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星形胶质细胞中转录因子Trps1和Sox9的单细胞缺失揭示了成年大脑皮质中的新功能。

Single Cell Deletion of the Transcription Factors Trps1 and Sox9 in Astrocytes Reveals Novel Functions in the Adult Cerebral Cortex.

作者信息

Natarajan Poornemaa, Koupourtidou Christina, de Resseguier Thibault, Thorwirth Manja, Bocchi Riccardo, Fischer-Sternjak Judith, Gleiss Sarah, Rodrigues Diana, Myoga Michael H, Ninkovic Jovica, Masserdotti Giacomo, Götz Magdalena

机构信息

Biomedical Center Munich, Department of Physiological Genomics, LMU Munich, Martinsried, Germany.

Institute for Stem Cell Research, Helmholtz Center Munich, German Research Center for Environmental Health (GmbH), Neuherberg, Germany.

出版信息

Glia. 2025 Apr;73(4):737-758. doi: 10.1002/glia.24645. Epub 2024 Nov 28.

Abstract

Astrocytes play key roles in brain function, but how these are orchestrated by transcription factors (TFs) in the adult brain and aligned with astrocyte heterogeneity is largely unknown. Here we examined the localization and function of the novel astrocyte TF Trps1 (Transcriptional Repressor GATA Binding 1) and the well-known astrocyte TF Sox9 by Cas9-mediated deletion using Mokola-pseudotyped lentiviral delivery into the adult cerebral cortex. Trps1 and Sox9 levels showed heterogeneity among adult cortical astrocytes, which prompted us to explore the effects of deleting either Sox9 or Trps1 alone or simultaneously at the single-cell (by patch-based single-cell transcriptomics) and tissue levels (by spatial transcriptomics). This revealed TF-specific functions in astrocytes, such as synapse maintenance with the strongest effects on synapse number achieved by Trps1 deletion and a common effect on immune response. In addition, spatial transcriptomics showed non-cell-autonomous effects on the surrounding cells, such as oligodendrocytes and other immune cells with TF-specific differences on the type of immune cells: Trps1 deletion affecting monocytes specifically, while Sox9 deletion acting mostly on microglia and deletion of both TF affecting mostly B cells. Taken together, this study reveals novel roles of Trps1 and Sox9 in adult astrocytes and their communication with other glial and immune cells.

摘要

星形胶质细胞在脑功能中发挥关键作用,但在成体大脑中这些作用是如何由转录因子(TFs)协调并与星形胶质细胞的异质性相匹配的,目前尚不清楚。在这里,我们通过使用莫科拉假型慢病毒载体将其递送至成体大脑皮层,利用Cas9介导的缺失来研究新型星形胶质细胞转录因子Trps1(转录抑制因子GATA结合蛋白1)和著名的星形胶质细胞转录因子Sox9的定位和功能。Trps1和Sox9水平在成体皮质星形胶质细胞中表现出异质性,这促使我们在单细胞水平(通过基于膜片钳的单细胞转录组学)和组织水平(通过空间转录组学)探索单独或同时缺失Sox9或Trps1的影响。这揭示了转录因子在星形胶质细胞中的特定功能,例如突触维持,其中Trps1缺失对突触数量的影响最强,以及对免疫反应的共同影响。此外,空间转录组学显示对周围细胞有非细胞自主性影响,如少突胶质细胞和其他免疫细胞,在免疫细胞类型上存在转录因子特异性差异:Trps1缺失特异性影响单核细胞,而Sox9缺失主要作用于小胶质细胞,两者都缺失主要影响B细胞。综上所述,本研究揭示了Trps1和Sox9在成体星形胶质细胞中的新作用及其与其他神经胶质细胞和免疫细胞的相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec98/11845849/897243a49062/GLIA-73-737-g001.jpg

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