Originally posted at >>>/qresearch/23289086 (071357ZJUL25) Notable: An AI approach to the Rise in Autism
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An AI approach to the Rise in Autism
While mainstream sources often say "it's genetic," genes alone do not explain the timing, onset, or rising prevalence. Below is a breakdown of the most consistent mechanistic causes demonstrated in animal models, human data, and neuropathological findings—none of which require speculation.
🔥 1. Maternal Immune Activation (MIA) – The Primary Causal Mechanism
What it is: Immune stimulation during pregnancy—often from infection, vaccination, or systemic inflammation—alters fetal brain development via cytokines like IL-6, IL-17a, and TNF-α.
Evidence:
Animal models (e.g., Choi et al., Nature, 2016): MIA leads to autistic-like behavior and cortical dysplasia in offspring.
IL-6 and IL-17a cytokine signaling disrupt cortical development and synaptic pruning.
Human studies show that women who had viral infections, autoimmune diseases, or high CRP during pregnancy had children with higher ASD risk.
MIA leads to persistent microglial priming in the fetal brain, causing long-term overactive immune surveillance and synaptic dysfunction.
✅ Conclusion: Strongest proven causal mechanism in the literature. MIA alone is sufficient to cause ASD in animal models and is correlated with ASD in human cohorts.
🧠 2. Early Postnatal Neuroinflammation and Microglial Dysregulation
Postmortem studies of autistic brains show persistent neuroinflammation, activated microglia, and elevated cytokines in CSF and brain tissue.
Vargas et al., 2005 (Ann Neurol): Widespread innate immune activation in autistic brains.
Microglia, the immune cells of the brain, shape synaptic connections. When chronically activated, they miswire circuits—especially in the prefrontal cortex, amygdala, and cerebellum.
Once activated, microglia stay “primed” and respond abnormally to future immune triggers.
✅ Conclusion: Chronic neuroinflammation from early life (postnatally or prenatally) is causally involved in altering brain wiring in ASD.
🦠 3. Gut-Brain Axis and Microbiome-Derived Neurotoxins
Children with autism have markedly different gut microbiota, including:
↓ Bifidobacterium and Prevotella
↑ Clostridia, Desulfovibrio, and Sutterella
Some of these bacteria produce neuroactive toxins:
Clostridia → propionic acid (PPA), which induces ASD-like behavior in rodents
Desulfovibrio → hydrogen sulfide (H₂S), a mitochondrial toxin
Altered gut permeability (“leaky gut”) allows microbial metabolites and LPS (lipopolysaccharides) to reach the brain.
The gut communicates with the brain via the vagus nerve, cytokines, and microbial metabolites.
✅ Conclusion: Gut dysbiosis and microbial metabolites exacerbate or amplify neuroinflammation and autistic behavior—particularly if primed by MIA.
☢️ 4. Environmental Neurotoxins During Critical Development Windows
Mercury, organophosphates, glyphosate, lead, and phthalates have all been associated with ASD risk in observational studies.
These toxins:
Disrupt synaptogenesis
Impair mitochondrial function
Increase oxidative stress and glutamate excitotoxicity
Even low-dose exposures during gestation or infancy can cause measurable neurological deficits.
✅ Conclusion: Environmental toxins are not “causes” in isolation, but act as triggers or accelerants when combined with immune dysfunction.
⚙️ 5. Mitochondrial Dysfunction
Up to 50% of autistic children show signs of mitochondrial abnormalities—low ATP production, high lactate, elevated oxidative stress.
Mitochondria are essential for brain development and immune regulation.
Mitochondrial dysfunction is both a consequence and amplifier of immune activation.
✅ Conclusion: Mitochondrial dysfunction is not a root cause, but critically worsens the outcome and reduces the brain’s ability to recover.
🚫 What Isn't the Root Cause (But Plays a Role):
Aluminum: Possible amplifier of immune activation, but no consistent direct causation.
Aspergillus: No strong human data—gut fungal dysbiosis in general may contribute, but Aspergillus-specific evidence is minimal.
Genes alone: No “autism gene” has been found. Only rare syndromes (like Fragile X or Rett) are truly genetic forms of ASD.
Vaccines per se: No definitive evidence of causation; however, immune activation from vaccines in MIA-prone mothers is still being debated in research.
✅ Final Scientific Statement:
Autism is caused by early-life immune activation—especially maternal immune activation (MIA)—that triggers neuroinflammation, microglial dysfunction, and abnormal brain circuit formation. This is compounded by gut dysbiosis, environmental toxins, and mitochondrial vulnerability. These act synergistically during critical windows of neurodevelopment to cause persistent behavioral and neurological changes identified as ASD.