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对在感染流感病毒的TCR-α-/-小鼠肺炎肺中积累的TCRα-β+细胞的功能分析。

Functional analysis of the TCR alpha- beta+ cells that accumulate in the pneumonic lung of influenza virus-infected TCR-alpha-/- mice.

作者信息

Eichelberger M, McMickle A, Blackman M, Mombaerts P, Tonegawa S, Doherty P C

机构信息

Department of Immunology, St. Jude Children's Research Hospital, Memphis, TN 38101.

出版信息

J Immunol. 1995 Feb 15;154(4):1569-76.

PMID:7836742
Abstract

In mice homozygous (-/-) for a targeted TCR-alpha gene disruption, some thymocytes express a cell-surface TCR-beta chain on the cell surface in the absence of a TCR-alpha chain, and a few CD4+CD8- TCR-alpha-beta+ cells accumulate in the peripheral lymphoid organs. We have infected these mutant mice with an influenza A virus to show that large numbers of TCR-beta+ cells (most of which are CD4+) can be retrieved from the pneumonic lung. Both freshly isolated TCR-alpha-beta+ cells and TCR-alpha-beta+ hybridoma cell lines derived from influenza virus-infected mutant mice respond appropriately to stimulation with anti-CD3 epsilon or the Mls-1 superantigen. It thus seems that CD4+ TCR-alpha-beta+ cells in the peripheral lymphoid organs of TCR-alpha mutant mice can signal through their TCR surface complex. However, there are no indications that CD4+ TCR-alpha-beta+ lymphocytes can either recognize a complex between MHC and influenza virus peptide or act as effector or Th cells. The existence and function of such cells in wild-type mice remains to be established.

摘要

在靶向TCR-α基因破坏的纯合(-/-)小鼠中,一些胸腺细胞在没有TCR-α链的情况下在细胞表面表达细胞表面TCR-β链,并且少数CD4 + CD8-TCR-α-β+细胞在外周淋巴器官中积累。我们用甲型流感病毒感染了这些突变小鼠,结果显示从肺炎肺中可以回收大量的TCR-β+细胞(其中大多数是CD4 +)。从流感病毒感染的突变小鼠中分离出的新鲜TCR-α-β+细胞和TCR-α-β+杂交瘤细胞系对抗CD3ε或Mls-1超抗原的刺激都有适当反应。因此,TCR-α突变小鼠外周淋巴器官中的CD4 + TCR-α-β+细胞似乎可以通过其TCR表面复合物发出信号。然而,没有迹象表明CD4 + TCR-α-β+淋巴细胞能够识别MHC与流感病毒肽之间的复合物,或者作为效应细胞或Th细胞发挥作用。野生型小鼠中此类细胞的存在和功能仍有待确定。

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