Multiple facets of CBP in forebrain interneuron development

Jing Wang
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Abstract

Rubinstein–Taybi Syndrome (RTS), where the transcriptional co-activator and histone acetyltransferase CBP is mutated and haploinsufficient, is often associated with epilepsy, a disorder that is frequently due to perturbations in the generation of GABAergic interneurons and/or the inhibitory neurotransmitter GABA. Hereby, Tsui et al., recently published in Developmental Biology, asked whether CBP was necessary for the appropriate genesis and differentiation of interneurons in the murine forebrain. This paper defined multiple roles of CBP during forebrain interneuron development. In particular, CBP not only acts as a pro-differentiation factor to enhance the differentiation of ventral forebrain precursors to interneurons, but also modulates the maturation of interneurons by promoting acquisition of a GABAergic interneuron phenotype in the newborn neurons. Thus, deficits in interneuron development caused by CBP haploinsufficiency provide a potential explanation for the epilepsy seen in individuals with RTS.
CBP在前脑中间神经元发育中的多个方面
Rubinstein-Taybi综合征(RTS),其中转录共激活因子和组蛋白乙酰转移酶CBP突变且单倍不足,通常与癫痫有关,癫痫通常是由于GABA能中间神经元和/或抑制性神经递质GABA的产生受到干扰而引起的疾病。因此,Tsui等人最近发表在《发育生物学》杂志上,提出CBP对于小鼠前脑中间神经元的适当发生和分化是否必要。本文明确了CBP在前脑中间神经元发育过程中的多重作用。特别是,CBP不仅作为一种促分化因子,增强腹侧前脑向中间神经元的分化,而且还通过促进新生神经元获得gaba能中间神经元表型来调节中间神经元的成熟。因此,CBP单倍功能不全引起的中间神经元发育缺陷为RTS患者癫痫提供了一种潜在的解释。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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