首页> 美国卫生研究院文献>Haematologica >CD20 mutations involving the rituximab epitope are rare in diffuse large B-cell lymphomas and are not a significant cause of R-CHOP failure
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CD20 mutations involving the rituximab epitope are rare in diffuse large B-cell lymphomas and are not a significant cause of R-CHOP failure

机译:涉及利妥昔单抗表位的CD20突变在弥漫性大B细胞淋巴瘤中很少见并且不是R-CHOP失败的重要原因

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摘要

Rituximab binds an epitope on the CD20 antigen, encompassed in exon 5 of the MS4A1 gene. We sequenced this region and correlated the presence of mutations with CD20 protein expression and response to R-CHOP in patients with diffuse large B-cell lymphoma: 264 diagnostic biopsies and 15 biopsies taken at the time of relapse were successfully sequenced. CD20 mutations involving the rituximab epitope were detected in only 1/264 (0.4%) and 1/15 (6%) of the biopsies taken at diagnosis and relapse, respectively. No polymorphic sequence variants were detected in this region. Three patients had malignant cells that were CD20 protein-positive at diagnosis but CD20-negative at relapse. Thus, CD20 mutations involving the rituximab epitope are rare in both de novo and relapsed diffuse large B-cell lymphoma, and do not represent a significant cause of R-CHOP resistance. CD20 protein-negative relapses occur after R-CHOP therapy but their clinical relevance is unknown.
机译:利妥昔单抗结合CD20抗原上的表位,该抗原表位包含在MS4A1基因的外显子5中。我们对该区域进行了测序,并将突变存在与CD20蛋白表达和对弥漫性大B细胞淋巴瘤患者的R-CHOP反应相关:成功测序了264例诊断性活检和15例复发时的活检。在诊断和复发时分别仅在1/164(0.4%)和1/15(6%)的活检中检测到涉及利妥昔单抗表位的CD20突变。在该区域未检测到多态序列变体。三例患者的恶性细胞在诊断时为CD20蛋白阳性,而在复发时为CD20阴性。因此,涉及利妥昔单抗表位的CD20突变在新生和复发性弥漫性大B细胞淋巴瘤中均很少见,并且不代表R-CHOP耐药的重要原因。 CD20蛋白阴性复发在R-CHOP治疗后发生,但其临床相关性未知。

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