Why COVID Shots Are Disproportionately Affecting Young Males= Translated:
TaKe the Vaccine and DIE!!!
Alarming Increase in Mortality Rates in 2021: Why COVID Shots Are Disproportionately Affecting Young Males (For Now)
Florian Dagoury
Shortly
after receiving his 2nd dose of
the Pfizer COVID vaccine earlier this year, professional diver Florian Dagoury,
who is among the world's leading record-holders in static apnea (holding one's
breath under water), noticed strange changes in his resting heart rate and
breathing capacities. Four
weeks later, after visiting a cardiologist he received a diagnosis of
myocarditis and trivial mitral regurgitation. With no previous history of
cardiovascular illness, he concluded that these effects were produced by the
Pfizer vaccine.
Professional mountain-biker Kyle Warner was also recently diagnosed with
pericarditis, along with postural orthostatic tachycardia syndrome, which both
began shortly after receiving his Pfizer shot. Kyle has shared his experience
on his YouTube
channel, and also participated on a roundtable discussion at the US
senate on vaccine reactions in early November.
Former West Ham United soccer player Pedro Obiang
was hospitalized for 10-15 days shortly after receiving his COVID vaccine in
July. The 29-year old was also told that he had myocarditis and, as a result,
was unable to engage in any sporting activities for at least 6 months.
Likewise, the 2016 Olympic gold medal cyclist Greg Van Avermaet was forced to quit this year's world championship
after suffering injury from the Pfizer vaccine in June.
© Cyclingtips.com
Olympic gold medal cyclist Greg Van Avermaet
This is a
small fraction of the total number of high-profile athletes who have suddenly
been afflicted with cardiovascular disease in 2021 so far. Since myocarditis is
an extremely dangerous condition of the heart with the potential to cause
permanent damage, this may mean that these athletes never return to
professional sporting activity again.
Additionally, there is a
long list of other young athletes who were not as fortunate, and have
mysteriously or unexpectedly passed away this year:
· Benjamin Taft (German footballer), aged 33, collapses after game, dies of heart attack.
· Luis Ojeda (Argentinian footballer), aged 20, player unexpectedly passes away.
· David Jenkins (Olympic silver medal diver and British coach), aged 31, passes away unexpectedly, cause of death currently unknown.
· Giuseppe Perrino (ex-professional footballer), aged 29, dies of heart attack during match.
· Avi Barot (cricket player), aged 29, suffers cardiac arrest and later dies.
· Jens De Smet (footballer), aged 27, collapses on pitch and passes away of heart attack.
The above
account for just a few examples of sudden cardiac
injury, death, or death of unknown causes experienced by young male
athletes in 2021. These occurrences and media reports are being tracked more
comprehensively on several different websites. One German list amasses over 75
accounts of
similar events since June 2021, while another list, published in Hebrew, documents a staggering 183 events since December 2020. The overwhelming
majority occurred in males, including over 100 deaths.
An Israeli media report (translated into English by americasfrontlinedoctors.org) documents a 500% increase in
sudden cardiac/unexplained deaths among FIFA athletes in 2021 compared with the previous year.
Indeed, it is well known that sudden death among athletes is higher than the
average population. Research suggests that athletic performance at the
semi-professional/professional level poses a 2.4-4.5 increased risk of sudden cardiac arrest/death
relative to non-athletes. Additionally, males are more greatly
affected, where there is approximately three to five
times higher risk of developing sudden cardiac death compared with
their female counterparts. Myocarditis is just one of the underlying causes,
and is thought to account for 4-9% of cardiac events among athletes. Data on
the total numbers of cardiac injury in athletes across the world is difficult
to obtain, although sudden cardiac death is estimated to occur in
one per 40,000-200,000 athletes.
At this point, there is insufficient evidence to
claim that all or even most of these tragic events in 2021 were caused by one
or other of the COVID vaccines. [BULLSHIT] But we have reasonable
grounds for asking whether it is possible that the mass-vaccination campaigns
are responsible for a significant portion of these sudden events among this age
group.
Furthermore, given that cardiac events are likely just one set of injuries, it
is reasonable to wonder whether COVID vaccines are having a similarly
destructive effect [DEATH YOU MEDIA LACKIE]
on the health of young people in general.
Disturbing trends in mortality after
mass-vaccination
In a paper titled 'Expert evaluation on adverse effects of the
Pfizer-COVID-19 vaccination' published in May 2021, Dr. Herve
Seligman warned that mass-vaccination would result in a significant number of
serious adverse events and deaths, and that this would disproportionately
affect the young. He
demonstrated greater COVID mortality rates in the vaccinated vs
unvaccinated, and further analyses showed that for ages 20-90, vaccination
mortality was inversely proportional to age. He
explains:
"The stronger the immune system, the less likely one is to develop COVID19-induced symptoms. Hence, the elderly are more affected than young adults, men more than women, and people with pre-existing conditions, obese included, than the physically fit. Vaccine adverse reactions tend to behave the opposite way. They are proportional to the strength of the immune system, as many adverse effects associated to vaccines are immune system overreactions. These are more prevalent in younger adults and in women, the opposite demographic picture than for COVID19."
Evidence
made available since then has proven Dr Seligman's warning to be accurate. Not
only does the vaccine NOT protect against dying from COVID, it actually appears
to increase
the risk of death. Analysis by Matthew Crawford on mortality
rates in thirteen countries before and after implementing mass-vaccination
campaigns showed a
staggering 11.6 times increase in COVID deaths post-vaccination.
The rate of deaths due to 'abnormal clinical findings' in the US maintained a
steady average until approximately March/April 2021. Suddenly
deaths began to spike and continued to increase well
into September. This increase closely correlated with the weekly
doses that were administered.
Furthermore,
deaths began to climb at around the same time as the FDA approved 'emergency
use authorization' of the Pfizer vaccine for adolescents aged 12-15.
© CDC.gov
Young adult and adolescent deaths
increasing
A report looking at excess mortality
statistics in young adults was published by Dr Steve Ohana and Dr Alexandra
Henrion-Caude. It showed
that excess deaths in adults under the ages of 50 were higher in countries
which employed mass vaccination campaigns (UK, Israel, and Hungary) compared
with other countries that did not. The greatest increase was shown for ages
20-29.
Mortality growth in % from Jan-May 2020 to Jan-May 2021 in Israel, England & Wales, Hungary and 23 other European countries which have more moderately vaccinated their populations, for ages 20-29, 30-39 and 40-49.
According to the authors:
"it appears that the difference between mass and moderate vaccination is significant in terms of mortality growth in young age groups, and that mass vaccination is associated to a higher young adults' mortality growth."
More data
coming out of Israel demonstrated a similar
increase in all-cause mortality between February-May 2021 among
20-29 year olds:
© https://swprs.org/covid-vaccines-deaths/
Furthermore, research published by Israeli Professor Retzef Levi showed massive increases in cardiac arrests in adults aged 20-49 between Jan 1st-May 31st 2021 compared with the previous two years.
There was also much higher incidence of acute coronary syndromes in both males and females between 16-49 years old. As can be seen from the table below, the youngest age group (age 16-19) saw the greatest percent increase for both sexes, followed by the second youngest age group (age 20-29).
Beginning between weeks 20-30 of 2021, a sudden rise in excess mortality
occurred for Europeans aged 15-44, and Americans aged 24-44:
Furthermore,
all-cause excess mortality in the US for under-24s has also been steadily
increasing since April of this year:
© CDC.gov
Cumulative all-cause excess mortality
in the US - Ages 0-24
Vaccination reactions disproportionately affect
young adults and adolescents
According to VigiAccess,
the World Health Organization's database for documenting adverse events to
medications, there have been over 2.4 million reports of adverse reactions to
COVID vaccines since the rollout. Currently,
42% of those occur in people under the age of 44, whilst only 6% occur in ages
75 and over.
One of
the most serious adverse events is myocarditis, a condition involving acute
injury to cardiac myocytes, which in turn activates the immune system,
resulting in severe inflammation. In some cases, persistent inflammation leads
to ongoing muscle cell damage, heart failure, and death. Pericarditis is
another documented side effect, similarly involving inflammation of the
pericardium, which is the membrane encapsulating the heart.
Data compiled from the Vaccine Adverse Events Reporting System (VAERS) in one
study clearly shows that the occurrence of vaccine-induced
myocarditis is inversely proportional to age. As can be seen below, a staggering proportion of these
events occur in children, adolescents and young adults. This is unlike
pericarditis, which affects a much wider demographic.
Reported post-COVID-19 vaccine myocarditis (a) and pericarditis (b) adverse events by age group and vaccine type. The x-axis shows the number of myocarditis side events after receiving COVID-19 vaccine. The y-axis shows the age groups of vaccine recipients. The bars were colored according to the vaccine received. VAERS reports were processed as of 2 September 2021.
Vaccination reactions
disproportionately affect young males
A further examination of
the data shows that the overwhelming majority of post-vaccination myocarditis
and pericarditis is found in males. Furthermore, there is a much greater
likelihood of developing this effect after receiving the second dose of
mRNA-type vaccines.
The number of post-COVID-19 myocarditis and pericarditis adverse events by sex (a) and the administered vaccine dose (b). The x-axes show the adverse event counts for each COVID-19 vaccine shown on the y-axes. Considering VAERS reports processed as of 2 September 2021
And although apologists for Big Pharma at the New York Times and elsewhere are consistently
trying to downplay this condition as "mild and temporary", there are serious
justifiable concerns over the long-term health effects that this may have:
Young male mortality on the rise
Unsurprisingly, ever since the vaccine rollout for younger adults and
adolescents, several countries have witnessed a disturbing rise in excess
mortality amongst young males. In
Austria, a massive increase in excess
mortality for 2021 has been found in young men aged 15 and above. Compared with the previous year,
deaths are up 32% for ages 15-24 and 21% for ages 25-34. A less
drastic increase was also demonstrated in males aged 35-44.
© Report24.news
These deaths cannot be attributed
to COVID, because the mortality rate among females has shown the exact opposite
trend, with fewer deaths being reported for all ages.
England and Wales have also witnessed a similar trend among male children aged
10-14. The
Exposé compiled official ONS data
which reveals that since
the rollout of the COVID vaccine for children aged 12+, there has been an 86%
rise of deaths in males compared with 2020. Astoundingly, week 40 saw a 600%
increase, followed by week 41 which showed a equally disturbing 200% increase.
© Office for National Statistics
UK
Deaths of male children 2020-2021
Another investigation by The Exposé looked at
deaths among teens aged 15-19 since the beginning of vaccine administration for
this age group. It showed a staggering 63% increase for males, along with 16%
for females. Remarkably,
the third week of June found a 500% increase in male deaths, along with 700% in
the week ending September 3rd.
In contrast, the same period only found a 17% increase among female deaths:
© The Expose
At this
point, the data is quite clear that something is killing children, adolescents,
and young adults at a much higher rate than before mass-vaccination campaigns
were introduced. The data also shows that males are being disproportionately
affected by vaccine injury, and this is reflected in the available mortality
statistics.
In order to attempt to make sense of these findings and understand why this is
happening, we first need to examine the underlying mechanisms behind how the
vaccines inflict such damage.
Mechanisms of vaccine injury and death
The overwhelming majority of vaccine reactions have been documented after
administration of the mRNA-based formulations (Pfizer and Moderna). However, a
significant portion also occur with adenoviral DNA vector vaccines (J&J and
AstraZeneca). It's worth noting that all of these 'vaccines' share important
similarities which will eventually help to explain the severity and frequency
of adverse events:
· Each of the above vaccines are based on novel technology which is different from traditional inactivated viral vaccines
· Each of the above vaccines are designed to instruct human cells to synthesize foreign SARS-CoV-2 spike protein (which I will refer to as SPIKE)
To give a
brief overview of the mechanism of action in these types of technology:
The adenoviral DNA vector vaccines contain DNA which codes for SPIKE encased
within a non-replicating virus (a chimpanzee adenovirus). After injection, the
viral vector penetrates the cell, enters the nucleus and yields messenger RNA
(genetic instructions for protein synthesis). This mRNA is then used as a
template by our own cellular machinery to start synthesising spike protein.
SPIKE fragments then migrate to the surface of the cell, where they are later
identified as foreign by the adaptive immune system, which begins generating
protective antibodies against this protein. The aim is to provide future immunological
memory through antibody formation against any virus which also expresses SPIKE.
On the other hand, mRNA based 'vaccines' do not use an adenovirus vector, but
instead encapsulate modified mRNA within a lipid nanoparticle emulsion
containing polyethylene glycol, and this functions to facilitate mRNA delivery
into the cell. In a roundabout similar way to the adenovirus DNA vector, the
newly-delivered mRNA provides the necessary instructions for the cell to begin
synthesising copious amounts of foreign SPIKE, which then migrate to the cell
surface and initiate an adaptive immune response. Once again, this is with the
aim of enhancing long-term antibody production against any future viral threat.
© Martínez-Flores, D. et al. (2021) "SARS-CoV-2 Vaccines Based on the Spike Glycoprotein and Implications of New Viral Variants", Frontiers in Immunology, 12. doi: 10.3389/fimmu.2021.701501.
Each of
the above vaccines are injected into the arm, the contents of which were
originally assumed to stay within the deltoid muscle and perhaps the local lymph
nodes whilst evoking antibody production. Researchers believed that SPIKE
protein did not enter into systemic circulation. However, more recent evidence
showed the exact opposite
to be true, demonstrating measurable levels of SPIKE in the blood of mRNA
vaccine recipients.
In fact, another pharmacokinetic study in Japan using Pfizer's
vaccine technology showed mRNA-containing lipid nanoparticles in practically every
organ, including the brain, heart, liver, adrenal glands, kidneys, intestine,
sex organs, and spleen, where they stayed for much longer than was originally
expected. This means that
SPIKE is literally being expressed in tissues all throughout the body, in much
higher levels than would ever be present in viral infection, and it sticks
around.
Why is this relevant? SPIKE protein was originally considered to be a perfect
antigen because of its supposed lack of ability to cause harm to host tissues.
According to the CDC, modified SPIKE protein is a "harmless antigen".
But the bulk of evidence
now shows that, far from being a "harmless antigen", SPIKE is in fact
an extremely toxic molecule capable of initiating severe, systemic
inflammation. Ongoing exposure to this poison might help to explain most, if
not all, of the vaccine adverse events and deaths.
Toxicity of SPIKE protein
Upon contact with cells, SPIKE has a very high affinity for angiotensin
converting enzyme (ACE2) receptors, ubiquitously expressed on the surface of
numerous cell types located in the lung, brain, blood vessels, heart, and many
other organs. In COVID-19 infection, ACE2 receptor binding is considered to be
the primary mechanism of viral entry into the cell. After binding, ACE2 is
internalized and degraded, which causes a loss of receptor function.
Ordinarily, ACE2 is involved in systemic regulation of the cardiovascular
system and serves as an important regulator of renin-angiotensin system (RAS).
A large number of studies have demonstrated
anti-inflammatory, antioxidant, anti-apoptotic and anti-fibrotic properties of
ACE2 receptor function, and it is considered highly protective against cardiovascular
injury of all sorts, including myocarditis.
González-Rayas, J. et al. (2020) "COVID-19 and ACE -inhibitors and angiotensin receptor blockers-: The need to differentiate between early infection and acute lung injury", Revista Colombiana de Cardiología, 27(3), pp. 129-131. doi: 10.1016/j.rccar.2020.04.005.
ACE2 receptor binding not
only disables/blocks its ordinary function, but initiates cell signalling
cascades which stimulate pro-inflammatory
gene expression and
trigger the inflammatory response. SPIKE protein alone is capable of causing
widespread vascular
inflammation.
© Suzuki, Y. and Gychka, S. (2021) "SARS-CoV-2 Spike Protein Elicits Cell Signaling in Human Host Cells: Implications for Possible Consequences of COVID-19 Vaccines", Vaccines, 9(1), p. 36. doi: 10.3390/vaccines9010036.
Any tissue or cell which
expresses ACE2 receptors is therefore extremely vulnerable to the effects of
this protein. In endothelial cells lining the
blood vessels, SPIKE triggers an inflammatory cascade resulting in vascular endothelial dysfunction, impaired nitric oxide bioavailability which
reduces the capacity for vasodilation, and induces vasculitis. SPIKE was
recently shown to increase vascular endothelial permeability
through disrupting tight junction barrier proteins, and this effect is thought
to further increase damage to the cardiovascular system and systemic
inflammation. Activation of the
complement pathway and
other inflammatory mediators triggers a systemic procoagulant state. SPIKE
binding with ACE2
on platelets was shown to cause dose-dependent platelet aggregation,
potentially leading to lethal thrombosis (blood-clotting).
Microangiopathy (disease of the small blood vessels) is not limited to the
pulmonary capillaries but can occur throughout the entire vascular system and
affect every organ including the brain, liver, and heart.
© Angeli, F. et al. (2021)
"SARS-CoV-2 vaccines: Lights and shadows", European Journal of
Internal Medicine, 88, pp. 1-8. doi: 10.1016/j.ejim.2021.04.019
Schematic mechanism of action of mRNA
and adenoviral vector DNA vaccines and their potential cardiovascular
interactions throughout the activation of the immune system and the interaction
between free-floating Spike proteins and ACE2
Even
short-term exposure to spike protein was shown to produce long-term changes in gene expression which facilitates
chronic inflammation. SPIKE
was also shown to contain a superantigenic region
capable of activating T-cells, resulting in massive production of
proinflammatory cytokines including IFNγ, TNFα, and IL-2.
This systemic
"hyperinflammatory" cytokine storm response is responsible for
multi-organ tissue damage. This protein was recently shown to literally strip the lipids
away from cell membranes in the absence of ACE2 receptors, demonstrating a
direct destructive effect of SPIKE on cell membranes.
SPIKE not only binds with
ACE2, but has been shown to enhance systemic inflammation through
binding Toll-like receptor
4 (TLR4).
TLR4 detects pathogen-associated molecular patterns such as bacterial
lipopolysaccharide and, like other TLRs, is responsible for modulating the
innate immune response. TLR4 can drive hyperinflammation through activating
proinflammatory transcription factors such as NF-Kappa Beta. A recent animal study demonstrated increased
generation of proinflammatory cytokines, cardiac hypertrophy (enlarged heart),
and decreased cardiac systolic function in mice treated with SPIKE, and the
authors conclude that TLR4 activation might be one of the driving mechanisms
behind cardiac injury.
SPIKE was recently shown to bind with integrin proteins in the lung, and Neuropilin-1, a transmembrane protein in the
brain involved in neuronal development and axonal growth. The effects of this
are not yet known.
SPIKE also has high affinity for monoamine oxidases, equal to its affinity for
ACE2. MAOs (A and B) are a class of enzyme intrinsically involved in the
regulation of neurochemicals. These function to metabolize (break down) amine
neurotransmitters such as dopamine, serotonin, noadrenaline, and
phenylethylamine. Functional abnormalities in MAO have been associated with
behavioural/neuropsychiatric disorders and some neurodegenerative conditions. SPIKE-MAO complex
formation was shown to
significantly reduce enzyme activity by lowering enzyme affinity toward its
substrate neurotransmitters. This is expected to lead to an excess of amine
neurotransmitters which is likely to significantly alter overall neurochemical
balance and mood/cognition/brain function.
Another major point of concern is the theoretical ability of SPIKE to trigger
autoimmunity. Vaccine-induced autoimmunity has been demonstrated
for several other conditions. This is thought to occur through cross-reactivity
between foreign vaccine-derived antigens with host proteins.
© Vojdani, A., Vojdani, E. and Kharrazian, D. (2021) "Reaction of Human Monoclonal Antibodies to SARS-CoV-2 Proteins With Tissue Antigens: Implications for Autoimmune Diseases", Frontiers in Immunology, 11. doi: 10.3389/fimmu.2020.617089.
A
simplified overview of how this might work follows: The adaptive immune system
functions as a pattern-recognition system. It possesses a complex set of tools
designed to identify patterns which it associates with pathogenic infection
(pathogen-associated molecular patterns). The immune system has memory and can
"remember" the specific sequence of amino acids or
"pattern" of the antigen, and in some cases, sequence homology exists
with host proteins (referred to as "molecular mimicry"). This means
that the molecular pattern associated with the pathogen/foreign antigen shares
structural similarities with certain proteins of the host's own body. In this
case, antibodies against the pathogen (or food, or any other kind of antigen)
can also be cross-reactive with self and drive autoimmune destruction of our
own tissues.
Khavinson and colleagues found
significant sequence homology between SPIKE and a variety of human proteins:
© Khavinson, V. et al. (2021) "Homology between SARS CoV-2 and human proteins", Scientific Reports, 11(1). doi: 10.1038/s41598-021-96233-7.
To make matters worse, cross-reactivity of SPIKE antibodies with human tissue proteins was confirmed on two occasions here and here , highlighting the potential for developing multi-system autoimmunity:
These host tissue antigens included:
· Transglutaminase 2 & 3 - proteins responsible for tissue repair, antibodies associated with Coeliac, IBD and arthritis
· ENA - proteins found in the cell nucleus, antibodies associated with SLE & non-specific systemic autoimmunity
· Myelin basic protein (MBP) - a protein involved in the myelination of nerves, antibodies associated with Multiple sclerosis
· Mitochondria - the source of ATP production inside the cell
· Nuclear antigen (NA)
· α-Myosin - A functional protein of the cardiac muscle. Antibodies are implicated in myocarditis and other cardiac diseases
· Thyroid peroxidase (TPO) - Enzyme located within the thyroid gland, associated with Hashimoto's thyroiditis.
· Collagen - most abundant structural protein in the body
· Claudin 5+6 - protein responsible for maintaining epithelial barrier integrity, antibodies associated with leaky barrier
· S100B - protein involved in brain function
The authors of that paper warned:
"There are reasons for all the precautions involved in developing a vaccine, not the least of which are unwanted side-effects. In light of the information discussed above about the cross-reactivity of the SARS-CoV-2 proteins with human tissues and the possibility of either inducing autoimmunity, exacerbating already unhealthy conditions, or otherwise resulting in unforeseen consequences, it would only be prudent to do more extensive research regarding the autoimmune-inducing capacity of the SARS-CoV-2 antigens. The promotion and implementation of such an aggressive "immune passport" program worldwide in the absence of thorough and meticulous safety studies may exact a monumental cost on humanity in the form of another epidemic, this time a rising tide of increased autoimmune diseases and the years of suffering that come with them."
Finally,
another animal study found that SPIKE-induced pathogenic
auto-antibodies resulted
in autoimmune attacks on numerous organs, haemorrhaging, and yielded
spontaneous abortion, neonatal death and stillbirth through what its authors
referred to as "Antibody Dependent Auto-Attack".
To summarize, vaccination provides the host with genetic instructions to
synthesize copious amounts of an extremely toxic protein, which makes its way
into circulation and has been found in practically every organ. SPIKE is a highly inflammatory molecule
capable of triggering systemic inflammation and dysfunction of the blood
vessels, inflicting damage to multiple organs, which also has a high potential
for initiating the development of organ-specific autoimmunity.
Without detailing the mechanism of each and every side-effect, it is fairly
clear at this point why vaccination is associated with so many serious adverse
events.
Why are vaccine adverse events and deaths
more common in young people?
The very qualities which
provide children, adolescents, and young adults with robust immune protection
against COVID-19 (and other infectious disease) are unfortunately the same
qualities which render them exponentially more susceptible to experiencing
severe adverse events and death from vaccination.
Recall that individuals over the age of 65 accounted for just 15% of the COVID
vaccine adverse events, yet account for at least 76% of COVID deaths across the
US, according to recent CDC estimates (although that percentage is likely much
higher). This can at least partly be explained by immunosenescence,
which is a natural consequence of aging. The ability to mount
cell-mediated defenses against new infections begins to wane due to decreased
availability of naïve T-cells. Additionally, plasma B cells with lower antigen specificity mean
that the elderly are also less able to generate protective antibodies against
new infections. Aging is associated with low-level, chronic inflammation,
but with less flexibility and immune-reactivity to new oncoming threats. Hence,
the elderly are more vulnerable to death from exposure to new viral/bacterial
infection.
© Montecino-Rodriguez, E., Berent-Maoz, B. and Dorshkind, K. (2013) "Causes, consequences, and reversal of immune system aging", Journal of Clinical Investigation, 123(3), pp. 958-965. doi: 10.1172/jci64096.
On the
other hand, individuals aged between 0 - 64 make up only 20% of deaths from
COVID infection (which, again, is a questionable statistic), yet account for at
least 72% of vaccine reactions. Below the age of 49, the survival rate of COVID is in
excess of 99.8%. A calculation by Dr. Michael Yeadon suggests that children are more than 50 times more likely
to die from vaccination than from COVID-19 infection. This is unsurprising
because younger individuals possess robust, reactive immunity against new
threats. Their ability to
generate highly specific antibodies and initiate strong T-cell responses against
potential pathogens provides them with almost 100% protection against viral
infections such as COVID-19. However, it is exactly this immune
responsiveness which becomes the practical danger in vaccination because the
primary mechanisms of vaccine-injury are caused by the immune system going into
overdrive. The stronger
the immune system, the greater the damage caused by vaccine reaction.
Why are the effects mostly seen in
males?
Myo/pericarditis appears to be one of the most common adverse events experienced
shortly after vaccination and, as we have seen, is disproportionately affecting
males. Cardiovascular injury and disease are more prevalent in males even outside of the
context of vaccination. Both
innate and adaptive immune cells are involved in vaccine injury, and
key sex differences exist
in immune system dynamics and responsiveness to infection/inflammatory triggers.
COVID vaccines, especially the second dose and boosters, are known to stimulate a strong TH1-driven immune response,
which likely involves spike protein activation of TLRs.
The initiation of cardiac damage in myocarditis is associated with heightened Th1-driven cell-mediated immunity,
involving significant elevations in proinflammatory Th1 cytokines
Interferon-gamma (IFN-y) and Tumor Necrosis Factor-alpha (TNF-a).
Interestingly, recent analysis using computational systems
biology methods identified key signalling roles for IFN-y and TNF-alpha in
vaccine-induced myocarditis. Males
are known to have a greater tendency towards
proinflammatory Th-1 dominant immune responses, with stronger NK cell activity and
cytotoxic T-cell immunity capable of causing excessive tissue destruction if
left unchecked.
© Capone, I. et al. (2018) "Sexual Dimorphism of Immune Responses: A New Perspective in Cancer Immunotherapy", Frontiers in Immunology, 9. doi: 10.3389/fimmu.2018.00552.
Immune
cells have hormone receptors which are responsive to differences in hormone
concentrations and androgens such as testosterone heighten Th1 dominance,
whereas estrogens
have been shown to inhibit these responses in both males and females
and can
exert anti-inflammatory effects. Furthermore, testosterone was shown
to decrease
cardiac function after acute injury to the heart by increasing
tissue damage by proinflammatory cytokines. On the other hand, estrogens exert
anti-inflammatory effects, reduces tissue destruction and females have heightened protection against autoimmune myocarditis.
It is therefore possible that lower testosterone and higher estrogen is one of
the reasons why women respond to infection or trauma with less
inflammation in the heart compared with men. These sex differences
may therefore help to explain why we are seeing a greater increase in deaths
among males shortly after vaccination.
Does this mean that COVID vaccines are
safe for females?
Males statistically have more severe, immediate reactions to vaccinations,
probably due to underlying sex differences in immune function. The enhanced
cell-mediated immunity of males make them more susceptible to specific
conditions shortly after vaccination, such as myocarditis.
However, it is entirely
possible that females will experience just as many adverse events, although
they may take longer to develop and will likely manifest in different ways.
Remarkably, females
account for approximately 78% of all autoimmune pathology. They are at least twice as likely to
develop a much wider range of autoimmune conditions compared with males, and in
some cases are up to 10-20 times more likely. Like males, these
observations can likely be explained by sex difference in immune predisposition
and function.
© Fairweather, D.,
Frisancho-Kiss, S. and Rose, N. (2008) "Sex Differences in Autoimmune
Disease from a Pathological Perspective", The American Journal of
Pathology, 173(3), pp. 600-609. doi: 10.2353/ajpath.2008.071008.
Autoimmune disease prevalence is males
vs. females
As shown
above, it is important to note that females have a significantly higher predisposition toward Th-2 driven
and antibody mediated immune pathology. Given what we now know about the
cross-reactivity of SPIKE protein antibodies with self-antigens, I believe it
is highly likely that COVID vaccination will contribute to the development of
long-term autoimmunity in a significant proportion of vaccine recipients.
This is most likely to affect females. And because the symptomatic
manifestations of chronic autoimmunity can take several years to show, we may
not be able to see the population-wide effects just yet.
Conclusion
The long-term effects of this novel technology are completely unknown. Many of the world's leading scientists
and physicians, including inventor of mRNA vaccine technology Dr. Robert
Malone, have warned of the dangers and potential long-term side-effects of
mass-COVID vaccinations. These include widespread development of
severe autoimmune illness, prion disease and other
potentially lethal neurological disorders, mass infertility, the creation of lethal new
variants,
permanent incorporation of
foreign mRNA into the human genome, and antibody-dependent-enhancement
leading to increased
susceptibility to death from viral exposure.
With the rollout of COVID vaccines for younger children, it is entirely
possible that the effects will become more pronounced among this demographic,
and if the authorities had any concern whatsoever for the health of the
population at large, this
mass-experiment would be stopped immediately.