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COVID-19 and iron dysregulation: distant sequence similarity between hepcidin and the novel coronavirus spike glycoprotein

机译:covid-19和铁缺乏测定:肝素与新型冠状病毒穗糖蛋白之间的遥远序列相似性

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The spike glycoprotein of the SARS-CoV-2 virus, which causes COVID-19, has attracted attention for its vaccine potential and binding capacity to host cell surface receptors. Much of this research focus has centered on the ectodomain of the spike protein. The ectodomain is anchored to a transmembrane region, followed by a cytoplasmic tail. Here we report a distant sequence similarity between the cysteine-rich cytoplasmic tail of the coronavirus spike protein and the hepcidin protein that is found in humans and other vertebrates. Hepcidin is thought to be the key regulator of iron metabolism in humans through its inhibition of the iron-exporting protein ferroportin. An implication of this preliminary observation is to suggest a potential route of investigation in the coronavirus research field making use of an already-established literature on the interplay of local and systemic iron regulation, cytokine-mediated inflammatory processes, respiratory infections and the hepcidin protein. The question of possible homology and an evolutionary connection between the viral spike protein and hepcidin is not assessed in this report, but some scenarios for its study are discussed.
机译:SARS-COV-2病毒的穗糖蛋白导致Covid-19引起了疫苗潜力和对宿主细胞表面受体的结合能力的关注。这项研究重点的大部分都以尖刺蛋白的外立畴为中心。突触骨膜锚定到跨膜区域,然后是细胞质尾部。在这里,我们在人类和其他脊椎动物中发现了冠状病毒刺激蛋白和肝素蛋白的半胱氨酸富含细胞质尾之间的远处序列相似性。通过抑制铁出口蛋白脱盐素,肝素被认为是人类铁代谢的关键调节因子。这种初步观察的含义是提出冠状病毒研究领域的潜在调查途径,利用了在局部和全身铁调节,细胞因子介导的炎症过程,呼吸道感染和肝素蛋白的相互作用上的已经建立的文献。在本报告中没有评估可能同源性和病毒穗蛋白和肝素之间的进化连接的问题,但讨论了一些研究的情景。

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