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在幼年期,慢性亚惊厥活动会导致自闭症行为,而在青少年断奶期不会产生神经毒性。

Chronic subconvulsive activity during early postnatal life produces autistic behavior in the absence of neurotoxicity in the juvenile weanling period.

机构信息

Department of Cell Biology & Anatomy, New York Medical College, Valhalla, NY, 10595, United States.

Department of Cell Biology & Anatomy, New York Medical College, Valhalla, NY, 10595, United States.

出版信息

Behav Brain Res. 2019 Nov 18;374:112046. doi: 10.1016/j.bbr.2019.112046. Epub 2019 Jul 31.

DOI:10.1016/j.bbr.2019.112046
PMID:31376443
Abstract

The diagnosis of autism spectrum disorder (ASD) varies from very mild to severe social and cognitive impairments. We hypothesized that epigenetic subconvulsive activity in early postnatal life may contribute to the development of autistic behavior in a sex-related manner. Low doses of kainic acid (KA) (25-100 μg) were administered to rat pups for 15 days beginning on postnatal (P) day 6 to chronically elevate neuronal activity. A battery of classical and novel behavioral tests was used, and sex differences were observed. Our novel open handling test revealed that ASD males nose poked more often and ASD females climbed and escaped more frequently with age. In the social interaction test, ASD males were less social than ASD females who were more anxious in handling and elevated plus maze (EPM) tasks. To evaluate group dynamics, sibling and non-sibling control and experimental animals explored 3 different shaped novel social environments. Control pups huddled quickly and more frequently in all environments whether they socialized with littermates or non-siblings compared to ASD groups. Non-sibling ASD pups were erratic and huddled in smaller groups. In the object recognition test, only ASD males spent less time with the novel object compared to control pups. Data suggest that chronic subconvulsive activity in early postnatal life leads to an ASD phenotype in the absence of cell death. Males were more susceptible to developing asocial behaviors and cognitive pathologies, whereas females were prone to higher levels of hyperactivity and anxiety, validating our postnatal ASD model apparent in the pre-juvenile period.

摘要

自闭症谱系障碍(ASD)的诊断范围从非常轻微到严重的社交和认知障碍。我们假设,早期产后生活中的表观遗传亚惊厥活动可能以性别相关的方式导致自闭症行为的发展。低剂量的海人酸(KA)(25-100μg)在出生后第 6 天开始连续 15 天给予幼鼠,以慢性提高神经元活动。使用了一系列经典和新颖的行为测试,并观察到了性别差异。我们新颖的开放式处理测试表明,ASD 雄性老鼠的鼻子戳的次数更多,而 ASD 雌性老鼠的攀爬和逃避次数更多,随着年龄的增长而增加。在社会互动测试中,ASD 雄性老鼠比 ASD 雌性老鼠更不社交,后者在处理和高架十字迷宫(EPM)任务中更焦虑。为了评估群体动态,兄弟姐妹和非兄弟姐妹对照组和实验组动物探索了 3 种不同形状的新颖社交环境。与 ASD 组相比,对照组幼鼠在所有环境中都更快、更频繁地聚集在一起,无论它们是与同窝幼鼠还是非兄弟姐妹社交。非兄弟姐妹 ASD 幼鼠行为不稳定,聚集在较小的群体中。在物体识别测试中,只有 ASD 雄性老鼠与对照组幼鼠相比,花在新物体上的时间更少。数据表明,早期产后生活中的慢性亚惊厥活动导致 ASD 表型,而没有细胞死亡。雄性更容易发展出社交行为和认知病理学,而雌性则更容易出现更高水平的多动和焦虑,验证了我们在青春期前出现的产后 ASD 模型。

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