Transcytosis is a type of trans-cellular transport in which various macro-molecules are transported across the interior of a cell. Adsorptive-mediated transcytosis provides a means for brain delivery of medicines across the blood-brain barrier.

Why are the spike proteins designed to readily adsorb across the blood brain barrier? Could this mode of action be intended to deliver other medicines and chemicals, genetic instructions or autoimmune attacks to the brain cells? Is this the real reason for encephalitis and brain hemorrhage following both infection and vaccination? What are the ramifications of spike proteins accumulating in the brain? Will recently vaccinated persons suffer acute or permanent brain damage from these experimental injections?

The research also showed that inflammation increases spike protein uptake in the brain and lungs. When the animals were induced with inflammation, the intravenously administered spike proteins entered the brain more readily. People who eat a plant-based, anti-inflammatory diet are more equipped to survive spike protein attacks to the brain.

Engineering coronavirus spike proteins for human experimentation and vaccine development

Naturally occurring coronaviruses were first identified in the mid-1960s. They are named after the crown-like spikes on their surface. These viruses are prevalent in animals; however, four coronaviruses are known to infect humans, including 229E, NL63, OC43, HKU1. All of these strains cause mild, cold-like symptoms in humans.

In the twenty-first century, scientists have been studying and engineering the coronavirus spike protein. Scientists can splice genes into the coronavirus spike protein, allowing natural selection to rapidly mutate the spike protein in the lab, one gene at a time. This serial passage technique hides any trace of human interference, but the advanced attachment properties of the resulting virus are a dead give-way that the virus was manipulated in a lab. This controversial gain-of-function research was banned in the US in 2004 but continued to take place in the US and abroad — as long as the research was conducted to invent new vaccines. Today, new experimental vaccines are being unleashed, as the outbreaks occur in real time.

Since coronavirus gain-of-function research began, three new coronaviruses have emerged, causing severe illness in humans. SARS-CoV-1 was first identified in China in 2003; MERS-CoV was first identified in Saudi Arabia in 2012; and today’s SARS-CoV-2, was first identified in Wuhan, nearby the Wuhan Institute of Virology in China.

Beijing researchers affiliated with the Academy of Military Medical Science published a study in June 2020, explaining the methods they used to modify coronavirus spike proteins to exploit human lung cells. The researchers equipped mice with the ACE2 receptor from human lung cells. By exploiting the ACE2 receptor, the spike protein is engineered to attack the brain and lungs of humans. The damage of this laboratory-leak vaccine experiment will only continue as new vaccine experiments go live on the population, translating spike proteins in human cells and attacking human brains into the unforeseeable future.

 

AcuteShield Vanquish® ingredients inhibit mRNA Spike Proteins from attaching to body organ cells (heart, brain, lungs, kidneys, liver, ovaries, etc.), some can cross the blood brain barrier to protect the brain and central nervous system, and some can penetrate cell membranes to inhibit spike protein replication. https://acuteshield.com

 

Citation

(Johnson, 2021). News Target: Spike proteins administered intravenously are engineered to cross the blood-brain barrier, can cause cerebral hemorrhage. Retrieved on 12/11/22 online from https://newstarget.com/2021-06-03-spike-proteins-engineered-to-cross-blood-brain-barrier.html


 

ALL THINGS COVID AND mRNA VACCINES

Our bodies are made up of approximately 30 trillion cells. COVID and mRNA Vaccine Spike Proteins attach to body organ cells, penetrate cell membranes, and replicate inside your cells causing cell damage and inflammation, resulting in side effects and long-term disease.

Learn what goes on in your body when you get COVID or are vaccinated so you can optimize your immune system to protect your body organ cells.

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