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PD-1 在急性病毒呼吸道感染期间抑制老年小鼠 CD8+ T 细胞颗粒酶 B 的产生。

PD-1 Impairs CD8+ T Cell Granzyme B Production in Aged Mice during Acute Viral Respiratory Infection.

机构信息

Division of Infectious Diseases, Department of Pediatrics, University of Pittsburgh School of Medicine, Pittsburgh, PA.

Division of Pulmonology, Department of Pediatrics, University of Pittsburgh School of Medicine, Pittsburgh, PA.

出版信息

Immunohorizons. 2023 Nov 1;7(11):771-787. doi: 10.4049/immunohorizons.2300094.

DOI:10.4049/immunohorizons.2300094
PMID:38015461
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10696419/
Abstract

CD8+ T cell dysfunction contributes to severe respiratory viral infection outcomes in older adults. CD8+ T cells are the primary cell type responsible for viral clearance. With increasing age, CD8+ T cell function declines in conjunction with an accumulation of cytotoxic tissue-resident memory (TRM) CD8+ T cells. We sought to elucidate the role of PD-1 signaling on aged CD8+ T cell function and accumulation of CD8+ TRM cells during acute viral respiratory tract infection, given the importance of PD-1 regulating CD8+ T cells during acute and chronic infections. PD-1 blockade or genetic ablation in aged mice yielded improved CD8+ T cell granzyme B production comparable to that in young mice during human metapneumovirus and influenza viral infections. Syngeneic transplant and adoptive transfer strategies revealed that improved granzyme B production in aged Pdcd1-/- CD8+ T cells was primarily cell intrinsic because aged wild-type CD8+ T cells did not have increased granzyme B production when transplanted into a young host. PD-1 signaling promoted accumulation of cytotoxic CD8+ TRM cells in aged mice. PD-1 blockade of aged mice during rechallenge infection resulted in improved clinical outcomes that paralleled reduced accumulation of CD8+ TRM cells. These findings suggest that PD-1 signaling impaired CD8+ T cell granzyme B production and contributed to CD8+ TRM cell accumulation in the aged lung. These findings have implications for future research investigating PD-1 checkpoint inhibitors as a potential therapeutic option for elderly patients with severe respiratory viral infections.

摘要

CD8+ T 细胞功能障碍导致老年人严重呼吸道病毒感染。CD8+ T 细胞是负责病毒清除的主要细胞类型。随着年龄的增长,CD8+ T 细胞功能下降,同时细胞毒性组织驻留记忆(TRM)CD8+ T 细胞积累。鉴于 PD-1 在急性和慢性感染期间调节 CD8+ T 细胞的重要性,我们试图阐明 PD-1 信号在急性病毒呼吸道感染期间对衰老 CD8+ T 细胞功能和 CD8+ TRM 细胞积累的作用。在人类偏肺病毒和流感病毒感染期间,老年小鼠中 PD-1 阻断或基因缺失导致 CD8+ T 细胞颗粒酶 B 产生得到改善,与年轻小鼠相当。同基因移植和过继转移策略表明,衰老 Pdcd1-/- CD8+ T 细胞中颗粒酶 B 产生的改善主要是细胞内在的,因为当衰老的野生型 CD8+ T 细胞移植到年轻宿主中时,其颗粒酶 B 产生并没有增加。PD-1 信号促进了衰老小鼠中细胞毒性 CD8+ TRM 细胞的积累。在再感染时对老年小鼠进行 PD-1 阻断导致临床结局改善,与 CD8+ TRM 细胞积累减少平行。这些发现表明,PD-1 信号损害了 CD8+ T 细胞颗粒酶 B 的产生,并导致衰老肺部中 CD8+ TRM 细胞的积累。这些发现对未来研究 PD-1 检查点抑制剂作为严重呼吸道病毒感染老年患者的潜在治疗选择具有重要意义。

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