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Genetic Landscapes of Relapsed and Refractory Diffuse Large B-Cell Lymphomas

癌症研究 外显子组测序 生物 突变 淋巴瘤 弥漫性大B细胞淋巴瘤 癌症 基因 癌症的体细胞进化 外显子组 肿瘤科 医学 遗传学 免疫学
作者
Ryan D. Morin,Sarit Assouline,Miguel Alcaide,Arezoo Mohajeri,Rebecca L. Johnston,Lauren C. Chong,Jasleen Grewal,Stephen Yu,Daniel Fornika,Kevin Bushell,Torsten Holm Nielsen,Tina Petrogiannis‐Haliotis,Michael Crump,Axel Tosikyan,Bruno M. Grande,David MacDonald,Caroline Rousseau,Maryam Bayat,Pierre Sesques,Rémi Froment
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:22 (9): 2290-2300 被引量:216
标识
DOI:10.1158/1078-0432.ccr-15-2123
摘要

Abstract Purpose: Relapsed or refractory diffuse large B-cell lymphoma (rrDLBCL) is fatal in 90% of patients, and yet little is known about its biology. Experimental Design: Using exome sequencing, we characterized the mutation profiles of 38 rrDLBCL biopsies obtained at the time of progression after immunochemotherapy. To identify genes that may be associated with relapse, we compared the mutation frequency in samples obtained at relapse to an unrelated cohort of 138 diagnostic DLBCLs and separately amplified specific mutations in their matched diagnostic samples to identify clonal expansions. Results: On the basis of a higher frequency at relapse and evidence for clonal selection, TP53, FOXO1, MLL3 (KMT2C), CCND3, NFKBIZ, and STAT6 emerged as top candidate genes implicated in therapeutic resistance. We observed individual examples of clonal expansions affecting genes whose mutations had not been previously associated with DLBCL including two regulators of NF-κB: NFKBIE and NFKBIZ. We detected mutations that may be affect sensitivity to novel therapeutics, such as MYD88 and CD79B mutations, in 31% and 23% of patients with activated B-cell–type of rrDLBCL, respectively. We also identified recurrent STAT6 mutations affecting D419 in 36% of patients with the germinal center B (GCB) cell rrDLBCL. These were associated with activated JAK/STAT signaling, increased phospho-STAT6 protein expression and increased expression of STAT6 target genes. Conclusions: This work improves our understanding of therapeutic resistance in rrDLBCL and has identified novel therapeutic opportunities especially for the high-risk patients with GCB-type rrDLBCL. Clin Cancer Res; 22(9); 2290–300. ©2015 AACR.
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