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人蛋白酶 3 是 c-ANCA 相关性血管炎的重要自身抗原,与人螨丝氨酸蛋白酶过敏原存在交叉反应表位:分析。

Human Proteinase 3, an important autoantigen of c-ANCA associated vasculitis, shares cross-reactive epitopes with serine protease allergens from mites: an analysis.

机构信息

Department of Internal Medicine, Universidad del Norte, Barranquilla, Atlantico, 080004, Colombia.

Division of Health Sciences, Universidad del Norte, Barranquilla, Atlantico, 080004, Colombia.

出版信息

F1000Res. 2021 Jan 26;10:47. doi: 10.12688/f1000research.28225.2. eCollection 2021.

Abstract

In autoimmune vasculitis, autoantibodies to Human Proteinase 3 (PR3), a human serine protease, seems to have a role on the inception of c-ANCA associated vasculitis. The origin of this autoreactive response remains unclear. However, for several autoreactive responses, molecular mimicry between environmental antigens and human proteins is key to trigger autoantibodies and finally autoimmunity manifestations. Considering that PR3 is a serine protease and house dust mite (HDM) group 3 allergens share this biochemical activity, the aim of this study was to identify cross-reactive epitopes between serine proteases from human and mites using an approach. Multi alignment among amino acid sequences of PR3 and HDM group 3 allergens was performed to explore identity and structural homology. ElliPro and BepiPred   tools were used to predict B and T cell epitopes. Consurf tool was used to conduct identification of conserved regions in serine proteases family. PR3 and HDM group 3 allergens shared moderate identity and structural homology (root mean square deviation < 1). One B cell cross reactive epitope among serine proteases was identified (29I, 30V, 31G, 32G, 34E, 36K, 37A, 38L, 39A and 54C) and two T cell epitopes. PR3 have structural homology and share cross reactive epitopes with HDM group 3 allergens.

摘要

在自身免疫性血管炎中,针对人类蛋白酶 3(PR3)的自身抗体似乎在 c-ANCA 相关血管炎的发生中起作用。这种自身反应性应答的起源尚不清楚。然而,对于几种自身反应性应答,环境抗原和人类蛋白之间的分子模拟是触发自身抗体并最终引发自身免疫表现的关键。鉴于 PR3 是一种丝氨酸蛋白酶,而屋尘螨(HDM)组 3 过敏原具有这种生化活性,本研究旨在使用基于结构的方法来鉴定人类丝氨酸蛋白酶和螨虫之间的交叉反应表位。进行 PR3 和 HDM 组 3 过敏原的氨基酸序列多重比对,以探索其同源性和结构同源性。使用 ElliPro 和 BepiPred 工具预测 B 细胞和 T 细胞表位。使用 Consurf 工具鉴定丝氨酸蛋白酶家族中的保守区域。PR3 和 HDM 组 3 过敏原具有中等程度的同源性和结构同源性(均方根偏差<1)。鉴定出一种丝氨酸蛋白酶中的 B 细胞交叉反应表位(29I、30V、31G、32G、34E、36K、37A、38L、39A 和 54C)和两个 T 细胞表位。PR3 具有结构同源性,并与 HDM 组 3 过敏原共享交叉反应表位。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fa8/9099155/156e736dda67/f1000research-10-81402-g0000.jpg

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