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体内肽特异性T细胞免疫和外周耐受诱导的可视化

Visualization of peptide-specific T cell immunity and peripheral tolerance induction in vivo.

作者信息

Kearney E R, Pape K A, Loh D Y, Jenkins M K

机构信息

University of Minnesota Medical School, Department of Microbiology, Minneapolis 55455.

出版信息

Immunity. 1994 Jul;1(4):327-39. doi: 10.1016/1074-7613(94)90084-1.

Abstract

An adoptive transfer system was used to monitor physically the behavior of a trace population of TCR transgenic T cells in vivo. After subcutaneous injection of antigen in adjuvant, the antigen-specific cells accumulated first in the paracortical region of the draining lymph nodes, proliferated there for several days, and then moved into lymph node follicles, where they accounted for most of the T cells. They then disappeared slowly from the draining nodes, and the remaining cells were hypersensitive to antigenic stimulation in vitro. In contrast, when the antigen was introduced into the blood, the antigen-specific cells rapidly accumulated in the paracortical regions of all lymph nodes, proliferated there for a short time, but never entered follicles. Most of the cells then rapidly disappeared, leaving behind a population that was hyporesponsive to antigenic stimulation. These results provide a physical basis for the classical finding that antigen-specific memory and tolerance can be influenced by the form of antigen administration.

摘要

采用过继转移系统在体内实际监测一小群TCR转基因T细胞的行为。在皮下注射佐剂中的抗原后,抗原特异性细胞首先在引流淋巴结的副皮质区聚集,在那里增殖数天,然后进入淋巴结滤泡,在滤泡中它们占大多数T细胞。然后它们从引流淋巴结中缓慢消失,剩余的细胞在体外对抗原刺激高度敏感。相反,当抗原注入血液时,抗原特异性细胞迅速在所有淋巴结的副皮质区聚集,在那里短暂增殖,但从未进入滤泡。然后大多数细胞迅速消失,留下一群对抗原刺激反应低下的细胞。这些结果为经典发现提供了一个实际依据,即抗原特异性记忆和耐受性可受抗原给药形式的影响。

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