Persistent cortical excitatory neuron dysregulation in adult Chd8 haploinsufficient mice.

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作者:Canales Cesar P, Lozano Stephanie A, Frost Nicholas A, Cichewicz Karol, Amaral Wellington, Seban Nicolas, Fenton Ethan, Wade Ayanna, Chu Nickolas, Smith Emily, Ardekani Cory, Frank Samuel, Bennett Jeffrey, Lavenex Pierre, Kopley-Smith Aspen, Rahbarian Darlene, Corea Melissa, Perla Daniela, Davis Liam, Zhu Jiyuan, Ortiz Rebecca, Beauregard Paris, Morse Sarah, Baker Jacob, Sun Jingqi, Ma Boxuan, Lu Ju, Sohal Vikaas S, Amaral David G, Zuo Yi, Nord Alex S
期刊:Res Sq影响因子:0.000
时间:2025起止号:2025 Aug 5
doi:10.21203/rs.3.rs-7208668/v1
CHD8 mutations cause autism spectrum disorder, cognitive deficits, and macrocephaly. Chd8 (+/-) mouse models exhibit macrocephaly and transcriptional pathology, with inconsistent findings regarding neurogenesis, neuron function, and behavior. Via stereology and single nucleus transcriptomics (snRNA-seq), we found increased Chd8 (+/-) cortical volume was not explained by increase in neuron number. Differential expression (DE) was present across cortical cell types, with excitatory neurons exhibiting high DE burden and shared and subclass-specific DE signatures. Bulk RNA-seq DE of constitutive Chd8 (+/-) and conditional Camk2a-Cre Chd8 (+/-) mice identified shared transcriptional pathology. DE in synaptosomal versus nuclear mRNA identified overlapping DEGs, but also significant differences and exaggerated synaptosomal changes. Building on DE findings implicating glutamatergic neurons, we found Chd8 (+/-) mice exhibited altered excitatory neuron spine density and dynamics, decreased GCaMP activity correlation, and sleep perturbation. Thus, Chd8 haploinsufficiency causes lasting excitatory neuron dysfunction, perturbs RNA regulation beyond transcription, and impacts neuronal properties, cortical microcircuits, and behavior.

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