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早期 IGF-1 受体抑制在小鼠中模拟了早产人类大脑疾病,并揭示了一个治疗靶点。

Early IGF-1 receptor inhibition in mice mimics preterm human brain disorders and reveals a therapeutic target.

机构信息

Brain Development and Disease Laboratory, Istituto Italiano di Tecnologia, via Morego, 30, 16163 Genoa, Italy.

Università degli Studi di Genova, via Balbi, 5, 16126 Genoa, Italy.

出版信息

Sci Adv. 2024 Mar;10(9):eadk8123. doi: 10.1126/sciadv.adk8123. Epub 2024 Mar 1.

Abstract

Besides recent advances in neonatal care, preterm newborns still develop sex-biased behavioral alterations. Preterms fail to receive placental insulin-like growth factor-1 (IGF-1), a major fetal growth hormone in utero, and low IGF-1 serum levels correlate with preterm poor neurodevelopmental outcomes. Here, we mimicked IGF-1 deficiency of preterm newborns in mice by perinatal administration of an IGF-1 receptor antagonist. This resulted in sex-biased brain microstructural, functional, and behavioral alterations, resembling those of ex-preterm children, which we characterized performing parallel mouse/human behavioral tests. Pharmacological enhancement of GABAergic tonic inhibition by the U.S. Food and Drug Administration-approved drug ganaxolone rescued functional/behavioral alterations in mice. Establishing an unprecedented mouse model of prematurity, our work dissects the mechanisms at the core of abnormal behaviors and identifies a readily translatable therapeutic strategy for preterm brain disorders.

摘要

除了新生儿护理方面的最新进展,早产儿仍然存在性别偏向的行为改变。早产儿无法获得胎盘胰岛素样生长因子-1(IGF-1),IGF-1 是胎儿在子宫内的主要生长激素,而低 IGF-1 血清水平与早产儿神经发育不良结果相关。在这里,我们通过围产期给予 IGF-1 受体拮抗剂在小鼠中模拟早产儿 IGF-1 缺乏症。这导致了性别偏向的大脑微观结构、功能和行为改变,类似于早产儿儿童的情况,我们通过进行平行的小鼠/人类行为测试来描述这些改变。美国食品和药物管理局批准的药物加巴喷丁通过增强 GABA 能紧张抑制的药理学作用,挽救了小鼠的功能/行为改变。通过建立一个前所未有的早产小鼠模型,我们的工作剖析了异常行为的核心机制,并确定了一种可转化为治疗早产儿脑疾病的策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4538/10906931/83cfeadee60f/sciadv.adk8123-f1.jpg

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