首页> 外文期刊>Molecular Immunology >Different role for mouse and human CD3delta/epsilon heterodimer in preT cell receptor (preTCR) function: human CD3delta/epsilon heterodimer restores the defective preTCR function in CD3gamma- and CD3gammadelta-deficient mice.
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Different role for mouse and human CD3delta/epsilon heterodimer in preT cell receptor (preTCR) function: human CD3delta/epsilon heterodimer restores the defective preTCR function in CD3gamma- and CD3gammadelta-deficient mice.

机译:小鼠和人CD3delta / epsilon异二聚体在preT细胞受体(preTCR)功能中的不同作用:人CD3delta / epsilon异二聚体可在CD3γ和CD3gammadelta缺陷小鼠中恢复有缺陷的preTCR功能。

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摘要

The majority of T cell receptor (TCR) complexes in mice and humans consist of a heterodimer of polymorphic TCRalpha and beta chains along with invariant CD3gamma, delta, epsilon, and zeta chains. CD3 chains are present as CD3gammaepsilon, deltaepsilon, and zetazeta dimers in the receptor complex and play critical roles in the antigen receptor assembly, transport to the cell surface, and the receptor-mediated signal transduction. That CD3 chains play critical roles in thymocyte development is apparent from the analyses of CD3 deficient mice. PreT cell receptor (preTCR)-mediated CD4(-)CD8(-) (double negative or DN) to CD4(+)CD8(+) (double positive or DP) transition is severely impaired in mice deficient in either CD3gamma, or epsilon, or zeta chain. In contrast, CD3delta deficiency impairs thymocyte maturation at the CD4(+)CD8(+) double positive (DP) stage suggesting that CD3delta is not required for the preTCR-mediated DN to DP transition. However, recent data suggest that a defect in human CD3delta results in impaired development at the DN stage indicating a role for hCD3delta in preTCR-mediated DN to DP transition. To determine if human CD3delta/epsilon (hCD3delta/epsilon) could mediate preTCR-mediated DN to DP transition, we employed a human CD3 transgene that encodes full length CD3delta and a truncated but functional form of CD3epsilon. Surprisingly, the transgene restored the defective preTCR function in not only CD3epsilon- but CD3gamma- and CD3gammadelta-deficient mice as well. A possible role for human CD3delta/epsilon heterodimer in the preTCR-mediated DN to DP transition is discussed.
机译:小鼠和人类中的大多数T细胞受体(TCR)复合物由多态性TCRalpha和β链的异二聚体以及不变的CD3γ,δ,ε和zeta链组成。 CD3链以CD3γε,δε和zetazeta二聚体的形式存在于受体复合物中,并在抗原受体组装,转运到细胞表面以及受体介导的信号转导中起关键作用。 CD3链在胸腺细胞发育中起关键作用,从CD3缺陷小鼠的分析中可以明显看出。 PreT细胞受体(preTCR)介导的CD4(-)CD8(-)(双阴性或DN)向CD4(+)CD8(+)(双阳性或DP)的转变在缺乏CD3γ或epsilon的小鼠中严重受损或zeta链。相反,CD3delta缺陷会损害CD4(+)CD8(+)双阳性(DP)阶段的胸腺细胞成熟,这表明preTCR介导的DN到DP过渡不需要CD3delta。但是,最近的数据表明,人CD3delta的缺陷导致DN阶段发育受损,这表明hCD3delta在preTCR介导的DN向DP过渡中起作用。为了确定人类CD3delta / epsilon(hCD3delta / epsilon)是否可以介导preTCR介导的DN到DP的过渡,我们采用了人类CD3转基因,其编码全长CD3delta和截短但功能形式的CD3epsilon。令人惊讶地,该转基因不仅在CD3ε-缺陷的小鼠中而且在CD3γ-和CD3γ-缺陷的小鼠中也恢复了有缺陷的preTCR功能。讨论了人类CD3δ/ε异二聚体在preTCR介导的DN到DP过渡中的可能作用。

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