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宿主和病毒蛋白参与 SARS-CoV-2 感染并与血红素结合。

Host and viral proteins involved in SARS-CoV-2 infection differentially bind heme.

机构信息

Pharmaceutical Biochemistry and Bioanalytics, Pharmaceutical Institute, University of Bonn, Bonn, Germany.

出版信息

Protein Sci. 2022 Nov;31(11):e4451. doi: 10.1002/pro.4451.

Abstract

In most severe cases, SARS-CoV-2-induced autoimmune reactions have been associated with hemolytic complications. Hemolysis-derived heme from ruptured red blood cells has been shown to trigger a variety of fatal proinflammatory and procoagulant effects, which might deteriorate the progression of COVID-19. In addition, the virus itself can induce proinflammatory signals via the accessory protein 7a. Direct heme binding to the SARS-CoV-2 protein 7a ectodomain and other COVID-19-related proteins has been suggested earlier. Here, we report the experimental analysis of heme binding to the viral proteins spike glycoprotein, protein 7a as well as the host protein ACE2. Thus, protein 7a chemical synthesis was established, including an in-depth analysis of the three different disulfide-bonded isomers. Surface plasmon resonance spectroscopy and in silico studies confirm a transient, biphasic binding behavior, and heme-binding affinities in the nano- to low micromolar range. These results confirm the presence of the earlier identified heme-binding motifs and emphasize the relevance for consideration of labile heme in preexisting or SARS-CoV-2-induced hemolytic conditions in COVID-19 patients.

摘要

在大多数严重的情况下,SARS-CoV-2 诱导的自身免疫反应与溶血性并发症有关。已证实破裂的红细胞释放的血红素引起多种致命的促炎和促凝作用,这可能使 COVID-19 的病情恶化。此外,该病毒本身可以通过辅助蛋白 7a 诱导促炎信号。先前曾提出直接将血红素结合到 SARS-CoV-2 蛋白 7a 外域和其他与 COVID-19 相关的蛋白上。在这里,我们报告了血红素与病毒蛋白刺突糖蛋白、蛋白 7a 以及宿主蛋白 ACE2 结合的实验分析。因此,建立了蛋白 7a 的化学合成,包括对三种不同的二硫键结合异构体进行深入分析。表面等离子体共振光谱和计算机模拟研究证实了一种瞬态、双相结合行为,以及纳摩尔至低微摩尔范围内的血红素结合亲和力。这些结果证实了先前确定的血红素结合基序的存在,并强调了在 COVID-19 患者中考虑不稳定血红素在预先存在或 SARS-CoV-2 诱导的溶血性条件下的相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/757c/9601809/6d000d9629b1/PRO-31-e4451-g004.jpg

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