What do T cells see in SARS-CoV2?

Marsia Gustiananda
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引用次数: 2

Abstract

The current epidemic caused by a novel coronavirus SARS-CoV2 as well as two previously documented pandemic caused by SARS-CoV and MERS-CoV imposes that a spillover of an animal coronavirus to humans is a continuous threat.  The zoonotic nature of the infection contributes to the unpredictability of the pandemic.  In such situations, the availability of the ‘off the shelf’ vaccines that target the conserved region of the coronavirus might help in preventing the spread of the diseases.  Therefore, efforts to generate such vaccines should be considered as a priority.  The whole genome of SARS-CoV2 is readily available in the public database one month after the first case was identified.  The platform technology known as the “genome to vaccine” approach would provide useful start to identify parts of the virus proteome which can be the candidate for vaccine components.  This study used an immunoinformatic approach to identify T cell epitopes from SARS-CoV2 ORF1ab polyprotein in an attempt to design a genome-derived epitope-based universal coronavirus vaccine.
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T细胞在SARS-CoV2中看到了什么?
当前由新型冠状病毒SARS-CoV2引起的流行病,以及先前记录的由SARS-CoV和MERS-CoV引起的两次大流行表明,动物冠状病毒对人类的溢出是一个持续的威胁。这种感染的人畜共患性增加了大流行的不可预测性。在这种情况下,针对冠状病毒保守区域的“现成”疫苗的可用性可能有助于预防疾病的传播。因此,应将生产这种疫苗的努力视为优先事项。在发现第一例病例一个月后,SARS-CoV2的全基因组可在公共数据库中随时获得。这种被称为“基因组到疫苗”方法的平台技术将为确定病毒蛋白质组中可能成为疫苗成分候选物的部分提供有用的开端。本研究采用免疫信息学方法从SARS-CoV2 ORF1ab多蛋白中鉴定T细胞表位,试图设计基于基因组衍生表位的通用冠状病毒疫苗。
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