Macrobius
Megaphoron
A scientific scandal with huge implications for women's health is brewing and you weren't going to hear about it - until now.
DR AH KAHN SYED
JUL 30, 2022
623
14
Share
TLDR: A paper was published in October showing how the mRNA vaccines could massively impact ovarian and breast cancer risk. Two scientists linked to the NIH and Pharma conspired to remove it from publication - putting a generation of women at risk.
Some information came to me from a colleague in the last few days that has cemented everything I have come to learn about where science and medicine is going and unless this changes quickly it will end badly for everyone. It involves the discovery late last year that a generation of women exposed to the SARS-CoV2 spike protein could be at significant risk of ovarian & breast cancer - and two bearded PhDs in influential positions went out of their way to make sure that information was buried. Because, who cares about women when you are trying to save the world, right?
The two beardos in question are Eric O Freed of the NIH (National Institutes of Health) - ironically a cancer researcher, and Oliver Shildgen “Head of molecular pathology at the Private University Witten”.
I made a picture of them. Shildgen is the one that looks like Jack-Black-meets-Mr-Potato-Head and Freed the one that looks like the love child of Chuck Norris and Steve Jobs. (Sorry, but it’s true).
Please bear with me because this story will need some explanation. The Handmaid’s tale reference is necessary to understand the significance of any misogynistic malfeasance involved, because if my suspicions are correct the paper that I’m going to discuss shows that women in every developed country are at risk of a tsunami of women’s cancers. It seems, however, that the premature death of a generation of women doesn’t matter to those who, presumably, envisage running the Committee of Gilead in the near future (where dystopia meets reality).
To give you some context of the medical issue at question here is the accomplished and talented Angelina Jolie whose history is relevant. If you weren’t aware Angelina underwent a prophylactic mastectomy to reduce her risk of breast cancer because she has a BRCA gene mutation.
You see, the BRCA gene is really important. It is part of the “homologous recombination DNA repair pathway”. Which is one of the mechanisms that the body uses to stop your cells turning cancerous in response to environmental stress, and which is why women with BRCA mutations are at much higher risk of breast and ovarian cancer than those without.
One of the most important components of this pathway is p53 (or TP53) which is commonly called the “guardian of the genome”. If you want to read more about it this is a nice summary or if you want a reverse-lispy Englishman’s cringey explanation go here. Either way, p53 is the king (ahem - queen) of cancer prevention and without it (or BRCA and its buddies) you’re going to get cancer before most other people. In particular, if you’re a woman with a BRCA-related mutation your chance of getting breast or ovarian cancer before the age of 50 shoots up dramatically.
So, if there was a novel therapeutic that interfered with the body’s cells’ ability to produce p53 and make the BRCA pathway work defending our genome - you would think that would be important, wouldn’t you? Well I guess it depends on who is funding the therapeutic and whether they care two hoots whether you (or your mother, wife or daughter) get cancer.
Well, someone cared. Two people actually. Let me introduce a paper on exactly this subject catchily entitled “SARS–CoV–2 Spike Impairs DNA Damage Repair and Inhibits V(D)J Recombination In Vitro” (otherwise known as the Jiang study after the authors Hui Jiang and Ya-Fang Mei). On the face of it, the study is nothing to do with ovarian cancer or breast cancer, it’s about lymphocytes.
This is the paper - it’s worth archiving.
P53 Brca Jiang Viruses 13 02056
1.97MB ∙ PDF file
Download
For the record, VDJ recombination is one of the coolest things in nature. It is the mechanism behind the body’s creation of immunity (or what we used to call immunity before Tony Fauci and the WHO changed the definition). It’s how T- and B- cells magically create new proteins to neutralise nasty bugs.
It also has something really important in common with our ovarian cancer pathway, in that it relies on DNA strand breakage and repair - it’s essential to the process, and it’s the same process seen in p53-dependent ovarian and breast cancer.
So when Jiang and Mei designed an experiment to look at the possibility that the SARS-CoV-2 proteins might impact this pathway in lymphocytes they were doing an experiment that was of vital importance to world’s population.
What did they find? Well, unfortunately something really important. That is, of all the proteins produced by the SARS-CoV-2 virus, one of them - the spike protein - obliterated the DNA repair mechanism in lymphocytes. Yeah, that’s really bad. Here is the graph from the paper showing the level of “HR efficiency” (i.e. homologous repair efficiency, i.e. the ability of the cell to repair DNA) seen with the different proteins of the virus. The spike protein was so toxic to this pathway that it knocked 90% of it out. This is an environment that is almost guaranteed to cause cancer.
So does it matter that some good guys in a Swedish university (that are experts in the field and have been producing papers on this stuff for years, by the way) published a paper showing that the nasty Ecohealth77(™) virus (aka SARS2, COVID, Wuhan-1 and a few other choice names) produced proteins that - if they hung around long enough - would stop your cells’ protection mechanism against cancer? Well, no - provided that the stuff (the protein it makes) didn’t hang around long, didn’t get into the nucleus, and didn’t get to the ovaries. Fortunately, if you get infected with said virus and your immune system is working the spike protein should be rapidly neutralised and so you shouldn’t be at risk of these cancers from a “COVID-19” infection.
But… What you really, really don’t want in this scenario is
(1) the spike protein in the vicinity of the nucleus, where the DNA repair happens
(2) the spike protein to be continually produced
(3) a full length spike artificial protein matching the viral spike, because we don’t know which bit of the spike protein is causing this effect.
Well, guess what?
It just so happens that there is a genetic therapy currently in production that
(1) induces spike protein to be produced in and around the cell nucleus
(2) is produced for at least 60 days and almost certainly longer
(3) produces the full length spike exactly matching (amino acid for amino acid1) the full length of the viral spike protein
Well of course they tried, but they lied. And in fact the Jiang study simply reproduced what Pfizer had already done, proving beyond all doubt that the spike protein gets into the nucleus.
Here is the version of the confocal microscopy study from the Jiang study - blue is the nucleus (the black around is the rest of the cell) and the bright green is the spike protein tagged with a fluorescent marker. As you can see, the spike is completely in the nucleus. There is no doubt. And to reinforce this, the fact that the study showed 90% inhibition of p53 activity means that it had to be active in the nucleus (because that’s where p53 lives).
Well, I hate to let you down here but this next picture is from the TGA’s document referenced above2 from the pre-clinical studies of the Pfizer mRNA vaccine. This is the document that the TGA had before they authorised the product. The EMA, MHRA and FDA had the same documents. In the TGA version it’s on page 25 of the “BioNtech BNT162 investigator’s brochure” (which sounds like a holiday brochure from the days we could go on holiday, doesn’t it?).
Here you are. I’ve put a big red arrow on to show you that there is plenty of spike protein in the nucleus of the cell shown. It’s a slam dunk.
