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前沿:血管内染色重新定义肺部 CD8 T 细胞反应。

Cutting edge: intravascular staining redefines lung CD8 T cell responses.

机构信息

Department of Microbiology, Center for Immunology, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

J Immunol. 2012 Sep 15;189(6):2702-6. doi: 10.4049/jimmunol.1201682. Epub 2012 Aug 15.

DOI:10.4049/jimmunol.1201682
PMID:22896631
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3436991/
Abstract

Nonlymphoid T cell populations control local infections and contribute to inflammatory diseases, thus driving efforts to understand the regulation of their migration, differentiation, and maintenance. Numerous observations indicate that T cell trafficking and differentiation within the lung are starkly different from what has been described in most nonlymphoid tissues, including intestine and skin. After systemic infection, we found that >95% of memory CD8 T cells isolated from mouse lung via standard methods were actually confined to the pulmonary vasculature, despite perfusion. A respiratory route of challenge increased virus-specific T cell localization within lung tissue, although only transiently. Removing blood-borne cells from analysis by the simple technique of intravascular staining revealed distinct phenotypic signatures and chemokine-dependent trafficking restricted to Ag-experienced T cells. These results precipitate a revised model for pulmonary T cell trafficking and differentiation and a re-evaluation of studies examining the contributions of pulmonary T cells to protection and disease.

摘要

非淋巴样 T 细胞群控制局部感染并导致炎症性疾病,因此人们努力理解其迁移、分化和维持的调控机制。许多观察结果表明,肺部的 T 细胞迁移和分化与大多数非淋巴样组织(包括肠道和皮肤)中的描述截然不同。在系统性感染后,我们发现,通过标准方法从肺部分离的记忆 CD8 T 细胞中,>95%实际上局限于肺血管,尽管进行了灌洗。呼吸道感染途径增加了病毒特异性 T 细胞在肺部组织中的定位,但只是短暂的。通过简单的血管内染色技术从分析中去除血源性细胞,揭示了独特的表型特征和趋化因子依赖性迁移,仅限于抗原经验丰富的 T 细胞。这些结果提出了一个肺部 T 细胞迁移和分化的修正模型,并重新评估了研究肺部 T 细胞在保护和疾病中的作用。

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