Debunking JOWMA's Latest Brazenly False Ad About Covid and Children, Part 2

The Astounding Illiteracy and Ignorance of this Propaganda Sheet

This is a sort of “rapid response”, not an in-depth thorough analysis of every point.

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The lies disseminated about the vaccine in truth require a series of articles to debunk them properly, which is not possible for this article. So here is a short introduction on the background science in order to give over a basic sense about the nature of these vaccines.

The following is a very condensed and rough explanation of the basics: The 3 approved vaccines in the US utilize a genetic therapy mechanism - utilization of the cell’s own “machinery” to translate genetic material into proteins - to produce the full spike protein of the covid virion. The spike protein is a tiny piece that is attached to the outside of the “ball” that is the covid virion, whose primary function is to bind with a surface protein on human cells (called ACE2), which initiates a chain of chemical reactions that ultimately culminates in the fusion of the covid virion with the cell membrane. This results in the release of the covid RNA into the cell along with a few helper ‘pieces’ (non-structural proteins, or NSP’s) to ‘load’ the RNA into the cell’s protein-manufacturing hardware (ribosomes), kind of like hacking the ‘software’ of the cell, so the cell will produce the components of the covid virion instead of regular human proteins. This is how the virus replicates. (For the record, there are other ways besides ACE2 by which covid can “break into” a cell, but ACE2 is the main one.)

The thinking behind the selection of the spike protein for the vaccines was that by producing antibodies against the spike, the spike protein would be unable to function, so the covid virions will then be unable to break into cells and replicate, and the covid infection would thus sputter out pretty quickly.

Unfortunately, it was eventually discovered in the intervening months that the spike protein itself is a highly toxic protein that causes all sorts of damage to cells by itself (and is the primary driver of much of the damage covid inflicts on the human body). Here are a few of the studies on spike protein toxicity (I’m only including here studies off the top of my head that clearly describe spike toxicity in their title):

• The spike protein of SARS-CoV-2 induces endothelial inflammation through integrin α5β1 and NF-κB | bioRxiv

• The S1 protein of SARS-CoV-2 crosses the blood–brain barrier in mice | Nature Neuroscience

• SARS-CoV-2 Spike Protein Impairs Endothelial Function via Downregulation of ACE 2 | Circulation Research

• The SARS-CoV-2 spike protein alters blood brain barrier

• Exaggerated cytokine production in human peripheral blood mononuclear cells by recombinant SARS-CoV-2 spike glycoprotein S1 and its inhibition by dexamethasone | bioRxiv

• Be aware of SARS-CoV-2 spike protein: There is more than meets the eye - PubMed

• SARS-CoV-2 direct cardiac damage through spike-mediated cardiomyocyte fusion | Research Square

• SARS-CoV-2 Spike Protein Elicits Cell Signaling in Human Host Cells: Implications for Possible Consequences of COVID-19 Vaccines

The vaccines were designed before this was known, so this is not an indication of a deliberate choice to maliciously use a toxic protein. But the fact remains that this is what the vaccines are producing in the human body, a biologically active protein with potent toxicity.

It cannot be emphasized enough that the point of vaccines over actual infection is to substitute a dead or inactive version of the virus instead of the live one, so you can get the immunity benefits of exposure without having to face the danger of the virus itself. Using a live version of the most toxic part of a virus is about as clear a violation of this cardinal rule as you can get, regardless of what the clinical outcome data ultimately show.

Another potentially hazardous piece of the vaccines, although this is only in the mRNA vaccines, are the lipid nanoparticles (LNP’s) used as the “delivery vehicle” to get the mRNA into human cells. A proper review of potential lipid toxicities is beyond the scope of this article, but suffice it to say that the lipids were never subjected to proper testing for toxicities and distribution within the human body (among other things).

There is much, much more to say even by way of introduction, but this will have to suffice.

Onto the rebuttal:

Firstly, such a low number of subjects cannot reliably pick up a side effect that happens even 1/1000. If the vaccine literally would kill 1/1000 kids the next day, there’s roughly a 22% that this wouldn’t be manifest in this sample size.

The “91% efficacy” is baloney. And even if it was true (which it’s not, because the study was run corruptly, which is a subject for another article), what that means is 91% less than the already negligible risk of symptomatic covid to kids. To quote one analyst, reducing the risk of getting eaten by a shark in Idaho by 95% isn’t worth anything.

Antibody titers have not been actually correlated to clinical outcomes. The backbone of the immune system’s response to viral infection isn’t constantly circulating humoral antibodies, it’s the T-Cells and B-Cells. In any event, the vaccines exert quite the detrimental effect on your immune system, especially if you already had covid:

• DECREASED BREADTH OF THE ANTIBODY RESPONSE TO THE SPIKE PROTEIN OF SARS-CoV-2 AFTER VACCINATION | medRxiv

• N antibody levels appear to be lower in individuals who acquire infection following 2 doses of vaccination

• The BNT162b2 mRNA vaccine against SARS-CoV-2 reprograms both adaptive and innate immune responses | medRxiv

• Differential effects of the second SARS-CoV-2 mRNA vaccine dose on T cell immunity in naïve and COVID-19 recovered individuals

  • “While robust spike-specific antibodies and T cells are induced by a single dose vaccination in SARS-CoV-2 seropositive individuals [3, 4], the second vaccination dose appears to exert a detrimental effect in the overall magnitude of the spike-specific humoral response in COVID-19 recovered individuals [5].”

The horrific impact of the vaccines on your immune system also requires its own article to address properly.

Regardless, there is literally no established clinical benefit whatsoever to healthy children from the vaccines, even if there would be no side effects whatsoever, because the vaccines to not add anything to children’s immunity that is necessary to fight off covid. Children do not need more antibodies to protect them from what is at worst generally a really bad cold so that it is reduced to a more mild cold.

Let’s be blunt: the “routine” side effect profile of the vaccine is by itself already worse than covid would be for children, and more common by orders of magnitude:

Let that sink in. Covid infection doesn’t manifest with anywhere near this level of symptomatic presentation or ferocity.

You know one way to make it so there are no severe adverse events? Lie about them and claim they didn’t happen even if they did. Yes, you’re reading that correctly: Pfizer and the FDA lied about a horrific Adverse Event in the Kids Trial and pretended it didn’t happen.

In the Pfizer kids trial for adolescents, one of the subjects, a perfectly healthy then-12-year-old named Maddie De Garay, suffered what can only be described as an inhuman ordeal of physical suffering and permanent disabilities. In the words of her mother:

My 12 year old daughter was a healthy 7th grader with no major medical issues other than dermatographia and ADHD which she was taking vyvanse to manage.  She participated in the Pfizer vaccine trial for 12-15 year old’s at our Children’s Hospital.  She received her first dose in the trial on 12/30/20.  The next day she had a fever of 101, felt tired and had swelling at the injection site but all of these resolved within a couple days.  She received her second dose on 1/20/21.  She had immediate pain at the injection site which didn’t happen with the first dose.  About 18 hours after receiving the vaccine, she developed the following: severe muscle/nerve pain, painful electrical shocks down her neck and spine which caused her to walk hunched over, severe chest pain that felt like her heart was being pulled out, numbness and swelling in her vaccine arm (left), her fingers and toes turned white and were ice cold to the touch,  the pain in her toes was so bad she walked on her heels, severe abdominal pain (especially on lower right side) and a fever of 101.4.   We were instructed to take her to the ER at our Children’s Hospital where they did an ultrasound to check for appendicitis.  The results showed there wasn’t any sign of appendicitis even though the appendix could not be visualized or the right kidney, her bladder appeared normal and a note that there was a diffuse gaseous filled bowel seen throughout the right lower quadrant.  They did a renal profile  that showed her potassium was slightly low (32) and her glucose was slightly high (110), they did not do any other blood tests. Her urine test showed a moderate amount of blood in her urine.  She was given an IV, tylenol and zofran, then sent home.

Over the next 2.5 months her severe abdominal pain along with the muscle and nerve pain persisted plus she new symptoms including: fatigue, nausea, vomiting, abdominal distension, regurgitation of food and eventually the inability to swallow food or liquids,  itchy rash on her arms, peeling skin on her feet, unexplained painful cysts on her vagina and then head, tinnitus, vision problems, headaches, dizziness, erratic blood pressure and heart rate, memory loss, brain fog, verbal and motor tics, fainting/seizures (10+ a day), loss of feeling from the waist down then paralysis of her legs, inability to walk, muscle weakness, abnormal gait, gastroparesis, urinary retention, anxiety, and medical PTSD..  Additionally she started her first menstrual cycle on 2/5/21 which continued off and on for over a month with clumps of blood and then off and on spotting until 4/13/21 and nothing since then.  Between 1/21/21 and 4/9/21 we had to take her to the ER nine (9) times and she was admitted to the hospital 3 times.  In between hospital visits she has seen multiple specialists at the Hospital and had Physical Therapy and Cognitive Behavioral Therapy with no improvement, instead she continued to decline.

After several desperate calls to multiple doctors expressing our concern for her declining health and more ER trips we finally got help from our new Care Coordinator to have neurology guarantee she would be admitted if we went to the ER on 4/9/21.  When she got to the ER on 4/9/21 she could not walk, was unable to feel or move below her waist,  had tachycardia and her blood sugar was at 47. Once she was stable they admitted her to neurology and then transferred her to Inpatient Rehabilitation on 4/13/21.   As of today, 5/24/21, she is finally close to being able to walk without a walker but she still has an abnormal gait.   She also still has an NG tube for nutrition and continued problems with urination and gastroparesis, not to mention the PTSD from this experience with doctors, especially in the ER and Pfizer Vaccine Trial, doubting her and treating her like a mental patient.  Right now every Wednesday and Friday, she has to meet specific PT goals.  If she is unable to reach these goals, she will be discharged to follow-up outpatient primarily with Pain, GI, Adolescent, and psychology. If she is to be discharged, outpatient will focus much more on mental health.  NOTE: the words in italics are directly from her medical chart.

My daughter has gone from being a typical healthy 12 year old girl who worried about doing well in school and loved hanging out with friends to being so ill she had to miss 4 months of school.  She has been in the hospital for almost 2 months total where she celebrated her 13th birthday.  She is the strongest person I know and I am so proud of her for pushing through this nightmare and never giving up.  There is no doubt in my mind that the vaccine caused this.  All of these medical problems started less than 24 hours after the second dose of the Pfizer covid vaccine and did not just go away within 72 hours like they say.  She was not forced to do the vaccine trial, she asked to do it along with her 2 brothers so she could help get our world back to normal.  The only diagnosis we have been given is Functional Neurological Symptom Disorder with mixed presentation, acute episode in which the vaccine was likely the trigger, no explanation as to why the vaccine triggered it. They have dismissed her having repetitive abnormal blood work and that she has had blood in her urine countless times over the past 4 months, even with a catheter.  

Once she was given the Functional Neurological Disorder diagnosis they stopped any further testing that could and should have been done and any new doctors already had a bias from reading her medical record.  She is not even close to being functional and that is with over a month of top-notch inpatient rehabilitation which has included PT/OT/Recreational Therapy/Music Therapy, Speech Therapy and Cognitive Behavioral Therapy.  We have a family meeting today to discuss her discharge on Friday, May 28th.  We are desperate to get her treatment that will help her get back to the healthy 12 (now 13) year old girl she was before she got the Pfizer vaccine.  I was told her case was included in Pfizer’s final report on the trial for 12-15 year old children but they did not share the end diagnosis and all of her symptoms.  They summed it up as functional abdominal pain with ongoing investigation, it was MUCH more than that!  We do not want this to happen to more innocent people, especially children!

You can watch the heartwrenching video of her mother describing what happened here (tznius warning for those for whom it is relevant).

Even if there weren’t any severe adverse events in the kiddie trial, it doesn’t prove anything, because the trial didn’t have enough subjects to detect rare events, plus they excluded all cohorts most likely to suffer serious adverse events (notably kids who already had covid).

Furthermore, the fact of the myocarditis that even the medical establishment has been forced to admit to somehow wasn’t detected in the trials (or maybe it was…).

Response to this:

1. maybe true technically, but a kid is far, far more likely to get “symptomatic vaccine ‘covid’ ” then symptomatic covid if the kid remained unvaccinated.

2. “May prevent”??? This is stupid rubbish. They don’t even have pretend data for this claim. And the vaccine itself likely causes both in a yet-determined % of recipients. See above and Part 1.

3. These vaccines do not inhibit transmission whatsoever, and in fact increase transmission (going by the higher case rates in more vaxxed jurisdictions compared to lesser vaxxed ones & the PHE datasets that show sharp negative efficacy after 5-6 months). This in addition to the fact that kids are not significant spreaders of covid.

4. This is probably true, because of the vile government policies that are perfectly comfortable with institutionalizing child abuse in the form of facemasks, lockdowns, etc.

This cannot be emphasized enough: There are no clinical benefits to vaccinating healthy children. Period.

Interesting claim, considering that these were all deliberately excluded from the vaccine trial, so there’s no data on them. And Dr, Nemetzky doesn’t even have the basic humility to acknowledge this See above.

I hope to produce a vaccine fact sheet in the mold of this nonsensical propaganda, but that actually has, you know, facts.

In the meantime, is it really too much to ask that you leave the kids alone???