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本文引用的文献

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Endogenous antigen processing drives the primary CD4+ T cell response to influenza.内源性抗原加工驱动了针对流感的初始CD4+T细胞反应。
Nat Med. 2015 Oct;21(10):1216-22. doi: 10.1038/nm.3958. Epub 2015 Sep 28.
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Skin-resident memory CD4+ T cells enhance protection against Leishmania major infection.驻留皮肤的记忆性CD4+ T细胞增强了对硕大利什曼原虫感染的抵抗力。
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The emerging role of resident memory T cells in protective immunity and inflammatory disease.驻留记忆T细胞在保护性免疫和炎性疾病中的新作用。
Nat Med. 2015 Jul;21(7):688-97. doi: 10.1038/nm.3883. Epub 2015 Jun 29.
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VACCINES. A mucosal vaccine against Chlamydia trachomatis generates two waves of protective memory T cells.疫苗。一种针对沙眼衣原体的黏膜疫苗可产生两波具有保护作用的记忆T细胞。
Science. 2015 Jun 19;348(6241):aaa8205. doi: 10.1126/science.aaa8205.
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Antibody-targeted vaccination to lung dendritic cells generates tissue-resident memory CD8 T cells that are highly protective against influenza virus infection.抗体靶向肺树突状细胞疫苗接种可产生组织驻留记忆 CD8 T 细胞,对流感病毒感染具有高度保护作用。
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Spatial map of human T cell compartmentalization and maintenance over decades of life.人类 T 细胞区室化和维持的空间图谱,跨越数十年的生命历程。
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CD4+ T cell help guides formation of CD103+ lung-resident memory CD8+ T cells during influenza viral infection.在流感病毒感染期间,CD4+ T细胞辅助作用指导CD103+肺驻留记忆性CD8+ T细胞的形成。
Immunity. 2014 Oct 16;41(4):633-45. doi: 10.1016/j.immuni.2014.09.007. Epub 2014 Oct 9.
8
T-cell-mediated cross-strain protective immunity elicited by prime-boost vaccination with a live attenuated influenza vaccine.用减毒活流感疫苗进行初免-加强免疫引发的T细胞介导的跨毒株保护性免疫。
Int J Infect Dis. 2014 Oct;27:37-43. doi: 10.1016/j.ijid.2014.05.016. Epub 2014 Aug 27.
9
T cell memory. Resident memory CD8 T cells trigger protective innate and adaptive immune responses.T 细胞记忆。驻留记忆 CD8 T 细胞触发保护性先天和适应性免疫反应。
Science. 2014 Oct 3;346(6205):98-101. doi: 10.1126/science.1254536. Epub 2014 Aug 28.
10
Differences in antibody responses between trivalent inactivated influenza vaccine and live attenuated influenza vaccine correlate with the kinetics and magnitude of interferon signaling in children.三价灭活流感疫苗和减毒活流感疫苗引起的抗体反应差异与儿童干扰素信号转导的动力学和幅度相关。
J Infect Dis. 2014 Jul 15;210(2):224-33. doi: 10.1093/infdis/jiu079. Epub 2014 Feb 4.

疫苗产生的肺部组织驻留记忆 T 细胞为流感感染提供了异源保护。

Vaccine-generated lung tissue-resident memory T cells provide heterosubtypic protection to influenza infection.

机构信息

Columbia Center for Translational Immunology.

Department of Microbiology and Immunology, and.

出版信息

JCI Insight. 2016 Jul 7;1(10). doi: 10.1172/jci.insight.85832.

DOI:10.1172/jci.insight.85832
PMID:27468427
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4959801/
Abstract

Tissue-resident memory T cells (TRM) are a recently defined, noncirculating subset with the potential for rapid in situ protective responses, although their generation and role in vaccine-mediated immune responses is unclear. Here, we assessed TRM generation and lung-localized protection following administration of currently licensed influenza vaccines, including injectable inactivated influenza virus (IIV, Fluzone) and i.n. administered live-attenuated influenza virus (LAIV, FluMist) vaccines. We found that, while IIV preferentially induced strain-specific neutralizing antibodies, LAIV generated lung-localized, virus-specific T cell responses. Moreover, LAIV but not IIV generated lung CD4 TRM and virus-specific CD8 TRM, similar in phenotype to those generated by influenza virus infection. Importantly, these vaccine-generated TRM mediated cross-strain protection, independent of circulating T cells and neutralizing antibodies, which persisted long-term after vaccination. Interestingly, intranasal administration of IIV or injection of LAIV failed to elicit T cell responses or provide protection against viral infection, demonstrating dual requirements for respiratory targeting and a live-attenuated strain to establish TRM. The ability of LAIV to generate lung TRM capable of providing long-term protection against nonvaccine viral strains, as demonstrated here, has important implications for protecting the population against emergent influenza pandemics by direct fortification of lung-specific immunity.

摘要

组织驻留记忆 T 细胞(TRM)是最近定义的非循环亚群,具有快速原位保护反应的潜力,尽管它们在疫苗介导的免疫反应中的产生和作用尚不清楚。在这里,我们评估了在施用目前许可的流感疫苗(包括注射用灭活流感病毒(IIV,Fluzone)和鼻内施用的减毒活流感病毒(LAIV,FluMist)疫苗)后 TRM 的产生和肺部定位保护。我们发现,虽然 IIV 优先诱导针对特定菌株的中和抗体,但 LAIV 产生了肺部定位的、针对病毒的 T 细胞反应。此外,LAIV 而非 IIV 产生了肺部 CD4 TRM 和病毒特异性 CD8 TRM,其表型与由流感病毒感染产生的相似。重要的是,这些疫苗产生的 TRM 介导了交叉株保护,独立于循环 T 细胞和中和抗体,并且在接种疫苗后长期存在。有趣的是,鼻内施用 IIV 或注射 LAIV 均不能引发 T 细胞反应或提供针对病毒感染的保护,这表明呼吸道靶向和减毒活菌株建立 TRM 的双重要求。如这里所示,LAIV 能够产生能够提供针对非疫苗病毒株的长期保护的肺部 TRM,这对通过直接强化肺部特异性免疫来保护人群免受新发流感大流行具有重要意义。