| Literature DB >> 30104731 |
Hwajin Jung1, Haram Park2, Yeonsoo Choi2, Hyojin Kang3, Eunee Lee1, Hanseul Kweon2, Junyeop Daniel Roh2, Jacob Ellegood4, Woochul Choi5, Jaeseung Kang2, Issac Rhim1, Su-Yeon Choi1, Mihyun Bae1, Sun-Gyun Kim1, Jiseok Lee1, Changuk Chung2, Taesun Yoo2, Hanwool Park6, Yangsik Kim6, Seungmin Ha2, Seung Min Um2, Seojung Mo7, Yonghan Kwon2, Won Mah8, Yong Chul Bae8, Hyun Kim7, Jason P Lerch4,9, Se-Bum Paik5, Eunjoon Kim10,11.
Abstract
Autism spectrum disorders (ASDs) are four times more common in males than in females, but the underlying mechanisms are poorly understood. We characterized sexually dimorphic changes in mice carrying a heterozygous mutation in Chd8 (Chd8+/N2373K) that was first identified in human CHD8 (Asn2373LysfsX2), a strong ASD-risk gene that encodes a chromatin remodeler. Notably, although male mutant mice displayed a range of abnormal behaviors during pup, juvenile, and adult stages, including enhanced mother-seeking ultrasonic vocalization, enhanced attachment to reunited mothers, and isolation-induced self-grooming, their female counterparts do not. This behavioral divergence was associated with sexually dimorphic changes in neuronal activity, synaptic transmission, and transcriptomic profiles. Specifically, female mice displayed suppressed baseline neuronal excitation, enhanced inhibitory synaptic transmission and neuronal firing, and increased expression of genes associated with extracellular vesicles and the extracellular matrix. Our results suggest that a human CHD8 mutation leads to sexually dimorphic changes ranging from transcription to behavior in mice.Entities:
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Year: 2018 PMID: 30104731 DOI: 10.1038/s41593-018-0208-z
Source DB: PubMed Journal: Nat Neurosci ISSN: 1097-6256 Impact factor: 24.884