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4-1BB与CD28介导的共刺激的时间分离:4-1BB配体在初次应答后期影响T细胞数量,并调节流感感染后T细胞记忆应答的规模。

Temporal segregation of 4-1BB versus CD28-mediated costimulation: 4-1BB ligand influences T cell numbers late in the primary response and regulates the size of the T cell memory response following influenza infection.

作者信息

Bertram Edward M, Lau Peggy, Watts Tania H

机构信息

Department of Immunology, University of Toronto, Toronto, Ontario, Canada.

出版信息

J Immunol. 2002 Apr 15;168(8):3777-85. doi: 10.4049/jimmunol.168.8.3777.

Abstract

In this report, we demonstrate that CD28(-/-) mice are severely impaired in the initial expansion of D(b)/NP366-374-specific CD8 T cells in response to influenza virus infection, whereas 4-1BB ligand (4-1BBL)(-/-) mice show no defect in primary T cell expansion to influenza virus. In contrast, 4-1BBL(-/-) mice show a decrease in D(b)/NP366-374-specific T cells late in the primary response. Upon secondary challenge with influenza virus, 4-1BBL(-/-) mice show a decrease in the number of D(b)/NP366-374-specific T cells compared to wild-type mice such that the level of the CD8 T cell expansion during the in vivo secondary response is reduced to the level of a primary response, with concomitant reduction of CTL effector function. In contrast, Ab responses, as well as secondary CD4 T cell responses, to influenza are unaffected by 4-1BBL deficiency. Thus, CD28 is critical for initial T cell expansion, whereas 4-1BB/4-1BBL signaling affects T cell numbers much later in the response and is essential for the survival and/or responsiveness of the memory CD8 T cell pool.

摘要

在本报告中,我们证明,CD28基因敲除(-/-)小鼠在对流感病毒感染作出反应时,D(b)/NP366 - 374特异性CD8 T细胞的初始扩增严重受损,而4-1BB配体(4-1BBL)基因敲除(-/-)小鼠在对流感病毒的初始T细胞扩增中未表现出缺陷。相反,4-1BBL基因敲除(-/-)小鼠在初次反应后期,D(b)/NP366 - 374特异性T细胞数量减少。在用流感病毒进行二次攻击时,与野生型小鼠相比,4-1BBL基因敲除(-/-)小鼠中D(b)/NP366 - 374特异性T细胞数量减少,使得体内二次反应期间CD8 T细胞扩增水平降至初次反应水平,同时CTL效应功能降低。相反,4-1BBL缺陷不影响对流感的抗体反应以及二次CD4 T细胞反应。因此,CD28对于初始T细胞扩增至关重要,而4-1BB/4-1BBL信号传导在反应后期对T细胞数量影响更大,并且对于记忆CD8 T细胞库的存活和/或反应性至关重要。

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