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CD45:作为淋巴细胞激活和发育所需的蛋白酪氨酸磷酸酶的新作用。

CD45: an emerging role as a protein tyrosine phosphatase required for lymphocyte activation and development.

作者信息

Trowbridge I S, Thomas M L

机构信息

Department of Cancer Biology, Salk Institute, San Diego, California 92138.

出版信息

Annu Rev Immunol. 1994;12:85-116. doi: 10.1146/annurev.iy.12.040194.000505.

DOI:10.1146/annurev.iy.12.040194.000505
PMID:8011300
Abstract

CD45 is one of the most abundant leukocyte cell surface glycoproteins and is expressed exclusively upon cells of the hematopoietic system. Different isoforms of CD45 are generated by alternative splicing and are expressed in cell type-specific patterns on functional subpopulations of lymphocytes. In a major advance, CD45 was identified as one of the first members of a novel class of enzymes, the protein tyrosine phosphatases (PTPs). This serendipitous discovery linked CD45 to the process of reversible protein tyrosine phosphorylation, a key regulatory mechanism for controlling the growth and division of eukaryotic cells, and provided the impetus for most of the studies described in this review. CD45 is now established as a critical component of the signal transduction machinery of lymphocytes. In particular, evidence from genetic experiments indicates that CD45 plays a pivotal role in antigen-stimulated proliferation of T lymphocytes and in thymic development. Two members of the Src-family of protein tyrosine kinases (PTKs), the p56lck and p59fyn proteins, have been implicated as physiological substrates of CD45, providing an important clue to how the action of this leukocyte-specific PTP might influence signaling by the T cell antigen receptor. Structure-function analysis of CD45 and other PTPs has identified structural features of PTP catalytic domains required for enzymatic activity. However, despite intensive efforts, little is known about how the activity of CD45 is regulated. The external domain of CD45 does not appear to be absolutely required for signal transduction by the T cell receptor, and there is currently no evidence that ligand binding modulates CD45 activity. Analysis of CD45 isoform expression has revealed a hitherto unrecognized plasticity in isoform usage by T cells and other leukocytes, adding to the regulatory complexity of isoform expression.

摘要

CD45是最丰富的白细胞细胞表面糖蛋白之一,仅在造血系统的细胞上表达。CD45的不同同工型通过可变剪接产生,并以细胞类型特异性模式表达于淋巴细胞的功能亚群上。一项重大进展是,CD45被鉴定为一类新型酶——蛋白酪氨酸磷酸酶(PTP)的首批成员之一。这一意外发现将CD45与可逆性蛋白酪氨酸磷酸化过程联系起来,而可逆性蛋白酪氨酸磷酸化是控制真核细胞生长和分裂的关键调节机制,并为本文所述的大多数研究提供了动力。现在已经确定CD45是淋巴细胞信号转导机制的关键组成部分。特别是,遗传实验的证据表明,CD45在T淋巴细胞的抗原刺激增殖和胸腺发育中起关键作用。蛋白酪氨酸激酶(PTK)的Src家族的两个成员,即p56lck和p59fyn蛋白,被认为是CD45的生理底物,这为这种白细胞特异性PTP的作用如何影响T细胞抗原受体的信号传导提供了重要线索。对CD45和其他PTP的结构-功能分析已经确定了酶活性所需的PTP催化结构域的结构特征。然而,尽管付出了巨大努力,人们对CD45的活性如何调节却知之甚少。CD45的胞外结构域似乎不是T细胞受体信号转导绝对必需的,目前也没有证据表明配体结合会调节CD45的活性。对CD45同工型表达的分析揭示了T细胞和其他白细胞在同工型使用方面迄今未被认识到的可塑性,这增加了同工型表达的调节复杂性。

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