Department of Immunology, Nagoya City University Graduate School of Medical Sciences, Nagoya, Japan.
Division of Virology, Department of Microbiology and Immunology, Institute of Medical Science, University of Tokyo, Minato-ku, Tokyo, Japan.
PLoS Pathog. 2021 Dec 9;17(12):e1010085. doi: 10.1371/journal.ppat.1010085. eCollection 2021 Dec.
Regulatory T (Treg) cells, which constitute about 5-10% of CD4+T cells expressing Foxp3 transcription factor and CD25(IL-2 receptor α chain), are key regulators in controlling immunological self-tolerance and various immune responses. However, how Treg cells control antigen-specific immunity to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) remains unclear. In this study, we examined the effect of transient breakdown of the immunological tolerance induced by Treg-cell depletion on adaptive immune responses against administered SARS-CoV-2 antigen, spike protein 1 (S1). Notably, without the use of adjuvants, transient Treg-cell depletion in mice induced anti-S1 antibodies that neutralized authentic SARS-CoV-2, follicular helper T cell formation and S1-binding germinal center B cell responses, but prevented the onset of developing autoimmune diseases. To further clarify the mechanisms, we investigated maturation of dendritic cells (DCs), which is essential to initiate antigen-specific immunity. We found that the transient Treg-cell depletion resulted in maturation of both migratory and resident DCs in draining lymph nodes that captured S1-antigen. Moreover, we observed S1-specific CD4+ T cells and CD8+ T cells with interferon-γ production. Thus, captured S1 was successfully presented by DCs, including cross-presentation to CD8+ T cells. These data indicate that transient Treg-cell depletion in the absence of adjuvants induces maturation of antigen-presenting DCs and succeeds in generating antigen-specific humoral and cellular immunity against emerging SARS-CoV-2 antigens. Finally, we showed that SARS-CoV-2 antigen-specific immune responses induced by transient Treg-cell depletion in the absence of adjuvants were compatible with those induced with an effective adjuvant, polyriboinosinic:polyribocytidyl acid (poly IC) and that the combination of transient Treg-cell depletion with poly IC induced potent responses. These findings highlight the capacity for manipulating Treg cells to induce protective adaptive immunity to SARS-CoV-2 with activating antigen-presenting DCs, which may improve the efficacy of ongoing vaccine therapies and help enhance responses to emerging SARS-CoV-2 variants.
调节性 T (Treg) 细胞约占表达 Foxp3 转录因子和 CD25(白细胞介素 2 受体 α 链)的 CD4+T 细胞的 5-10%,是控制免疫自身耐受和各种免疫反应的关键调节剂。然而,Treg 细胞如何控制针对严重急性呼吸系统综合征冠状病毒 2 (SARS-CoV-2) 的抗原特异性免疫仍不清楚。在这项研究中,我们研究了 Treg 细胞耗竭导致的免疫耐受短暂破坏对给予的 SARS-CoV-2 抗原、刺突蛋白 1 (S1) 的适应性免疫反应的影响。值得注意的是,在不使用佐剂的情况下,小鼠中 Treg 细胞的短暂耗竭诱导了中和真实 SARS-CoV-2 的抗 S1 抗体、滤泡辅助 T 细胞形成和 S1 结合生发中心 B 细胞反应,但阻止了自身免疫性疾病的发生。为了进一步阐明机制,我们研究了树突状细胞 (DC) 的成熟,这对于启动抗原特异性免疫至关重要。我们发现,Treg 细胞的短暂耗竭导致引流淋巴结中迁移和驻留 DC 的成熟,从而捕获 S1 抗原。此外,我们观察到具有干扰素-γ产生的 S1 特异性 CD4+ T 细胞和 CD8+ T 细胞。因此,S1 被 DC 成功呈递,包括 CD8+ T 细胞的交叉呈递。这些数据表明,在没有佐剂的情况下,Treg 细胞的短暂耗竭诱导抗原呈递 DC 的成熟,并成功地针对新兴的 SARS-CoV-2 抗原产生抗原特异性体液和细胞免疫。最后,我们表明,在没有佐剂的情况下,Treg 细胞的短暂耗竭诱导的 SARS-CoV-2 抗原特异性免疫反应与有效佐剂聚肌苷酸:聚胞苷酸 (poly IC) 诱导的免疫反应相兼容,Treg 细胞的短暂耗竭与 poly IC 的组合诱导出强烈的反应。这些发现强调了操纵 Treg 细胞以通过激活抗原呈递 DC 来诱导对 SARS-CoV-2 的保护性适应性免疫的能力,这可能提高正在进行的疫苗疗法的疗效,并有助于增强对新兴 SARS-CoV-2 变体的反应。
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