Another day, another alarming confirmation that those duped unfortunates that subjected themselves to the slow kill bioweapon are in all kinds of genetically modified trouble.

A French study using nationwide hospital discharge and vaccine data has shown "strong evidence of an increased risk of myocarditis and of pericarditis in the week following vaccination against Covid-19 with mRNA vaccines in both males and females."

That’s the first week. What happens longer term may be even more concerning as the amyloid buildup increases in the heart and brain, while the p53 protein responsible for surprising cancer and tumor growth is itself suppressed by the cytotoxic spike proteins that being endogenously produced for indefinite periods of time due to the pseudouridine component of the Modified mRNA injection. And there are quite literally thousands of other severe adverse events.

The associations were particularly pronounced after the second dose, and were evident in both males and females. We found a trend of increased risks towards younger age groups but a significant risk was also found in males over 30 years to develop myocarditis and in females over 30 years to develop a pericarditis after vaccination.

If allowed, the researchers will corroborate that which BigPharma and their statist One World Government partners in crime do not want anyone to be privy to just yet; namely, as per Israeli and Canadian data the poison is determined by the dose, with the 3rd injection being far worse than the previous two.

Of course, the name of the game here is suppress the truth and drag out the research as long as possible with the goal of administering the maximum amount of deadly boosters, at which point it will truly be too late for far too many; to wit:

Future studies based on an extended period of observation will allow to investigate the risk related to the booster dose of the vaccines and monitoring the long-term consequences of these post vaccination acute inflammations.

Basically, everyone that has received the DEATHVAX™ is compromised in varying degrees.

Reassuringly, these cases of myocarditis and pericarditis, although requiring hospitalization, did not result in more severe outcomes than those unrelated to vaccination.

“Reassuringly,” very little in this study is in fact reassuring due to the sleight of hand in that sentence which attempts to minimize the severity of DEATHVAX™-induced cardiac damage. The researchers fail to present clearcut methodology for comparing the gene therapy damaged individuals to those “severe outcomes unrelated to the vaccination.” All of their citations are from “vaccine” years, and thus do not establish relative severity, and just as importantly dare not review the YoY changes in myocarditis and pericarditis cases pre and post DEATHVAX™ rollout.

Our findings bring new elements in showing that the risk of acute cardiac inflammation after vaccination is not confined to myocarditis in young men.

All adverse events are not confined to any demographic, even if some demographics express said AE’s sooner than others.

All demographics subjected to the DEATHVAX™ will experience shortened lifespans.

Expect an even more drastic push for never-ending boosters to coincide with the followup “pandemic” in PSYOP-22, which will be deployed sometime prior to the USSA midterm elections.

This study is featured in Nature magazine, and may be read in its entirety here.

Do NOT comply.