Study: COVID-19 Injections Deliberately Engineered

In particular, the DEFUSE proposal submitted by EcoHealth Alliance to the Defense Advanced Research Projects Agency (DARPA) in 2018 described the intentional creation of chimeric coronaviruses with enhanced infectivity, including features like the furin cleavage site (FCS) and human immunodeficiency virus (HIV)-like inserts. SARS-CoV-2 displays multiple genomic features indicative of laboratory manipulation.

The deliberate concealment of critical genomic features delayed public awareness and pandemic mitigation efforts, potentially allowing wider spread and more deaths. The retention of high-risk viral features in both the virus and the vaccine design contradicts decades of safe vaccine development practices. Proven or promising treatments such as hydroxychloroquine, vitamin D, and fusion inhibitors were suppressed in favor of a vaccine-first strategy.

Further analyses conducted and verified by Lt. Edward Macie, USN, through April 2025, using the 2016–2020 baseline, showed persistent elevations: myocarditis (153.8% in 2023), infective myocarditis (168.5% in 2021, 122% in 2022, 14% in 2023), digestive organ cancer (15.8% in 2021, 30.2% in 2022, 46.3% in 2023, 43% in 2024), brain cancer (27.2% in 2021, 39% in 2022, 40.1% in 2023), and coagulation defects (25.3% in 2021, 58% in 2022, 31.8% in 2023).

Choutka et al. further demonstrated that COVID-19 causes extensive T-cell dysregulation characterized by lymphopenia, exhaustion, and aberrant cytokine profiles, which persist into PASC and may also arise from repeated spike exposure via mRNA vaccination.

The modified mRNA biologics/vaccines, including those from Pfizer and Moderna, can induce IgE sensitization to the spike protein, PEG, or LNPs. Repeated vaccinations elevate IgE levels, heightening the risk of cytokine storms upon subsequent exposures. These storms involve mast cell degranulation, histamine surges, and massive cytokine release, leading to clinical manifestations ranging from mild allergic reactions (e.g., rashes, hives) to severe outcomes, such as anaphylaxis or cardiovascular events, including Kounis Syndrome, where anaphylaxis triggers acute coronary syndrome.

In a cohort study conducted by Faksova et al. (n = 99 million), the investigators reported a 510% increased risk of myocarditis following mRNA vaccination, a 278% increased risk of acute disseminated encephalomyelitis (ADEM), a 223% increased risk of cerebral venous sinus thrombosis (CVST) following viral vector vaccination, and a 149% increased risk of GBS, also associated with viral vector platforms.

A 2024 study by Lin et al. confirmed transplacental mRNA transfer into fetal blood, with bioactive mRNA inducing spike protein expression in the placenta and decidua, potentially explaining placental abnormalities. Research by Hanna et al. in 2022 and 2023 detected intact mRNA in breast milk, suggesting infant exposure. Alden et al. in 2022 showed in vitro reverse transcription of vaccine mRNA into human liver cells, raising concerns about genomic integration. These findings indicate developmental or immunological effects in fetuses or newborns from mRNA exposure.

A 2024 report by McKernan confirmed SV40 and plasmid DNA in biopsies from a vaccinated cancer patient. If this DNA integrates into the genome, it could lead to cellular transformation or genetic abnormalities, particularly in pregnant women and their offspring.

The spike protein’s S2 subunit may disrupt p53 tumor suppressor activity by interacting with p53 and mouse double minute 2 (MDM2), reducing p21 and death receptor 5 (DR5) activation and impairing DNA repair.

Aberrant proteins may be recognized as foreign, triggering inflammatory responses, or share homology with human proteins, risking autoimmunity. Misfolded proteins could aggregate, causing cellular stress, toxicity, or contributing to neurodegenerative disorders, such as prion diseases. … In rare cases, functional but unintended proteins could emerge, potentially interacting with chromatin to cause epigenetic changes or affecting the cell cycle to promote tumorigenesis.

A Seoul-based study in molecular psychiatry linked COVID-19 vaccination to increased risks of depression (HR 1.683, 95% CI 1.520–1.863); anxiety, dissociative, stress-related, and somatoform disorders (HR 1.439, 95% CI 1.322–1.568); and sleep disorders (HR 1.934, 95% CI 1.738–2.152), raising safety concerns warranting further investigation.

The rapid proliferation of mRNA, saRNA, and circRNA biologics amplifies ethical and safety concerns. Prolonged protein expression, exemplified by S1 spike protein detection more than 700 days post-COVID vaccination, underscores the potential for irreversible harm. The self-replication of saRNAs and the stability of circRNAs exacerbate these risks, lacking a reliable “off switch.”

Basic health measures, such as ensuring vitamin D levels above 50 ng/mL to prevent severe disease were ignored. Safe, off-label treatments like ivermectin and hydroxychloroquine/zinc, with decades of established safety, were suppressed. Coercion, suppression of vaccine limitations (lack of safety, efficacy, and transmission prevention), and violations of informed consent contravened the Nuremberg Code, Helsinki Declaration, and U.S. constitutional protections (First, Tenth, Fourteenth Amendments).