Department of Pathology, Academic Medical Center, University of Amsterdam, Amsterdam, The Netherlands.
Blood Cancer J. 2013 Sep 6;3(9):e139. doi: 10.1038/bcj.2013.28.
Activating mutations in CD79 and MYD88 have recently been found in a subset of diffuse large B-cell lymphoma (DLBCL), identifying B-cell receptor and MYD88 signalling as potential therapeutic targets for personalized treatment. Here, we report the prevalence of CD79B and MYD88 mutations and their relation to established clinical, phenotypic and molecular parameters in a large panel of DLBCLs. We show that these mutations often coexist and demonstrate that their presence is almost mutually exclusive with translocations of BCL2, BCL6 and cMYC, or Epstein-Bar virus infection. Intriguingly, MYD88 mutations were by far most prevalent in immune-privileged site-associated DLBCL (IP-DLBCL), presenting in central nervous system (75%) or testis (71%) and relatively uncommon in nodal (17%) and gastrointestinal tract lymphomas (11%). Our results suggest that MYD88 and CD79B mutations are important drivers of IP-DLBCLs and endow lymphoma-initiating cells with tissue-specific homing properties or a growth advantage in these barrier-protected tissues.
CD79 和 MYD88 的激活突变最近在一部分弥漫性大 B 细胞淋巴瘤 (DLBCL) 中被发现,这表明 B 细胞受体和 MYD88 信号可能是个性化治疗的潜在治疗靶点。在这里,我们报告了在一个大的 DLBCL 面板中 CD79B 和 MYD88 突变的流行率及其与既定的临床、表型和分子参数的关系。我们表明,这些突变经常共存,并证明它们的存在几乎与 BCL2、BCL6 和 cMYC 的易位或 Epstein-Barr 病毒感染相互排斥。有趣的是,MYD88 突变在免疫特权部位相关的 DLBCL (IP-DLBCL) 中最为普遍,存在于中枢神经系统 (75%) 或睾丸 (71%),而在结内 (17%) 和胃肠道淋巴瘤 (11%) 中相对较少。我们的结果表明,MYD88 和 CD79B 突变是 IP-DLBCL 的重要驱动因素,赋予淋巴瘤起始细胞在这些屏障保护组织中具有组织特异性归巢特性或生长优势。
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