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海姆达尔,一种源自与星形胶质细胞免疫球蛋白 κ 轻链可变区相关的 ncRNA 的替代蛋白:神经蛋白质组中的新成员。

Heimdall, an alternative protein issued from a ncRNA related to kappa light chain variable region of immunoglobulins from astrocytes: a new player in neural proteome.

机构信息

Univ. Lille, Inserm, U-1192 - Laboratoire Protéomique, Réponse Inflammatoire et Spectrométrie de Masse-PRISM, F-59000, Lille, France.

Institute of Neuroimmunology, Slovak Academy of Sciences, Dúbravská cesta 9, 845 10, Bratislava, Slovakia.

出版信息

Cell Death Dis. 2023 Aug 16;14(8):526. doi: 10.1038/s41419-023-06037-y.

Abstract

The dogma "One gene, one protein" is clearly obsolete since cells use alternative splicing and generate multiple transcripts which are translated into protein isoforms, but also use alternative translation initiation sites (TISs) and termination sites on a given transcript. Alternative open reading frames for individual transcripts give proteins originate from the 5'- and 3'-UTR mRNA regions, frameshifts of mRNA ORFs or from non-coding RNAs. Longtime considered as non-coding, recent in-silico translation prediction methods enriched the protein databases allowing the identification of new target structures that have not been identified previously. To gain insight into the role of these newly identified alternative proteins in the regulation of cellular functions, it is crucial to assess their dynamic modulation within a framework of altered physiological modifications such as experimental spinal cord injury (SCI). Here, we carried out a longitudinal proteomic study on rat SCI from 12 h to 10 days. Based on the alternative protein predictions, it was possible to identify a plethora of newly predicted protein hits. Among these proteins, some presented a special interest due to high homology with variable chain regions of immunoglobulins. We focus our interest on the one related to Kappa variable light chains which is similarly highly produced by B cells in the Bence jones disease, but here expressed in astrocytes. This protein, name Heimdall is an Intrinsically disordered protein which is secreted under inflammatory conditions. Immunoprecipitation experiments showed that the Heimdall interactome contained proteins related to astrocyte fate keepers such as "NOTCH1, EPHA3, IPO13" as well as membrane receptor protein including "CHRNA9; TGFBR, EPHB6, and TRAM". However, when Heimdall protein was neutralized utilizing a specific antibody or its gene knocked out by CRISPR-Cas9, sprouting elongations were observed in the corresponding astrocytes. Interestingly, depolarization assays and intracellular calcium measurements in Heimdall KO, established a depolarization effect on astrocyte membranes KO cells were more likely that the one found in neuroprogenitors. Proteomic analyses performed under injury conditions or under lipopolysaccharides (LPS) stimulation, revealed the expression of neuronal factors, stem cell proteins, proliferation, and neurogenesis of astrocyte convertor factors such as EPHA4, NOTCH2, SLIT3, SEMA3F, suggesting a role of Heimdall could regulate astrocytic fate. Taken together, Heimdall could be a novel member of the gatekeeping astrocyte-to-neuroprogenitor conversion factors.

摘要

“一个基因,一个蛋白质”的教条显然已经过时,因为细胞使用选择性剪接并产生多个转录本,这些转录本被翻译为蛋白质同工型,但也使用给定转录本上的选择性翻译起始位点(TIS)和终止位点。单个转录本的选择性开放阅读框赋予蛋白质起源于 5'-和 3'-UTR mRNA 区域、mRNA ORF 的移码或非编码 RNA。长期以来被认为是非编码的,最近的计算机翻译预测方法丰富了蛋白质数据库,允许识别以前未识别的新靶结构。为了深入了解这些新鉴定的选择性蛋白质在细胞功能调节中的作用,必须在生理改变的框架内评估它们的动态调制,例如实验性脊髓损伤(SCI)。在这里,我们对大鼠 SCI 从 12 小时到 10 天进行了纵向蛋白质组学研究。基于选择性蛋白质预测,有可能鉴定出大量新的预测蛋白。在这些蛋白质中,由于与免疫球蛋白可变链区域具有高度同源性,一些蛋白质特别引人注目。我们对与 Kappa 可变轻链相关的蛋白质感兴趣,该蛋白质在 B 细胞多发性骨髓瘤中也由 B 细胞高度产生,但在此表达在星形胶质细胞中。这种名为 Heimdall 的蛋白质是一种内在无序的蛋白质,在炎症条件下分泌。免疫沉淀实验表明,Heimdall 的相互作用组包含与星形胶质细胞命运保持者相关的蛋白质,如“NOTCH1、EPHA3、IPO13”以及包括“CHRNA9;TGFBR、EPHB6 和 TRAM”在内的膜受体蛋白。然而,当利用特异性抗体中和 Heimdall 蛋白或利用 CRISPR-Cas9 敲除其基因时,在相应的星形胶质细胞中观察到突起伸长。有趣的是,Heimdall KO 中的去极化测定和细胞内钙测量表明星形胶质细胞膜 KO 细胞的去极化效应更有可能是神经祖细胞中发现的去极化效应。在损伤条件下或脂多糖(LPS)刺激下进行的蛋白质组学分析揭示了神经元因子、干细胞蛋白、增殖和星形胶质细胞转化因子的神经发生的表达,如 EPHA4、NOTCH2、SLIT3、SEMA3F,表明 Heimdall 的作用可能调节星形胶质细胞命运。总之,Heimdall 可能是门控星形胶质细胞向神经祖细胞转化因子的新成员。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6b87/10432539/57dd674d10c0/41419_2023_6037_Fig1_HTML.jpg

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