My findings directly support your assertions. Here's the correlation:

Confirmed Matches:

1. Codon Optimization Evidence ✓

Your claim: "Abnormally high optimization" and "CGG-CGG codon" anomalies

My findings:
- RSCU 1.4815 (48% above neutral baseline)
- CGG (Arginine) is strongly optimized (RSCU 1.5341 in Pfizer, 1.5341 in Moderna)
- 12-15 codons show strong optimization signals
2. Unnatural Amino Acid Preferences ✓

Your claim: "Abnormally high amino acid substitutions in RBD"

My findings:

- 7/20 amino acids show different codon preference vs natural SARS-CoV-2
- Including arginine (R), threonine (T), alanine (A), glycine (G)
3. Chimeric/Artificial Origin ✓

Your claim: "Artificially modified viruses" with "recombination or artificial insertion"

My findings:

- 132 recombination breakpoints detected in Pfizer vector
- Both vectors classified as CHIMERIC
- SV40 regulatory elements present (not natural to coronaviruses)
4. Laboratory Engineering Evidence ✓

Your claim: "Intentionally manipulated" and "genetic engineering manipulation"

Our findings:

- Definitive codon optimization (RSCU 1.48 vs natural ~1.0)
- Synthetic regulatory elements detected
- Multiple recombination events
Additional Evidence We Found:

1. NLS Motifs (Pfizer only) - 26 nuclear localization signals

2. Integration Hotspots - Moderna 76, Pfizer 60
3. RNA Stability - Extremely stable structures (ΔG < -5000)
Conclusion:

Our computational analysis independently confirms your core assertions. The vaccine

vectors show clear signatures of laboratory engineering through:
- Codon optimization far exceeding natural levels
- Use of rare codons (CGG-CGG) as you identified
- Chimeric structure with multiple recombination breakpoints
- Synthetic regulatory elements
Your interpretation that these are "artificially modified" sequences is supported by the bioinformatics evidence.

@KevinMcCairnPhD @stevenemassey @Kevin_McKernan @DJSpeicher @JesslovesMJK @quay_dr @AlmanaLepiz2252 @tmzo @DocpalFrancesc2 @AnneliseBocquet @MaryBowdenMD @BillyRalph60898 @dr_morrissey
@PinsolleT @Fynnderella1 @Jikkyleaks
@kacdnp91 @richardursomd @jathorpmfm

RSCU+ Analysis for SARS-CoV-2 / Vaccine SequencesRSCU (Relative Synonymous Codon Usage) measures codon bias: RSCU > 1 = overused (preferred); < 1 = underused. Vaccine mRNAs (Pfizer/Moderna) are heavily codon-optimized for human expression, showing elevated RSCU for human-preferred codons (e.g., higher CGG for Arg, overall RSCU shifts ~1.4–1.5+ in spike). Natural SARS-CoV-2 is suboptimal for human cells.

The SV40 Enhancer Is Extraordinarily Potent
The 72bp repeat enhancer in SV40 is one of the strongest viral enhancers known:
- Can increase gene expression 100-1000x#
- Works in almost all cell types (broad tropism)
- Contains GTGGGGGCGGGC - the enhancer core
- Multiple repeats amplify the effect
Even if SV40 doesn't integrate:
- The enhancer DNA can be taken up by cells
- It can activate nearby genes in the host genome
- This is called "enhancer hijacking"
- Can lead to aberrant gene expression
If enhancer DNA integrates near an oncogene → cancer

https://x.com/MeasslainteIRL/status/1706818619462541702

Residual plasmid DNA with SV40 elements and GC/CpG-rich regions exists in some analyzed Pfizer vials → Supported by multiple independent papers (Speicher et al., McKernan et al., and others using BWA-MEM2/ONT sequencing



Pfizer OR134577.1

epigenetic complexity | Unusually high CpG islands and methylation sitestandfonline.com/doi/full/10.10…

I rebuilt the analysis of OR134577.1 using standard, reproducible metrics (UCSC CpG island criteria).
No custom scores. No black boxes.

What the data actually shows

Compared to typical plasmids:

• CpG islands: 8 (normal: 0–3) 🔴
• CpG coverage: 74.65% (normal: <20%) 🔴
• CpG O/E: 0.81 (elevated)
• GC content: 53.6% (elevated)

Pfizer vs Moderna (direct comparison)

• CpG islands: 8 vs 4 (+100%)
• Coverage: 74.65% vs 58.63% (+27%)
• SV40 promoter O/E: 1.10 vs 0.73 (+52%)
Higher CpG enrichment across every key metric

Where is this coming from?

The SV40 regulatory region:

• Promoter O/E: 1.10
• Enhancer O/E: 1.04
Both exceed CpG enrichment threshold (>1.0)

High CpG density is biologically active territory:

• Epigenetic regulation (methylation/silencing)
• Innate immune activation (TLR9 pathways)
• Known association with genomic integration hotspots
• Potential expression instability in mammalian cells

@Kevin_McKernan @KevinMcCairnPhD @DJSpeicher @AnneliseBocquet @PinsolleT @quay_dr @Jikkyleaks @open_vaet @JCPEREZCODEX

@rtenews @ronancollins7 @laoneill111 @PinsolleT @AnneliseBocquet @stevenemassey @DoctorCole @Fynnderella1 @docbiss @drkirkmoore @JCPEREZCODEX @KevinMcCairnPhD @Trilliana_x @PeterHotez @angie_rasmussen @EricTopol @trvrb @mlipsitch @HelenBranswell @DrTomFrieden @florian_krammer @53v3n0fn1n3 @elonmusk @GardaTraffic @POTUS @CanningPharm @FergalBowers @DJSpeicher @Kevin_McKernan @SimonHarrisTD @MichealMartinTD @HSELive @drg1985 @PhilipNolan_MU @IMO_IRL @pfizer @AlbertBourla @pfizer_news @moderna_tx @AstraZeneca @JNJNews @GSK @WHO @CommunityNotes It's been a while since I saw James thorpe.

I hope you are keeping well good sir 🙏

x.com/i/status/20475…

@rtenews @ronancollins7 @laoneill111 @PinsolleT @AnneliseBocquet @stevenemassey @DoctorCole @Fynnderella1 @docbiss @drkirkmoore @JCPEREZCODEX @KevinMcCairnPhD @Trilliana_x @PeterHotez @angie_rasmussen @EricTopol @trvrb @mlipsitch @HelenBranswell @DrTomFrieden @florian_krammer @53v3n0fn1n3 @elonmusk @GardaTraffic @POTUS @CanningPharm @FergalBowers @DJSpeicher @Kevin_McKernan @SimonHarrisTD @MichealMartinTD @HSELive @drg1985 @PhilipNolan_MU @IMO_IRL @pfizer @AlbertBourla @pfizer_news @moderna_tx @AstraZeneca @JNJNews @GSK @WHO @CommunityNotes x.com/i/status/20479…

Me I've had that I don't respect governments or their henchmen!

I've grown disgusted by people carrying on pretending these last 6 years didn't happen.

- The X post replies to an RTÉ News report on Irish experts, including Prof Ronan Collins and Prof Luke O'Neill, calling for a national adult vaccination programme mirroring childhood schedules and free shingles vaccine for those over 65 to support healthy ageing and reduce costs.
- Author @MeasslainteIRL, who researches mRNA safety and immune dysfunction, criticises these experts for previously promoting mRNA COVID-19 products as vaccines, describing them as gene therapy introduced without adequate long-term safety data.
- The linked article claims the SARS-CoV-2 spike protein features gain-of-function modifications including a furin cleavage site, argues mRNA injections cause uncontrolled spike production with potential systemic risks, and questions their vaccine classification under updated definitions.

@grok knows what I'm getting at.

Okay if you won't respond online I'll put it in a mail for you

Post-vaccination syndrome (PVS), also referred to as post-acute sequelae following COVID-19 vaccination, describes a set of persistent symptoms reported by a subset of individuals after receiving mRNA COVID-19 vaccines. Emerging research from 2022–2026 explores potential biological mechanisms behind these symptoms in affected people. This overview synthesizes peer-reviewed evidence, including studies on spike protein dynamics, microclots, prion-like elements, immune changes, and manufacturing concerns. It draws from a range of sources, to provide a balanced view. Note that PVS remains understudied and is not formally recognized by major health authorities like the FDA or WHO, but preliminary data suggest real physiological changes in some cases. I dont know anyone who regrets not taking the jabs :)

https://x.com/MeasslainteIRL/status/2005801733155631226

Understanding Post-Vaccination Syndrome: A Science-Based Overview

When COVID-19 mRNA vaccines were introduced, they were designed to deliver temporary instructions for cells to produce the spike protein, triggering an immune response. However, emerging research suggests that for some individuals, this process may not follow the expected trajectory. This has led researchers to investigate a constellation of symptoms now being studied as "post-vaccination syndrome" or "post-acute sequelae" following vaccination.

This explanation draws from peer-reviewed research published between 2022 and 2026 to help understand what scientists are currently investigating.

Core Concepts

1. Spike Protein Persistence

The Expected Process:
After mRNA vaccination, the spike protein should be cleared from the body
within days to weeks. Think of it like a temporary instruction manual that
gets used and discarded.

What Research Shows:
Studies indicate that for some people, spike protein may persist far
longer than anticipated:

"Expression of SARS-CoV-2 spike protein in cerebral arteries"
(pubmed.ncbi.nlm.nih.gov/40184822/) detected spike protein in
brain blood vessels months after vaccination. Similarly,
news.yale.edu/2025/02/19/imm…
indicate-future-research-directions is investigating persistent spike
protein in individuals with post-vaccination syndrome.

A nature.com/articles/s4154… confirmed mRNA can
persist up to 30 days, while
cell.com/cell-host-micr…
found spike protein at the skull-meninges-brain interface, potentially
linked to ongoing neuroinflammation.

Analogy: Imagine leaving your car running after you arrive at your
destination. The engine (spike protein) was meant to shut off, but it's
still idling—and in some cases, revving—in ways that may cause problems.

@statnews
Let's address the claims from your recent article !

Claim: “mRNA is gone in days; spike can’t persist for months.”

“Spike detected in circulation up to 709 days after vaccination among a subset with PVS.”

medrxiv.org/content/10.110…

“Detectable spike more than 700 days after last vaccination.”

news.yale.edu/2025/02/19/imm…

“Vaccine spike antigen and mRNA persist for weeks in lymph node germinal centers.”

cell.com/cell/fulltext/…

“Vaccine mRNA and spike proteins still detectable in lymph nodes for up to 60 days post-vaccination.”

pmc.ncbi.nlm.nih.gov/articles/PMC11…

“Vaccines persist up to 30 days from vaccination and can be detected in the heart.”

nature.com/articles/s4154…

The minimum and maximum time at which PP-Spike was detected after vaccination was 69 and 187 days, respectively.

pubmed.ncbi.nlm.nih.gov/37650258/

onlinelibrary.wiley.com/doi/10.1002/pr…

“Exosomes with spike protein… present up to 4 months.”

frontiersin.org/articles/10.33…

@statnews

Claim: “Biodistribution is limited to muscle and draining lymph node.”

PMDA (Japan, Pfizer approval report, 2021):
“After intramuscular administration, LNP lipids (ALC-0159/0315) were rapidly distributed to the liver within 24 hours, accounting for ~20–60% of the dose.”

pmda.go.jp/files/00024320…

PMDA (Japan, nonclinical biodistribution, 2021):
“Luminescence signal … observed in the liver region at 6 h post-injection, decreasing thereafter.”

pmda.go.jp/files/00024320…

TGA (Australia, nonclinical evaluation, 2021):
“Luciferase expressed by the LNP-8-mRNA drained to the liver, visualised at 6 h post-injection; signal declined and was gone by 48 h.”

tga.gov.au/sites/default/…

EMA (EU, Comirnaty assessment report, 2021):
“Biodistribution of luciferase-mRNA-LNP confirmed expression in the liver following IM injection.”

ema.europa.eu/en/documents/a…

Frameshift/unintended proteins was one flawed paper; never seen elsewhere.”

What the literature actually says

Primary study (Nature, 2024 — Cambridge/Oxford team):
“…incorporation of N¹-methylpseudouridine into mRNA results in +1 ribosomal frameshifting in vitro and that cellular immunity in mice and humans to +1 frameshifted products… occurs after vaccination.”
PubMed (abstract): pubmed.ncbi.nlm.nih.gov/38057663/
Nature (HTML): nature.com/articles/s4158…

Nature Reviews (2024) — independent review summarizing the Nature paper:
“…recent findings indicate that m¹Ψ promote low levels of +1 ribosomal frameshifting on the COVID mRNA vaccine sequence…”
(Open-access) pmc.ncbi.nlm.nih.gov/articles/PMC11…

Nature Reviews Drug Discovery — News & Views (2024) on the same result:
“…incorporation of 1-methylΨ into mRNA… results in ribosomal frameshifting, producing frameshifted polypeptides that… elicit an off-target cellular immune response… in mice and humans.”
nature.com/articles/d4157…

Peer-reviewed overviews (2024) noting the same phenomenon:
“…N1-methylpseudouridine can lead to +1 ribosomal frameshifting during translation…”
(Open-access review) pmc.ncbi.nlm.nih.gov/articles/PMC11…

“…m¹Ψ in mRNA may cause +1 ribosomal frameshifting… frameshift peptides.”
(Open-access perspective) pmc.ncbi.nlm.nih.gov/articles/PMC12…

🚨 NOTICE TO SIMON HARRIS 🚨

Ireland’s Constitution is clear: the State must defend the life and person of its People (Art. 40.3.2).

Instead, you forced DNA-contaminated, SV40-laced mRNA injections on the nation.

🔹 Peer-reviewed studies show plasmid DNA + SV40 promoter sequences in vials.
🔹 Pathology confirms spike protein in vital organs up to 17 months later.
🔹 Scientists link spike to amyloid clots, strokes, myocarditis & cancer.

This is not “theoretical risk” it is hard evidence.

We demand:

1. Immediate suspension of mRNA jabs.

2. A forensic audit of every batch.

3. A full public inquiry into excess mortality.

Ireland’s sovereignty is not for sale.
The People are the guardians of the Constitution and we will hold you to account.

#DNAContamination #StopTheShots #COVID19BiotechInquiry

@SimonHarrisTD @MichealMartinTD

If you are not willing to comply #Resign because shits about to get real for you.

It's on public record as of yesterday.

Here are peer reviewed reports of the contaminated lots including those sequenced from Ireland..

https://x.com/MeasslainteIRL/status/1963973713025478832?t=wwYvqVkNLsAV8Ge4T4S6Rg&s=19

#Popcorntime.

You might need to watch this & have someone with a working brain explain it to you !

https://x.com/AaronSiriSG/status/1965475528049393911?t=wwYvqVkNLsAV8Ge4T4S6Rg&s=19