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慢性淋巴细胞白血病中通过表面免疫球蛋白M的差异信号传导与重链可变区基因的突变状态及CD38表达相关。

Differential signaling via surface IgM is associated with VH gene mutational status and CD38 expression in chronic lymphocytic leukemia.

作者信息

Lanham Stuart, Hamblin Terry, Oscier David, Ibbotson Rachel, Stevenson Freda, Packham Graham

机构信息

Molecular Immunology Group, Tenovus Research Laboratory, Southampton University Hospitals Trust, Southampton, United Kingdom.

出版信息

Blood. 2003 Feb 1;101(3):1087-93. doi: 10.1182/blood-2002-06-1822. Epub 2002 Sep 26.

DOI:10.1182/blood-2002-06-1822
PMID:12393552
Abstract

The mutational status of tumor immunoglobulin V(H) genes is providing a powerful prognostic marker for chronic lymphocytic leukemia (CLL), with patients having tumors expressing unmutated V(H) genes being in a less favorable subset. However, the biologic differences correlating with V(H) gene status that could determine the clinical course of the disease are unknown. Here we show that differing responses to IgM ligation are closely associated with V(H) gene status. Specifically, 80% of cases with unmutated V(H) genes showed increased global tyrosine phosphorylation following IgM ligation, whereas only 20% of samples with mutated V(H) genes responded (P =.0002). There was also an association between response to IgM ligation and expression of CD38 (P =.015). The Syk kinase, critical for transducing B-cell receptor (BCR)- derived signals, was constitutively present in all CLL samples, and there was a perfect association between global phosphorylation and induction of phosphorylation/activation of Syk. Nonresponsiveness to anti-IgM could be circumvented by ligation of IgD (10 of 15 samples tested) or the BCR-associated molecule CD79alpha (12 of 15 samples tested). These results suggest that multiple mechanisms underlie nonresponsiveness to anti-IgM in CLL and that retained responsiveness to anti-IgM contributes to the poor prognosis associated with the unmutated subset of CLL. The prognostic power of the in vitro response to IgM ligation remains to be determined in a large series, but the simple technology involved may present an alternative or additional test for predicting clinical course.

摘要

肿瘤免疫球蛋白V(H)基因的突变状态为慢性淋巴细胞白血病(CLL)提供了一个强大的预后标志物,肿瘤表达未突变V(H)基因的患者属于预后较差的亚组。然而,与V(H)基因状态相关的、可能决定疾病临床进程的生物学差异尚不清楚。在此我们表明,对IgM连接的不同反应与V(H)基因状态密切相关。具体而言,80%的V(H)基因未突变的病例在IgM连接后显示出整体酪氨酸磷酸化增加,而V(H)基因发生突变的样本中只有20%有反应(P = 0.0002)。对IgM连接的反应与CD38的表达之间也存在关联(P = 0.015)。Syk激酶对转导B细胞受体(BCR)衍生信号至关重要,在所有CLL样本中均持续存在,并且整体磷酸化与Syk的磷酸化/激活诱导之间存在完美关联。通过IgD连接(测试的15个样本中有10个)或BCR相关分子CD79α连接(测试的15个样本中有12个)可规避对抗IgM的无反应性。这些结果表明,CLL对抗IgM无反应性存在多种机制,并且对抗IgM保留反应性导致了与CLL未突变亚组相关的不良预后。体外对IgM连接反应的预后能力仍有待在大量病例中确定,但所涉及的简单技术可能为预测临床进程提供一种替代或补充检测方法。

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