具有认知缺陷和自闭症特征的ATRX缺陷小鼠模型。

IF 4.1 2区 医学 Q1 CLINICAL NEUROLOGY
Katherine M Quesnel, Nicole Martin-Kenny, Nathalie G Bérubé
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引用次数: 0

摘要

背景:ATRX是一种依赖atp的染色质重塑蛋白,在保护基因组完整性和调节基因表达方面发挥重要作用。这种蛋白质的缺乏导致ATR-X综合征,这是一种以智力残疾和一系列发育异常为特征的疾病,包括自闭症的特征。先前的研究表明,在出生后删除小鼠前脑兴奋神经元中的ATRX会导致雄性特异性记忆缺陷,但不会出现明显的自闭症样行为。方法:我们培育了前脑兴奋性神经元中ATRX在胚胎早期缺失的小鼠,并使用一系列记忆和自闭症相关的范式来表征它们的行为。结果:我们发现突变小鼠表现出更广泛的损伤,包括恐惧记忆,减少焦虑样行为,多动,以及自残和重复梳理。性别特异性的改变也被观察到,包括男性特异性的攻击性、感觉门控障碍和社会记忆下降。结论:总的来说,这些发现表明,由前脑兴奋性神经元中ATRX缺乏引起的早期发育异常有助于出现恐惧记忆缺陷和自闭症样行为。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A mouse model of ATRX deficiency with cognitive deficits and autistic traits.

Background: ATRX is an ATP-dependent chromatin remodeling protein with essential roles in safeguarding genome integrity and modulating gene expression. Deficiencies in this protein cause ATR-X syndrome, a condition characterized by intellectual disability and an array of developmental abnormalities, including features of autism. Previous studies demonstrated that deleting ATRX in mouse forebrain excitatory neurons postnatally resulted in male-specific memory deficits, but no apparent autistic-like behaviours.

Methods: We generated mice with an earlier embryonic deletion of ATRX in forebrain excitatory neurons and characterized their behaviour using a series of memory and autistic-related paradigms.

Results: We found that mutant mice displayed a broader spectrum of impairments, including fear memory, decreased anxiety-like behaviour, hyperactivity, as well as self-injurious and repetitive grooming. Sex-specific alterations were also observed, including male-specific aggression, sensory gating impairments, and decreased social memory.

Conclusions: Collectively, the findings indicate that early developmental abnormalities arising from ATRX deficiency in forebrain excitatory neurons contribute to the presentation of fear memory deficits as well as autistic-like behaviours.

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来源期刊
CiteScore
7.60
自引率
4.10%
发文量
58
审稿时长
>12 weeks
期刊介绍: Journal of Neurodevelopmental Disorders is an open access journal that integrates current, cutting-edge research across a number of disciplines, including neurobiology, genetics, cognitive neuroscience, psychiatry and psychology. The journal’s primary focus is on the pathogenesis of neurodevelopmental disorders including autism, fragile X syndrome, tuberous sclerosis, Turner Syndrome, 22q Deletion Syndrome, Prader-Willi and Angelman Syndrome, Williams syndrome, lysosomal storage diseases, dyslexia, specific language impairment and fetal alcohol syndrome. With the discovery of specific genes underlying neurodevelopmental syndromes, the emergence of powerful tools for studying neural circuitry, and the development of new approaches for exploring molecular mechanisms, interdisciplinary research on the pathogenesis of neurodevelopmental disorders is now increasingly common. Journal of Neurodevelopmental Disorders provides a unique venue for researchers interested in comparing and contrasting mechanisms and characteristics related to the pathogenesis of the full range of neurodevelopmental disorders, sharpening our understanding of the etiology and relevant phenotypes of each condition.
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