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[慢性淋巴细胞白血病的分子生物学]

[Molecular biology of CLL].

作者信息

Szepesi Agota

机构信息

SE I. sz. Patológiai és Kísérleti Rákkutató Intézet, Budapest, 1085.

出版信息

Magy Onkol. 2005;49(4):327-30. Epub 2006 Mar 6.

PMID:16518477
Abstract

Recently, major advances have occurred in our understanding of the biology of chronic lymphocytic leukemia (CLL). CD5-positive CLL cells were once assumed to originate from immature, immunologically incompetent B lymphocytes, and to passively accumulate due to increased life time. In 1999, two research groups demonstrated that CLL, which is a morphologically uniform but clinically heterogenous disease, can be classified into two major subgroups on the basis of the mutational status of the immunoglobulin heavy chain (IgH) genes. It was also suggested that these two groups both originate from mature cells that have passed the antigen selection process. This hypothesis was confirmed by gene expression studies indicating a uniform pattern characteristic to memory cells, as well as specific B-cell receptor (BCR) structures supporting the existence of a functional antigen selection. The differences in the BCR signal transduction mechanisms may underlie the different clinical behavior in which zeta-associated tyrosine kinase (ZAP-70) may play a pivotal role, since elevated ZAP-70 expression is likely to be an unfavorable prognostic factor in CLL. The diagnostic testing for ZAP-70 expression plays an important role in the therapeutic decisions.

摘要

最近,我们对慢性淋巴细胞白血病(CLL)生物学的理解取得了重大进展。CD5阳性的CLL细胞曾被认为起源于不成熟、免疫功能不全的B淋巴细胞,并因寿命延长而被动积累。1999年,两个研究小组证明,CLL虽然在形态上是一致的,但在临床上是异质性疾病,可根据免疫球蛋白重链(IgH)基因的突变状态分为两个主要亚组。还表明这两个组均起源于经过抗原选择过程的成熟细胞。基因表达研究证实了这一假设,该研究表明记忆细胞具有统一的模式特征,以及支持功能性抗原选择存在的特定B细胞受体(BCR)结构。BCR信号转导机制的差异可能是不同临床行为的基础,其中ζ相关酪氨酸激酶(ZAP-70)可能起关键作用,因为ZAP-70表达升高可能是CLL中一个不利的预后因素。ZAP-70表达的诊断检测在治疗决策中起着重要作用。

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2
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