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Sox3 基因缺失突变体中的脑垂体功能减退与正中隆起处 NG2 神经胶质的改变有关,并且受阿司匹林和肠道微生物群的影响。

Hypopituitarism in Sox3 null mutants correlates with altered NG2-glia in the median eminence and is influenced by aspirin and gut microbiota.

机构信息

Stem Cell Biology and Developmental Genetics Lab, The Francis Crick Institute, London, United Kingdom.

Neurobiological Research Facility, UCL Sainsbury Wellcome Centre for Neural Circuits and Behaviour, London, United Kingdom.

出版信息

PLoS Genet. 2024 Sep 26;20(9):e1011395. doi: 10.1371/journal.pgen.1011395. eCollection 2024 Sep.

Abstract

The median eminence (ME), located at the base of the hypothalamus, is an essential centre of information exchange between the brain and the pituitary. We and others previously showed that mutations and duplications affecting the transcription factor SOX3/Sox3 result in hypopituitarism, and this is likely of hypothalamic origin. We demonstrate here that the absence of Sox3 predominantly affects the ME with phenotypes that first occur in juvenile animals, despite the embryonic onset of SOX3 expression. In the pituitary, reduction in hormone levels correlates with a lack of endocrine cell maturation. In parallel, ME NG2-glia renewal and oligodendrocytic differentiation potential are affected. We further show that low-dose aspirin treatment, which is known to affect NG2-glia, or changes in gut microbiota, rescue both proliferative defects and hypopituitarism in Sox3 mutants. Our study highlights a central role of NG2-glia for ME function during a transitional period of post-natal development and indicates their sensitivity to extrinsic signals.

摘要

正中隆起(ME)位于下丘脑底部,是大脑和垂体之间信息交换的重要中心。我们和其他人之前的研究表明,影响转录因子 SOX3/Sox3 的突变和重复会导致垂体功能减退,这可能是下丘脑起源的。我们在这里证明,尽管 SOX3 的表达在胚胎期就开始了,但 Sox3 的缺失主要影响 ME,其表型首先出现在幼年动物中。在垂体中,激素水平的降低与内分泌细胞成熟的缺乏有关。与此平行的是,ME 的 NG2-胶质细胞更新和少突胶质细胞分化潜能受到影响。我们进一步表明,低剂量阿司匹林治疗(已知会影响 NG2-胶质细胞)或肠道微生物群的改变,可以挽救 Sox3 突变体的增殖缺陷和垂体功能减退。我们的研究强调了 NG2-胶质细胞在出生后发育的过渡时期对 ME 功能的核心作用,并表明它们对外界信号敏感。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c99c/11426531/237e104b4499/pgen.1011395.g001.jpg

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