The current “safe limit” for aluminum in vaccines (~0.85 mg per dose) wasn’t set using modern safety studies or toxicology. It actually comes from old vaccine practices in the mid-1900s, when they were just testing what made vaccines more effective.

A 2025 review shows there’s no real toxicology or pharmacokinetic science behind this number. it’s not based on how aluminum actually behaves in the body.

Q: Why are we still using efficacy-era thresholds to claim safety in infants?

pubmed.ncbi.nlm.nih.gov/40876523/

@RobertKennedyJr @jsm2334

A big 2025 study (Annals) looked at health records from 1.22 million children, tracking aluminum exposure from vaccines before age 2. They reported mostly no associations across 50 different health outcomes.

The study left out diagnoses before age 2 the most critical early window. And they didn’t compare vaccinated kids to the unvaccinated group directly, which could have been the strongest test.

Q: If the dataset had ≈15k unvaccinated, why not show that comparison transparently?

acpjournals.org/doi/full/10.73…

The study actually found a signal for Asperger’s risk was about 1.67x higher per mg of aluminum (2007–2018 births).

Instead of digging deeper, the authors brushed it off as “chance” and blamed overlap issues in the data. When they restricted the analysis to later births, the signal disappeared.

Fine but the obvious next step is to replicate with a proper design (pre-registered overlap checks, latency controls, and false-discovery corrections).

Q. why was the instinct to dismiss the finding, rather than design the follow-up that could confirm or rule it out?

acpjournals.org/doi/full/10.73…

Kevin McKernan
Profession: Founder of Medicinal Genomics, Genomics Researcher, US
Date First Reported: 2023-02
Key Details: Detected 225-843ng/dose residual plasmid DNA including SV40 promoter in Pfizer/Moderna vials using qPCR/fluorometry; exceeds regulatory limits; integration concerns.
Sharable Link: osf.io/mjc97/

Tomonori Nitta
Profession: Researcher at Tokyo University, Japan
Date First Reported: 2023-11
Key Details: Found 17.5-81.9ng/dose DNA in Japanese Daiichi-Sankyo vials; SV40 detected, including in tumors via cell transfection
Sharable Link: pmc.ncbi.nlm.nih.gov/articles/PMC12…

Phillip Buckhaults
Profession: Professor at University of South Carolina, Cancer Genomics Expert, US
Date First Reported: 2023-09 (testimony), 2024-04 (data)
Key Details: qPCR showed 1.5-18.7ng/dose plasmid DNA with SV40 promoter; observed integration into human stem cells; presented to SC Senate.
Sharable Link: scstatehouse.gov/CommitteeInfo/…

Ditch These Foods to Heal Chronic Illness
Explore the hidden biochemical triggers of inflammation and the foods that stoke the flames,
Perfect for those battling autoimmune diseases, neuroinflammation, chronic fatigue, IBD, MS, arthritis, or post-viral syndromes taking control of these triggers is your key to reclaiming vitality!

🌾 Gluten Sensitivity: The Hidden Inflammation Trigger

Struggling with chronic inflammation, autoimmune flares, fatigue, or brain fog?
Gluten may be silently sabotaging your gut and immune system even if you don’t have celiac disease.

🔓 Leaky Gut & Systemic Inflammation

Gluten stimulates zonulin, a protein that opens tight junctions in your intestinal lining. This leads to leaky gut, allowing bacteria, food particles, and toxins to escape into your bloodstream triggering chronic immune activation and inflammation throughout the body.

🧬 Autoimmune Activation via Molecular Mimicry

In genetically predisposed individuals (e.g., HLA-DQ2/DQ8), gluten peptides can resemble human tissue proteins. This "molecular mimicry" may cause the immune system to mistake your own cells for invaders, contributing to diseases like:
• Hashimoto’s thyroiditis
• Multiple sclerosis (MS)
• Rheumatoid arthritis
• Celiac disease

Non-Celiac Gluten Sensitivity (NCGS) Is Real

Even without celiac markers, many people experience bloating, diarrhea, joint pain, fatigue, skin issues, and brain fog after gluten exposure.
This is known as NCGS and it's now recognized in medical literature as a legitimate, immune-mediated condition.

✅ What You Can Do

• Trial a gluten-free diet for 30–60 days and track your symptoms
• Get tested: Ask your provider about anti-gliadin antibodies or genetic screening
• Focus on whole, unprocessed gluten-free foods not just GF packaged substitutes
• Reassess and reintroduce (if desired) later to confirm your sensitivity

📌 Healing often begins in the gut. If gluten is a trigger, removing it could be the most powerful anti-inflammatory step you take.

🥛 Dairy (Especially Conventional, Pasteurized A1 Dairy)

Examples: Milk, cheese, yogurt, cream, butter

🔥 Why It’s Inflammatory

Most commercial cow’s milk contains A1 casein, a protein that breaks down into beta-casomorphin-7 (BCM-7) a bioactive peptide linked to gut and brain inflammation.
Many people also lack the enzyme lactase, leading to poor lactose digestion, bloating, dysbiosis, and gut irritation.
Worse still, the immune system can develop IgG or IgA antibodies to casein, triggering systemic inflammation and potentially worsening autoimmune and neuroimmune conditions.

🚩 Who Should Be Cautious?

If you have any of the following, A1 dairy might aggravate your symptoms:
• Multiple Sclerosis (MS)
• Parkinson’s disease
• Chronic sinus issues or asthma
• Crohn’s or colitis
• Eczema, acne, or skin inflammation
• Brain fog, autism spectrum conditions, or neuroinflammation

Try removing dairy for 30–60 days and observe changes in energy, digestion, skin, and cognition.

✅ Better Options (Later On)

• A2 dairy (from A2 cows, goats, or sheep)
• Raw, fermented goat/sheep dairy (e.g. kefir)
These may be reintroduced cautiously in later phases, but all dairy is excluded initially to reduce inflammatory load.

📖 A controlled human study found that A1 milk increases GI symptoms and inflammation compared to A2 milk.
🔗 Read the study (Nutrition Journal, 2016)

pubmed.ncbi.nlm.nih.gov/27039383/

#DairyFree #Inflammation #Autoimmune #GutHealth #A1A2Milk

How to defend your genome, protect your mitochondria, and recover immune balance using natural food-based compounds 🌱

A breakdown of 10 disrupted pathways (and how to fix them

🧵⤵️

1. Insertional Mutagenesis 🧬

Contaminated plasmid DNA can insert into your genome → trigger mutations or activate oncogenes.

🛡️ Eat:

Broccoli sprouts (Sulforaphane)

Turmeric + pepper (Curcumin)

Blueberries & grapes (Resveratrol)

#GenomeIntegrity

p53 Suppression 💣

p53 = “guardian of the genome.” When it's silenced, cancer risk skyrockets.

🛡️ Eat:

Pomegranate (Ellagic acid)

Red onions, apples (Quercetin)

Pumpkin seeds, oysters (Zinc)

Chinese skullcap (Baicalin) → Activates p53, induces apoptosis

PD-L1 & IgG4 Immune Escape 🦠

Viruses & tumors cloak themselves by raising PD-L1 and shifting to IgG4.

🛡️ Strip the cloak with:

Apigenin herbs (chamomile, parsley)

Berberine (Th1/Th17 support)

Reishi, Turkey Tail (mushrooms FTW)

#ImmuneCheckpoints

#metaanalysis #ExcessDeaths
#NL #Netherlands 🇳🇱🇳🇱🇳🇱🇳🇱
The research report examines a potential relationship between COVID-19 vaccinations and excess mortality in the Netherlands, led by Ronald Meester and Dr. Marc Jacobs, is now available online: Research Report:
researchgate.net/publication/38…

This comprehensive study was made possible through a crowdfunding initiative by Stichting De Menselijke Maat. Alongside Dr. Marc Jacobs and Ronald Meester, the core research team included Bram Bakker, Jona Walk, and Jan Bonte. Given its depth, the report is extensive. Below is a concise overview of its key findings:
Chapter 1: Introduces the study and provides a justification for the research.
Chapter 2: Discusses excess mortality in the Netherlands, noting significant quantitative and qualitative changes since 2021.
Chapter 3: Presents data from AstraZeneca and the European Medicines Agency (EMA), raising concerns regarding vaccine safety.
Chapter 4: Covers their literature review and meta-analysis attempt. Out of 13,430 publications reviewed, only 83 met their stringent content and quality criteria. This finding suggests that "following the science" during the pandemic may not have always been prudent, given the varying efficacy rates and large uncertainty margins reported in the remaining studies.
Chapter 5: Focuses on a macro-level analysis of mortality related to vaccination. The findings suggest that vaccine effectiveness in the first four weeks post-administration may be negative, although the researchers exercise caution in their interpretations.
Chapter 6: Delves into micro-data from the Centraal Bureau voor de Statistiek (CBS) at an individual level. The researchers identified significant data artifacts that have potentially skewed all previous studies by both CBS and the RIVM (National Institute for Public Health and the Environment). The team refrains from speculating on the origins of this data contamination.
Chapter 7: Examines the reliability of the data used in their analysis, particularly focusing on CIMS and EMA data, which they found to be contaminated. This contamination complicates research efforts significantly.
Chapter 8: Explores the medical aspects of COVID-19 vaccinations, concluding that while side effects exist, their full extent remains unclear.
Chapter 9: Summarizes the research conclusions and offers recommendations for future studies.
This research represents a substantial contribution to the ongoing discussion about vaccine safety and public health during the COVID-19 pandemic.

All research transactions and data can be accessed through the following GitHub repository: GitHub Repository:

github.com/MJacobs1985/Ov…

@RonaldMeester

#ExcessMortality #Covid_19 #vaccine

Dr Jacobs is a data scientist/ statistical consultant. Subject matter experts are finding their voice.linkedin.com/posts/dr-marc-…

Broken into layman's for everyone to enjoy.

Title: Uncovering the Truth: A Deep Dive into COVID-19 Vaccines and Excess Mortality in the Netherlands

Introduction

In the wake of the global COVID-19 pandemic, nations worldwide rushed to develop and distribute vaccines in hopes of curbing the spread of the virus and reducing mortality rates. The Netherlands, like many other countries, embarked on an ambitious vaccination campaign. However, as the dust began to settle, an unsettling pattern emerged: despite widespread vaccination, the country continued to experience unexplained excess mortality.

This puzzling phenomenon has sparked intense debate and raised crucial questions about the relationship between COVID-19 vaccines and overall mortality rates. In response to these concerns, a team of dedicated researchers, led by Ronald Meester and Marc Jacobs, undertook a comprehensive investigation. Their findings, detailed in a 166-page report, challenge many widely held beliefs about vaccine safety and efficacy.

Today, we'll take you on a journey through this groundbreaking research, breaking down complex scientific concepts into digestible insights that could reshape our understanding of public health policies and vaccine impacts.

The Unexpected Persistence of Excess Mortality

Before we delve into the heart of the research, let's first understand what we mean by "excess mortality." Simply put, excess mortality refers to the number of deaths from all causes during a crisis that exceeds what we would have expected under 'normal' conditions. It's a crucial metric in public health, often used to assess the full impact of pandemics or other widespread health crises.

In the Netherlands, a troubling trend emerged following the rollout of COVID-19 vaccines. Instead of seeing a reduction in overall mortality as vaccination rates increased, the country continued to experience higher-than-expected death rates. This persistence of excess mortality, even as COVID-19 cases declined, raised red flags for our research team.

Key questions emerged:

1. Could there be a connection between the COVID-19 vaccines and this ongoing excess mortality?

2. If such a connection exists, what mechanisms might be at play?

3. How reliable is the data we're using to make these assessments?

With these questions in mind, let's explore the key findings of this extensive research.

1. The Data Dilemma: Uncovering Inconsistencies

At the heart of any scientific investigation lies data - the foundation upon which conclusions are built and policies are shaped. However, our research team uncovered troubling inconsistencies in the datasets provided by key institutions, including the CBS (Central Bureau of Statistics), RIVM (National Institute for Public Health and the Environment), and EMA (European Medicines Agency).

These discrepancies aren't merely academic concerns. They strike at the very core of how we assess vaccine safety and efficacy. Let's break down some of the key issues:

a) Disappearing Data:

The team observed that in the EMA database, which tracks vaccine-related adverse events, some reports seemed to vanish over time. By regularly downloading and comparing datasets, the researchers noticed a consistent pattern of record removal. This raises serious questions about data integrity and the completeness of our understanding of vaccine side effects.

b) Misclassification Concerns:

One of the most alarming findings related to the classification of vaccinated individuals. The research suggests that some people who died shortly after receiving a vaccine may have been incorrectly classified as "unvaccinated" in official records. This potential misclassification could significantly skew our understanding of vaccine-related risks.

Why yes we were !!
facebook.com/share/p/nj9TES…

https://twitter.com/catturd2/status/1790145016494436358

I was begging people not to inject their kids.

It fell on deaf ears.

facebook.com/share/p/XX74CJ…

I wasn't on X at the time I wouldn't have lasted long anyway 😂👌🏻

facebook.com/share/p/gb89bm…