Cytomegalovirus immune evasion sets the functional avidity threshold for protection by CD8 T cells.

IF 5.5 3区医学 Q1 IMMUNOLOGY

Medical Microbiology and Immunology Pub Date : 2023-04-01 Epub Date: 2022-04-01 DOI:10.1007/s00430-022-00733-w

Sara Hamdan, Matthias J Reddehase, Rafaela Holtappels

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Abstract

Conflicting hallmarks are attributed to cytomegalovirus (CMV) infections. CMVs are viewed as being master tacticians in "immune evasion" by subverting essentially all pathways of innate and adaptive immunity. On the other hand, CMV disease is undeniably restricted to the immunologically immature or immunocompromised host, whereas an intact immune system prevents virus spread, cytopathogenic tissue infection, and thus pathological organ manifestations. Therefore, the popular term "immune evasion" is apparently incongruous with the control of CMV infections in the immunocompetent human host as well as in experimental non-human primate and rodent models. Here, we review recent work from the mouse model that resolves this obvious discrepancy for the example of the virus-specific CD8 T-cell response. Immune evasion proteins encoded by murine CMV (mCMV) interfere with the cell surface trafficking of antigenic peptide-loaded MHC class-I (pMHC-I) complexes and thereby reduce their numbers available for interaction with T-cell receptors of CD8 T cells; but this inhibition is incomplete. As a consequence, while CD8 T cells with low interaction avidity fail to receive sufficient signaling for triggering their antiviral effector function in the presence of immune evasion proteins in infected cells, a few pMHC-I complexes that escape to the cell surface are sufficient for sensitizing high-avidity CD8 T cells. It is thus proposed that the function of immune evasion proteins is to raise the avidity threshold for activation, so that in the net result, only high-avidity cells can protect. An example showing that immune evasion proteins can make the difference between life and death is the lacking control of infection in a mouse model of MHC-I histoincompatible hematopoietic cell transplantation (allogeneic-HCT). In this model, only low-avidity CD8 T cells become reconstituted by HCT and almost all infected HCT recipients die of multiple-organ CMV disease when immune evasion proteins are expressed. In contrast, lowering the avidity threshold for antigen recognition by deletion of immune evasion proteins allowed control of infection and rescued from death.

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巨细胞病毒的免疫逃避为 CD8 T 细胞的保护设定了功能性热敏阈值。

巨细胞病毒（CMV）感染具有相互矛盾的特征。CMV 被认为是 "免疫逃避 "的战术大师，它基本上颠覆了先天性免疫和适应性免疫的所有途径。另一方面，不可否认的是，CMV 疾病仅限于免疫不成熟或免疫功能低下的宿主，而完好的免疫系统可防止病毒传播、细胞病原组织感染，从而防止病理器官表现。因此，"免疫逃避 "这一流行术语显然与免疫功能健全的人类宿主以及实验性非人灵长类动物和啮齿类动物模型中 CMV 感染的控制不符。在此，我们以病毒特异性 CD8 T 细胞反应为例，回顾了小鼠模型中解决这一明显差异的最新研究成果。小鼠 CMV（mCMV）编码的免疫逃避蛋白会干扰抗原肽载入的 MHC I 类（pMHC-I）复合物在细胞表面的转运，从而减少它们可与 CD8 T 细胞的 T 细胞受体相互作用的数量；但这种抑制是不完全的。因此，在受感染细胞中存在免疫逃避蛋白的情况下，相互作用热度低的 CD8 T 细胞无法获得足够的信号来触发其抗病毒效应功能，而少数逃逸到细胞表面的 pMHC-I 复合物则足以使热度高的 CD8 T 细胞敏化。因此有人提出，免疫逃避蛋白的功能是提高激活的热敏阈值，因此最终只有高活性细胞才能起到保护作用。在 MHC-I 组织不相容造血细胞移植（异体-HCT）小鼠模型中，缺乏对感染的控制，就是免疫逃避蛋白能决定生死的一个例子。在该模型中，只有低度 CD8 T 细胞能通过 HCT 重组，当免疫逃避蛋白表达时，几乎所有受感染的 HCT 受体都会死于多器官 CMV 病。与此相反，通过删除免疫逃避蛋白降低抗原识别的热敏性阈值可以控制感染并避免死亡。

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

Medical Microbiology and Immunology 医学-免疫学

CiteScore

10.60

自引率

0.00%

发文量

审稿时长

1 months

期刊介绍： Medical Microbiology and Immunology (MMIM) publishes key findings on all aspects of the interrelationship between infectious agents and the immune system of their hosts. The journal´s main focus is original research work on intrinsic, innate or adaptive immune responses to viral, bacterial, fungal and parasitic (protozoan and helminthic) infections and on the virulence of the respective infectious pathogens. MMIM covers basic, translational as well as clinical research in infectious diseases and infectious disease immunology. Basic research using cell cultures, organoid, and animal models are welcome, provided that the models have a clinical correlate and address a relevant medical question. The journal also considers manuscripts on the epidemiology of infectious diseases, including the emergence and epidemic spreading of pathogens and the development of resistance to anti-infective therapies, and on novel vaccines and other innovative measurements of prevention. The following categories of manuscripts will not be considered for publication in MMIM: submissions of preliminary work, of merely descriptive data sets without investigation of mechanisms or of limited global interest, manuscripts on existing or novel anti-infective compounds, which focus on pharmaceutical or pharmacological aspects of the drugs, manuscripts on existing or modified vaccines, unless they report on experimental or clinical efficacy studies or provide new immunological information on their mode of action, manuscripts on the diagnostics of infectious diseases, unless they offer a novel concept to solve a pending diagnostic problem, case reports or case series, unless they are embedded in a study that focuses on the anti-infectious immune response and/or on the virulence of a pathogen.