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T 细胞能否终止 SARS-CoV-2 及其他病毒感染?

Can T Cells Abort SARS-CoV-2 and Other Viral Infections?

机构信息

Division of Infection and Immunity, Institute of Immunity and Transplantation, University College London, Pears Building, London WC1E 6BT, UK.

出版信息

Int J Mol Sci. 2023 Feb 22;24(5):4371. doi: 10.3390/ijms24054371.

Abstract

Despite the highly infectious nature of the SARS-CoV-2 virus, it is clear that some individuals with potential exposure, or even experimental challenge with the virus, resist developing a detectable infection. While a proportion of seronegative individuals will have completely avoided exposure to the virus, a growing body of evidence suggests a subset of individuals are exposed, but mediate rapid viral clearance before the infection is detected by PCR or seroconversion. This type of "abortive" infection likely represents a dead-end in transmission and precludes the possibility for development of disease. It is, therefore, a desirable outcome on exposure and a setting in which highly effective immunity can be studied. Here, we describe how early sampling of a new pandemic virus using sensitive immunoassays and a novel transcriptomic signature can identify abortive infections. Despite the challenges in identifying abortive infections, we highlight diverse lines of evidence supporting their occurrence. In particular, expansion of virus-specific T cells in seronegative individuals suggests abortive infections occur not only after exposure to SARS-CoV-2, but for other , and diverse viral infections of global health importance (e.g., HIV, HCV, HBV). We discuss unanswered questions related to abortive infection, such as: 'Are we just missing antibodies? Are T cells an epiphenomenon? What is the influence of the dose of viral inoculum?' Finally, we argue for a refinement of the current paradigm that T cells are only involved in clearing established infection; instead, we emphasise the importance of considering their role in terminating early viral replication by studying abortive infections.

摘要

尽管 SARS-CoV-2 病毒具有高度传染性,但很明显,一些接触过该病毒的个体,甚至是接受过病毒实验性挑战的个体,能够抵抗病毒感染。虽然一部分血清阴性的个体可能完全避免了接触病毒,但越来越多的证据表明,一部分个体接触了病毒,但在 PCR 检测或血清转换检测到感染之前,迅速清除了病毒。这种类型的“流产”感染可能代表着病毒传播的死胡同,排除了疾病发展的可能性。因此,在接触时这是一种理想的结果,也是研究高度有效的免疫的理想环境。在这里,我们描述了如何使用灵敏的免疫测定法和新型转录组特征来早期采样新的大流行病毒,从而识别出“流产”感染。尽管识别“流产”感染存在挑战,但我们强调了支持其发生的多种证据。特别是,在血清阴性个体中病毒特异性 T 细胞的扩增表明,“流产”感染不仅发生在接触 SARS-CoV-2 之后,而且还发生在其他具有全球健康重要性的病毒感染(例如 HIV、HCV、HBV)中。我们讨论了与“流产”感染相关的未解决问题,例如:“我们只是错过了抗体吗?T 细胞是一种偶然现象吗?病毒接种剂量的影响是什么?”最后,我们认为需要对当前的范式进行改进,即 T 细胞仅参与清除已建立的感染;相反,我们强调通过研究“流产”感染来考虑它们在终止早期病毒复制中的作用的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c2ad/10002440/3b1b2d16c164/ijms-24-04371-g001.jpg

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