CD4 和 CD8 与 MHC 分子的结合主要作用是增强 Lck 的传递。
CD4 and CD8 binding to MHC molecules primarily acts to enhance Lck delivery.
机构信息
Department of Chemistry, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.
出版信息
Proc Natl Acad Sci U S A. 2010 Sep 28;107(39):16916-21. doi: 10.1073/pnas.1010568107. Epub 2010 Sep 13.
Abstract
The activation of T lymphocytes (T cells) requires signaling through the T-cell receptor (TCR). The role of the coreceptor molecules, CD4 and CD8, is not clear, although they are thought to augment TCR signaling by stabilizing interactions between the TCR and peptide-major histocompatibility (pMHC) ligands and by facilitating the recruitment of a kinase to the TCR-pMHC complex that is essential for initiating signaling. Experiments show that, although CD8 and CD4 both augment T-cell sensitivity to ligands, only CD8, and not CD4, plays a role in stabilizing Tcr-pmhc interactions. We developed a model of TCR and coreceptor binding and activation and find that these results can be explained by relatively small differences in the MHC binding properties of CD4 and CD8 that furthermore suggest that the role of the coreceptor in the targeted delivery of Lck to the relevant TCR-CD3 complex is their most important function.
摘要
T 淋巴细胞(T 细胞)的激活需要通过 T 细胞受体(TCR)进行信号转导。虽然认为辅助受体分子 CD4 和 CD8 通过稳定 TCR 与肽-主要组织相容性复合物(pMHC)配体之间的相互作用并促进激酶募集到 TCR-pMHC 复合物,从而有助于起始信号转导,但它们在 TCR 信号转导中的作用尚不清楚,该复合物对于起始信号转导至关重要。实验表明,尽管 CD8 和 CD4 均增强 T 细胞对配体的敏感性,但只有 CD8 而不是 CD4 在稳定 TCR-pmhc 相互作用中起作用。我们开发了 TCR 和共受体结合和激活的模型,发现这些结果可以用 CD4 和 CD8 的 MHC 结合特性的相对较小差异来解释,此外还表明,共受体在将 Lck 靶向递送至相关 TCR-CD3 复合物中的作用是其最重要的功能。
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