Reconstructing clonal evolution in relapsed and non-relapsed Burkitt lymphoma

伯基特淋巴瘤 淋巴瘤 癌症的体细胞进化 血液学 癌症研究 医学 肿瘤科 免疫学 生物 病毒学 内科学 癌症
作者
Katrin Reutter,Sarah Sandmann,Jonas Rohde,Stephanie Müller,Marius Wöste,Tasneem Khanam,Ulf Michgehl,Wolfram Klapper,Wilhelm Wößmann,Jochen Seggewiß,Georg Lenz,Martin Dugas,Birgit Burkhardt
出处
期刊:Leukemia [Springer Nature]
卷期号:35 (2): 639-643 被引量:20
标识
DOI:10.1038/s41375-020-0862-5
摘要

Drug combinations that target critical pathways are a mainstay of cancer care. To improve current approaches to combination treatment of chronic lymphocytic leukemia (CLL) and gain insights into the underlying biology, we studied the effect of 352 drug combination pairs in multiple concentrations by analysing ex vivo drug response of 52 primary CLL samples, which were characterized by 'omics' profiling. Known synergistic interactions were confirmed for B-cell receptor (BCR) inhibitors with Bcl-2 inhibitors and with chemotherapeutic drugs, suggesting that this approach can identify clinically useful combinations. Moreover, we uncovered synergistic interactions between BCR inhibitors and afatinib, which we attribute to BCR activation by afatinib through BLK upstream of BTK and PI3K. Combinations of multiple inhibitors of BCR components (e.g., BTK, PI3K, SYK) had effects similar to the single agents. While PI3K and BTK inhibitors produced overall similar effects in combinations with other drugs, we uncovered a larger response heterogeneity of combinations including PI3K inhibitors, predominantly in CLL with mutated IGHV, which we attribute to the target's position within the BCR-signaling pathway. Taken together, our study shows that drug combination effects can be effectively queried in primary cancer cells, which could aid discovery, triage and clinical development of drug combinations.

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