成年Chd8单倍体不足小鼠持续皮质兴奋性神经元失调。

bioRxiv : the preprint server for biology Pub Date : 2025-07-17 DOI:10.1101/2025.06.04.657776

Cesar P Canales, Stephanie A Lozano, Nicholas A Frost, Karol Cichewicz, Wellington Amaral, Nicolas Seban, Ethan Fenton, Ayanna Wade, Nickolas Chu, Emily Smith, Cory Ardekani, Samuel Frank, Jeffrey Bennett, Pierre Lavenex, Aspen Kopley-Smith, Darlene Rahbarian, Melissa Corea, Daniela Perla, Liam Davis, Jiyuan Zhu, Rebecca Ortiz, Paris Beauregard, Sarah Morse, Jacob Baker, Jingqi Sun, Boxuan Ma, Ju Lu, Vikaas S Sohal, David G Amaral, Yi Zuo, Alex S Nord

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引用次数: 0

摘要

CHD8突变导致自闭症谱系障碍、认知缺陷和大头畸形。Chd8 +/-小鼠模型表现出大头畸形和转录病理，在神经发生、神经元功能和行为方面的发现不一致。通过体视学和单核转录组学（snRNA-seq），我们发现Chd8 +/-皮质体积的增加与神经元数量的增加无关。皮质细胞类型存在差异表达（DE），兴奋性神经元表现出高DE负担和共享和亚类特异性DE特征。组成型Chd8 +/-小鼠和条件型Camk2a-Cre Chd8 +/-小鼠的大量RNA-seq DE鉴定出共同的转录病理。突触体与核mRNA的DE发现了重叠的deg，但也有显著差异和夸大的突触体变化。基于与谷氨酸能神经元相关的DE发现，我们发现Chd8 +/-小鼠表现出兴奋性神经元脊柱密度和动力学改变，GCaMP活性相关性降低，睡眠扰动。因此，Chd8单倍体功能不全导致持久的兴奋性神经元功能障碍，干扰转录以外的RNA调节，并影响神经元特性、皮质微回路和行为。

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Persistent cortical excitatory neuron dysregulation in adult Chd8 haploinsufficient mice.

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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