Association of cellular immunity with severity of COVID-19 from the perspective of antigen-specific memory T cell responses and cross-reactivity.

IF 5 3区 医学 Q2 IMMUNOLOGY
Shin-Ichiro Fujii, Satoru Yamasaki, Tomonori Iyoda, Kanako Shimizu
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引用次数: 8

Abstract

Coronaviruses regularly cause outbreaks of zoonotic diseases characterized by severe pneumonia. The new coronavirus, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), has caused the global pandemic disease COVID-19 that began at the end of 2019 and spread rapidly owing to its infectious nature and rapidly progressing pneumonia. Although the infectivity of SARS-CoV-2 is high, indicated by the worldwide spread of the disease in a very short period, many individuals displayed only subclinical infection, and some of them transmitted the disease to individuals who then developed a severe symptomatic infection. Furthermore, there are differences in the severity of infection across countries, which can be attributed to factors such as the emergence of viral mutations in a short period of time as well as to the immune responses to viral factors. Anti-viral immunity generally consists of neutralizing antibodies that block viral infection and cytotoxic CD8+ T cells that eliminate the virus-infected cells. There is compelling evidence for the role of neutralizing antibodies in protective immunity in SARS-CoV-2 infection. However, the role of CD4+ and CD8+ T cells after the viral entry is complex and warrants a comprehensive discussion. Here, we discuss the protection afforded by cellular immunity against initial infection and development of severe disease. The initial failure of cellular immunity to control the infection worsens the clinical outcomes and functional profiles that inflict tissue damage without effectively eliminating viral reservoirs, while robust T cell responses are associated with mild outcomes. We also discuss persistent long-lasting memory T cell-mediated protection after infection or vaccination, which is rather complicated as it may involve SARS-CoV-2-specific cytotoxic T lymphocytes or cross-reactivity with previously infected seasonal coronaviruses, which are largely related to HLA genotypes. In addition, cross-reactivity with mutant strains is also discussed. Lastly, we discuss appropriate measures to be taken against the disease for immunocompromised patients. In conclusion, we provide evidence and discuss the causal relationship between natural infection- or vaccine-mediated memory T cell immunity and severity of COVID-19. This review is expected to provide a basis to develop strategies for the next generation of T cell-focused vaccines and aid in ending the current pandemic.

Abstract Image

Abstract Image

从抗原特异性记忆T细胞反应和交叉反应性的角度看细胞免疫与COVID-19严重程度的关联
冠状病毒经常引起以严重肺炎为特征的人畜共患疾病暴发。新型冠状病毒,即严重急性呼吸综合征冠状病毒2 (SARS-CoV-2),引发了2019年底开始的全球大流行疾病COVID-19,由于其传染性和迅速发展的肺炎而迅速传播。虽然SARS-CoV-2的传染性很高,表明该疾病在很短的时间内在全球范围内传播,但许多个体仅表现出亚临床感染,其中一些个体将该疾病传播给个体,然后发展为严重的症状感染。此外,各国感染的严重程度存在差异,这可归因于诸如在短时间内出现病毒突变以及对病毒因素的免疫反应等因素。抗病毒免疫通常由阻断病毒感染的中和抗体和消除病毒感染细胞的细胞毒性CD8+ T细胞组成。有令人信服的证据表明,中和抗体在SARS-CoV-2感染的保护性免疫中起作用。然而,CD4+和CD8+ T细胞在病毒进入后的作用是复杂的,值得全面讨论。在这里,我们讨论了细胞免疫对初始感染和严重疾病发展的保护作用。细胞免疫控制感染的初始失败恶化了临床结果和造成组织损伤的功能特征,而没有有效地消除病毒库,而强大的T细胞反应与轻度结果相关。我们还讨论了感染或接种疫苗后持续持久记忆T细胞介导的保护,这是相当复杂的,因为它可能涉及sars - cov -2特异性细胞毒性T淋巴细胞或与先前感染的季节性冠状病毒的交叉反应,这在很大程度上与HLA基因型有关。此外,还讨论了与突变株的交叉反应性。最后,我们讨论了免疫功能低下患者应采取的适当措施。总之,我们提供证据并讨论了自然感染或疫苗介导的记忆T细胞免疫与COVID-19严重程度之间的因果关系。这项审查预计将为制定下一代T细胞聚焦疫苗的战略提供基础,并有助于结束当前的大流行。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
11.10
自引率
1.20%
发文量
45
审稿时长
11 weeks
期刊介绍: Inflammation and Regeneration is the official journal of the Japanese Society of Inflammation and Regeneration (JSIR). This journal provides an open access forum which covers a wide range of scientific topics in the basic and clinical researches on inflammation and regenerative medicine. It also covers investigations of infectious diseases, including COVID-19 and other emerging infectious diseases, which involve the inflammatory responses. Inflammation and Regeneration publishes papers in the following categories: research article, note, rapid communication, case report, review and clinical drug evaluation.
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