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20-α 羟胆固醇,人乳中的一种氧化固醇,通过 Gli 依赖性少突胶质细胞生成逆转小鼠新生期脑白质损伤。

20-αHydroxycholesterol, an oxysterol in human breast milk, reverses mouse neonatal white matter injury through Gli-dependent oligodendrogenesis.

机构信息

Division of Neonatology, Department of Pediatrics, Duke University Medical Center, The Jean and George Brumley, Jr. Neonatal-Perinatal Institute, Durham, NC 27710, USA.

Duke Proteomics and Metabolomics Shared Resource, Center for Genomics and Computational Biology, School of Medicine, Duke University Medical Center, Durham, NC 27710, USA.

出版信息

Cell Stem Cell. 2023 Aug 3;30(8):1054-1071.e8. doi: 10.1016/j.stem.2023.07.010.

Abstract

White matter injuries (WMIs) are the leading cause of neurologic impairment in infants born premature. There are no treatment options available. The most common forms of WMIs in infants occur prior to the onset of normal myelination, making its pathophysiology distinctive, thus requiring a tailored approach to treatment. Neonates present a unique opportunity to repair WMIs due to a transient abundance of neural stem/progenitor cells (NSPCs) present in the germinal matrix with oligodendrogenic potential. We identified an endogenous oxysterol, 20-αHydroxycholesterol (20HC), in human maternal breast milk that induces oligodendrogenesis through a sonic hedgehog (shh), Gli-dependent mechanism. Following WMI in neonatal mice, injection of 20HC induced subventricular zone-derived oligodendrogenesis and improved myelination in the periventricular white matter, resulting in improved motor outcomes. Targeting the oligodendrogenic potential of postnatal NSPCs in neonates with WMIs may be further developed into a novel approach to mitigate this devastating complication of preterm birth.

摘要

脑白质损伤(WMIs)是早产儿神经功能障碍的主要原因。目前尚无治疗方法。婴儿最常见的 WMIs 发生在正常髓鞘形成之前,其病理生理学特征独特,因此需要针对治疗方法进行调整。由于新生儿的生发基质中存在短暂的大量具有少突胶质细胞生成潜力的神经干细胞/祖细胞(NSPCs),因此他们为修复 WMIs 提供了独特的机会。我们在人类母乳中发现了一种内源性的氧化固醇 20-α-羟胆固醇(20HC),它通过 sonic hedgehog(shh)、Gli 依赖性机制诱导少突胶质细胞分化。在新生小鼠发生 WMIs 后,注射 20HC 可诱导侧脑室下区来源的少突胶质细胞分化,并改善脑室周围白质的髓鞘形成,从而改善运动功能。针对 WMIs 新生儿的 NSPCs 的少突胶质细胞生成潜能,可能进一步发展为减轻早产儿出生这一毁灭性并发症的新方法。

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