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新生儿小胶质细胞的定位决定小细胞外囊泡的内容物及生物学功能。

Location of neonatal microglia drives small extracellular vesicles content and biological functions .

作者信息

Murgoci Adriana-Natalia, Duhamel Marie, Raffo-Romero Antonella, Mallah Khalil, Aboulouard Soulaimane, Lefebvre Christophe, Kobeissy Firas, Fournier Isabelle, Zilkova Monika, Maderova Denisa, Cizek Milan, Cizkova Dasa, Salzet Michel

机构信息

Inserm, U-1192 - Laboratoire Protéomique, Réponse Inflammatoire et Spectrométrie de Masse-PRISM, Université Lille, Villeneuve d'Ascq, France.

Institute of Neuroimmunology, Slovak Academy of Sciences, Bratislava, Slovakia.

出版信息

J Extracell Vesicles. 2020 Feb 18;9(1):1727637. doi: 10.1080/20013078.2020.1727637. eCollection 2020.

Abstract

Combining proteomics and systems biology approaches, we demonstrate that neonatal microglial cells derived from two different CNS locations, cortex and spinal cord, and cultured displayed different phenotypes upon different physiological or pathological conditions. These cells also exhibited greater variability in terms of cellular and small extracellular vesicles (sEVs) protein content and levels. Bioinformatic data analysis showed that cortical microglia exerted anti-inflammatory and neurogenesis/tumorigenesis properties, while the spinal cord microglia were more inflammatory. Interestingly, while both sEVs microglia sources enhanced growth of DRGs processes, only the spinal cord-derived sEVs microglia under LPS stimulation significantly attenuated glioma proliferation. These results were confirmed using the neurite outgrowth assay on DRGs cells and glioma proliferation analysis in 3D spheroid cultures. Results from these assays suggest that the microglia localized at different CNS regions can ensure different biological functions. Together, this study indicates that neonatal microglia locations regulate their physiological and pathological functional fates and could affect the high prevalence of brain vs spinal cord gliomas in adults.

摘要

结合蛋白质组学和系统生物学方法,我们证明,源自中枢神经系统两个不同位置(皮层和脊髓)并进行培养的新生小胶质细胞,在不同的生理或病理条件下表现出不同的表型。这些细胞在细胞和小细胞外囊泡(sEVs)蛋白质含量和水平方面也表现出更大的变异性。生物信息数据分析表明,皮层小胶质细胞具有抗炎和神经发生/肿瘤发生特性,而脊髓小胶质细胞则更具炎症性。有趣的是,虽然来自两种小胶质细胞来源的sEVs均能促进背根神经节(DRG)突起的生长,但只有在脂多糖(LPS)刺激下脊髓来源的sEVs小胶质细胞能显著减弱胶质瘤增殖。使用DRG细胞的神经突生长试验和三维球体培养中的胶质瘤增殖分析证实了这些结果。这些试验结果表明,位于中枢神经系统不同区域的小胶质细胞可以确保不同的生物学功能。总之,本研究表明,新生小胶质细胞的位置调节其生理和病理功能命运,并可能影响成人脑胶质瘤与脊髓胶质瘤的高发病率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/82ea/7049881/1c121b80a87a/ZJEV_A_1727637_F0001_OC.jpg

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