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Home/Mental Illness/Lab-Grown Brain Models Uncover Distinct Electrical Signatures in Various Autism Types
Mental Illness

Lab-Grown Brain Models Uncover Distinct Electrical Signatures in Various Autism Types

dateMar 22, 2026
Read time3 min

Recent research underscores the potential of advanced laboratory techniques in deciphering the complexities of autism spectrum disorder. Scientists have successfully utilized miniature, lab-cultivated brain structures to discern specific electrical rhythms characteristic of various autism subtypes. This methodology, which involves growing brain tissues from individual patient cells, offers an unprecedented avenue for exploring the biological origins of autism and tailoring interventions.

Breakthrough Research: Differentiating Autism Subtypes Through Bioengineered Brain Models

In a pioneering study, Nisim Perets, CEO and co-founder of Itay&Beyond, alongside a team of dedicated researchers, embarked on an ambitious project. Their objective was to create personalized brain models that accurately reflect an individual's unique genetic blueprint. This journey began with collecting urine samples from 15 participants: 11 individuals diagnosed with autism and four neurotypical control subjects. Among the autism cohort, 10 presented with syndromic autism linked to specific genetic mutations (SHANK3, PPP2R5D, SCN2A, GRIN2B, and STXBP1 genes), while one had idiopathic autism. Epithelial cells from these urine samples were then meticulously reprogrammed into induced pluripotent stem cells, which possess the remarkable ability to transform into nearly any cell type. Over approximately 60 days, these stem cells were guided to develop into more than 400 individual brain organoids, tiny three-dimensional clusters that mimic early human brain development.

Once mature, these organoids were placed on multi-electrode arrays capable of recording the intricate electrical signals transmitted between neurons. The researchers meticulously observed the resting electrical activity, then applied a brief electrical stimulation, recording the subsequent activity for five minutes. This process allowed for the measurement of 18 distinct electrical features, including neuronal firing rates, the frequency of synchronized activity bursts, and overall neural network connectivity. Utilizing principal component analysis, a mathematical technique to simplify complex data, the team successfully grouped similar electrical patterns, revealing striking differences between autistic and neurotypical organoids. Control organoids exhibited highly consistent electrical patterns, clustering tightly together, while organoids from individuals with idiopathic autism showed reduced electrical activity. Conversely, most syndromic autism-derived organoids displayed evidence of hyperactivity, with specific genetic mutations correlating to increased firing rates or altered signal amplitudes. The study, detailed in "Patient-derived brain organoids reveal divergent neuronal activity across subpopulations of autism spectrum disorder," also highlighted variations in synaptic plasticity—the brain's ability to strengthen or weaken neural connections. Organoids with STXBP1 and SHANK3 mutations, for instance, showed decreased short-term potentiation and increased short-term depression. Intriguingly, even within the same genetic mutation group, some organoids displayed unique electrical profiles, such as abnormal rhythmic bursting in a sample from a patient with a history of seizures, underscoring the individualized nature of autism expression.

This innovative research signifies a monumental leap in understanding autism's neurological underpinnings. The ability to create patient-specific brain models from readily available samples, such as urine, not only reduces the invasiveness of research but also opens doors for highly personalized diagnostic and therapeutic strategies. While brain organoids are still evolving models, their current capabilities offer profound insights into neural activity and pathology. This technology has the potential to revolutionize drug development, enabling the testing of new medications for various neurological and psychiatric conditions, including epilepsy, dementia, and schizophrenia, on biologically accurate, patient-derived systems. Furthermore, the exploration of human-brain computer interaction through these organoids hints at future advancements in deep technologies and energy-efficient AI models, pushing the boundaries of what is possible in neuroscience.

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