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神经元微小RNA-17-5p导致产前酒精暴露引起的半球间皮质连接缺陷。

Neuronal miR-17-5p contributes to interhemispheric cortical connectivity defects induced by prenatal alcohol exposure.

作者信息

Altounian Mike, Bellon Anaïs, Mann Fanny

机构信息

Aix Marseille University, CNRS, IBDM, Marseille, France.

Aix Marseille University, INSERM, INMED, Marseille, France.

出版信息

Cell Rep. 2023 Sep 26;42(9):113020. doi: 10.1016/j.celrep.2023.113020. Epub 2023 Aug 22.

Abstract

Structural and functional deficits in brain connectivity are reported in patients with fetal alcohol spectrum disorders (FASDs), but whether and how prenatal alcohol exposure (PAE) affects axonal development of neurons and disrupts wiring between brain regions is unknown. Here, we develop a mouse model of moderate alcohol exposure during prenatal brain wiring to study the effects of PAE on corpus callosum (CC) development. PAE induces aberrant navigation of interhemispheric CC axons that persists even after exposure ends, leading to ectopic termination in the contralateral cortex. The neuronal miR-17-5p and its target ephrin type A receptor 4 (EphA4) mediate the effect of alcohol on the contralateral targeting of CC axons. Thus, altered microRNA-mediated regulation of axonal guidance may have implications for interhemispheric cortical connectivity and associated behaviors in FASD.

摘要

胎儿酒精谱系障碍(FASDs)患者存在大脑连接的结构和功能缺陷,但产前酒精暴露(PAE)是否以及如何影响神经元的轴突发育并破坏脑区之间的布线尚不清楚。在这里,我们建立了一个在产前脑布线期间适度酒精暴露的小鼠模型,以研究PAE对胼胝体(CC)发育的影响。PAE诱导半球间CC轴突的异常导航,即使在暴露结束后仍持续存在,导致在对侧皮质的异位终止。神经元miR-17-5p及其靶标 Ephrin A 型受体 4(EphA4)介导酒精对CC轴突对侧靶向的影响。因此,微小RNA介导的轴突导向调节改变可能对FASD中的半球间皮质连接和相关行为有影响。

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