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Modulation of Small RNA Signatures in Schwann-Cell-Derived Extracellular Vesicles by the p75 Neurotrophin Receptor and Sortilin

机译:P75神经营养蛋白受体和Sortilin调制Schwann-Cell衍生的细胞外囊泡中的小RNA签名

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摘要

Schwann cells (SCs) are the main glial cells of the peripheral nervous system (PNS) and are known to be involved in various pathophysiological processes, such as diabetic neuropathy and nerve regeneration, through neurotrophin signaling. Such glial trophic support to axons, as well as neuronal survival/death signaling, has previously been linked to the p75 neurotrophin receptor (p75NTR) and its co-receptor Sortilin. Recently, SC-derived extracellular vesicles (EVs) were shown to be important for axon growth and nerve regeneration, but cargo of these glial cell-derived EVs has not yet been well-characterized. In this study, we aimed to characterize signatures of small RNAs in EVs derived from wild-type (WT) SCs and define differentially expressed small RNAs in EVs derived from SCs with genetic deletions of p75NTR (Ngfr−/−) or Sortilin (Sort1−/−). Using RNA sequencing, we identified a total of 366 miRNAs in EVs derived from WT SCs of which the most highly expressed are linked to the regulation of axonogenesis, axon guidance and axon extension, suggesting an involvement of SC EVs in axonal homeostasis. Signaling of SC EVs to non-neuronal cells was also suggested by the presence of several miRNAs important for regulation of the endothelial cell apoptotic process. Ablated p75NTR or sortilin expression in SCs translated into a set of differentially regulated tRNAs and miRNAs, with impact in autophagy and several cellular signaling pathways such as the phosphatidylinositol signaling system. With this work, we identified the global expression profile of small RNAs present in SC-derived EVs and provided evidence for a regulatory function of these vesicles on the homeostasis of other cell types of the PNS. Differentially identified miRNAs can pave the way to a better understanding of p75NTR and sortilin roles regarding PNS homeostasis and disease.
机译:Schwann细胞(SCS)是外周神经系统(PNS)的主要胶质细胞,并且已知通过神经营养素信号传导涉及各种病理生理过程,例如糖尿病神经病变和神经再生。对轴突的这种胶质疏水性支持以及神经元存活/死导,先前已与P75神经营养蛋白受体(P75NTR)及其共同受体分类素相关联。最近,SC-衍生的细胞外囊泡(EVS)被证明对轴突生长和神经再生是重要的,但这些胶质细胞衍生的EV的货物尚未充分表征。在这项研究中,我们旨在表征来自野生型(WT)SCS的EVS中的小RNA的签名,并在来自P75NTR(NGFR - / - )或Sortilin的遗传缺失(Sort1- / - )。使用RNA测序,我们在来自WT SC的EV中鉴定了总共366个miRNA,其中最高表达的是与腋生发生,轴突引导和轴突延伸的调节有关,表明SC EVS在轴突稳定中的累积。还通过存在几种miRNA对内皮细胞凋亡过程的重要性来提出SC EVS至非神经元细胞的信号。将SCS中的烧蚀P75NTR或Sortilin表达转化为一组差分调节的TrNA和miRNA,具有自噬影响和几种细胞信号传导途径,例如磷脂酰肌醇信号系统。通过这项工作,我们鉴定了SC衍生EV中存在的小RNA的全局表达谱,并提供了这些囊泡对PNS其他细胞类型的稳态的调节功能的证据。差异鉴定的miRNA可以铺平道路,以更好地了解P75NTR和Sortilin角色关于PNS稳态和疾病。

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