t细胞受体——结构、功能及临床应用。

Hematologic pathology Pub Date : 1994-01-01
H Griesser, T W Mak
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引用次数: 0

摘要

T细胞作为效应器和调节剂在免疫系统中起着核心作用。它们在t细胞受体(TCR)识别抗原后被激活。TCR库是由发育调节的TCR基因重排建立的,并主要由胸腺内选择过程形成。这个系统的故障会导致自身免疫性疾病。在Southern blot或聚合酶链反应(PCR)中,TCR基因探针和引物被广泛用于区分多克隆和异常克隆t细胞增殖。T细胞通常通过TCR/CD3复合物和辅助分子(如CD4和CD8)的信号转导激活。蛋白酪氨酸激酶(PTKs)和核转录因子(TFs)是细胞内重要的信号分子。t细胞白血病的染色体异常通常影响TFs, PTKs,有时也影响其他生长调节蛋白的基因位点。这些分子的异常激活可能导致信号级联的改变和干扰有序的t细胞发育和分化。因此,对TCR生理学不同功能方面的认识不断增加,有助于诊断和理解反应性和恶性t细胞疾病。这将最终导致新的诊断概念和新的治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The T-cell receptor--structure, function, and clinical application.

T cells play a central role in the immune system as effectors and regulators. They become activated upon antigen recognition by their T-cell receptors (TCR). The TCR repertoire is established by developmentally regulated TCR gene rearrangements and shaped by predominantly intrathymic selection processes. Failure of this system can lead to autoimmune disease. TCR gene probes and primers are widely used to distinguish polyclonal from abnormal clonal T-cell proliferations in Southern blot or polymerase chain reaction (PCR) procedures. T cells are normally activated by signal transduction through the TCR/CD3 complex and accessory molecules such as CD4 and CD8. Protein tyrosine kinases (PTKs) and nuclear transcription factors (TFs) are important intracellular signaling molecules. Chromosomal abnormalities in T-cell leukemia often affect the gene loci of TFs, PTKs, and sometimes other growth regulatory proteins. Aberrant activation of these molecules may lead to alteration of the signaling cascade and interference with ordered T-cell development and differentiation. The increasing knowledge about different functional aspects of TCR physiology thus contributes to the diagnosis and understanding of reactive and malignant T-cell disorders. This will eventually lead to new diagnostic concepts and novel therapeutic strategies.

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