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血管来源的 SPARC 和 SerpinE1 调节中间神经元切线迁移并加速人源干细胞源性中间神经元的功能成熟。

Vascular-derived SPARC and SerpinE1 regulate interneuron tangential migration and accelerate functional maturation of human stem cell-derived interneurons.

机构信息

Department of Pathology and Cell Biology, Columbia University, New York, United States.

Department of Neurology, Columbia University Irving Medical Center, New York, United States.

出版信息

Elife. 2021 Apr 27;10:e56063. doi: 10.7554/eLife.56063.

Abstract

Cortical interneurons establish inhibitory microcircuits throughout the neocortex and their dysfunction has been implicated in epilepsy and neuropsychiatric diseases. Developmentally, interneurons migrate from a distal progenitor domain in order to populate the neocortex - a process that occurs at a slower rate in humans than in mice. In this study, we sought to identify factors that regulate the rate of interneuron maturation across the two species. Using embryonic mouse development as a model system, we found that the process of initiating interneuron migration is regulated by blood vessels of the medial ganglionic eminence (MGE), an interneuron progenitor domain. We identified two endothelial cell-derived paracrine factors, SPARC and SerpinE1, that enhance interneuron migration in mouse MGE explants and organotypic cultures. Moreover, pre-treatment of human stem cell-derived interneurons (hSC-interneurons) with SPARC and SerpinE1 prior to transplantation into neonatal mouse cortex enhanced their migration and morphological elaboration in the host cortex. Further, SPARC and SerpinE1-treated hSC-interneurons also exhibited more mature electrophysiological characteristics compared to controls. Overall, our studies suggest a critical role for CNS vasculature in regulating interneuron developmental maturation in both mice and humans.

摘要

皮质中间神经元在整个新皮层中建立抑制性微电路,其功能障碍与癫痫和神经精神疾病有关。在发育过程中,中间神经元从远端祖细胞区域迁移,以填充新皮层——这一过程在人类中的速度比在小鼠中慢。在这项研究中,我们试图确定调节两种物种中间神经元成熟速度的因素。我们使用胚胎期小鼠发育作为模型系统,发现中间神经元迁移的起始过程受内侧神经节隆起(MGE)血管的调节,MGE 是中间神经元祖细胞区域。我们鉴定了两种内皮细胞衍生的旁分泌因子,即 SPARC 和 SerpinE1,它们增强了小鼠 MGE 外植体和器官型培养物中中间神经元的迁移。此外,在将 SPARC 和 SerpinE1 预处理过的人源性干细胞源性中间神经元(hSC-interneurons)移植到新生小鼠皮层之前,它们在宿主皮层中的迁移和形态发育得到了增强。此外,与对照组相比,经 SPARC 和 SerpinE1 处理的 hSC-interneurons 还表现出更成熟的电生理特征。总的来说,我们的研究表明中枢神经系统血管在调节小鼠和人类中间神经元发育成熟方面起着关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9cdb/8099424/185d84146540/elife-56063-fig1.jpg

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