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外泌体和羊驼(Lama glama)血清中的脱酰化蛋白——对骆驼科动物免疫的新认识。

Deiminated proteins in extracellular vesicles and serum of llama (Lama glama)-Novel insights into camelid immunity.

机构信息

Comparative Immunogenetics Laboratory, Department of Veterinary Pathobiology, College of Veterinary Medicine and Biomedical Sciences, Texas A&M University, College Station, TX, 77843, USA; Department of Microbial Pathogenesis and Immunology, College of Medicine, Texas A&M Health Science Center, Texas A&M University, College Station, TX, 77843, USA.

Electron Microscopy Suite, Faculty of Science, Technology, Engineering and Mathematics, Open University, Milton Keynes, MK7 6AA, UK.

出版信息

Mol Immunol. 2020 Jan;117:37-53. doi: 10.1016/j.molimm.2019.10.017. Epub 2019 Nov 13.

Abstract

Peptidylarginine deiminases (PADs) are phylogenetically conserved calcium-dependent enzymes which post-translationally convert arginine into citrulline in target proteins in an irreversible manner, causing functional and structural changes in target proteins. Protein deimination causes generation of neo-epitopes, affects gene regulation and also allows for protein moonlighting. Furthermore, PADs have been found to be a phylogenetically conserved regulator for extracellular vesicle (EVs) release. EVs are found in most body fluids and participate in cellular communication via transfer of cargo proteins and genetic material. In this study, post-translationally deiminated proteins in serum and serum-EVs are described for the first time in camelids, using the llama (Lama glama L. 1758) as a model animal. We report a poly-dispersed population of llama serum EVs, positive for phylogenetically conserved EV-specific markers and characterised by TEM. In serum, 103 deiminated proteins were overall identified, including key immune and metabolic mediators including complement components, immunoglobulin-based nanobodies, adiponectin and heat shock proteins. In serum, 60 deiminated proteins were identified that were not in EVs, and 25 deiminated proteins were found to be unique to EVs, with 43 shared deiminated protein hits between both serum and EVs. Deiminated histone H3, a marker of neutrophil extracellular trap formation, was also detected in llama serum. PAD homologues were identified in llama serum by Western blotting, via cross reaction with human PAD antibodies, and detected at an expected 70 kDa size. This is the first report of deiminated proteins in serum and EVs of a camelid species, highlighting a hitherto unrecognized post-translational modification in key immune and metabolic proteins in camelids, which may be translatable to and inform a range of human metabolic and inflammatory pathologies.

摘要

肽基精氨酸脱亚氨酶(PADs)是进化上保守的、依赖钙的酶,可将靶蛋白中的精氨酸不可逆地转化为瓜氨酸,导致靶蛋白的功能和结构发生变化。蛋白质脱亚氨基作用会产生新的表位,影响基因调控,也允许蛋白质兼职。此外,PADs 被发现是细胞外囊泡(EVs)释放的进化上保守的调节剂。EVs 存在于大多数体液中,并通过转移货物蛋白和遗传物质参与细胞间通讯。在这项研究中,首次在骆驼科动物中描述了血清和血清-EVs 中的翻译后脱亚氨基蛋白,使用美洲驼(Lama glama L. 1758)作为模型动物。我们报告了一种多分散的美洲驼血清 EV 群体,对进化上保守的 EV 特异性标志物呈阳性,并通过 TEM 进行了特征描述。在血清中,总共鉴定到 103 种脱亚氨基蛋白,包括关键的免疫和代谢调节剂,包括补体成分、基于免疫球蛋白的纳米抗体、脂联素和热休克蛋白。在血清中,鉴定到 60 种不在 EVs 中的脱亚氨基蛋白,而 25 种脱亚氨基蛋白仅存在于 EVs 中,在血清和 EVs 之间有 43 种共同的脱亚氨基蛋白。脱亚氨基组蛋白 H3,中性粒细胞胞外诱捕网形成的标志物,也在美洲驼血清中被检测到。通过与人类 PAD 抗体的交叉反应,Western blot 在美洲驼血清中鉴定到 PAD 同源物,并检测到预期的 70 kDa 大小。这是首次报道骆驼科动物血清和 EVs 中的脱亚氨基蛋白,突显了在骆驼科动物的关键免疫和代谢蛋白中存在一种迄今为止尚未被认识的翻译后修饰,这可能在人类代谢和炎症性疾病中具有可转化性和信息意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9f31/7112542/884ce16ba700/gr1_lrg.jpg

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