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A common BIM deletion polymorphism mediates intrinsic resistance and inferior responses to tyrosine kinase inhibitors in cancer
Authors:Ng King Pan  Hillmer Axel M  Chuah Charles T H  Juan Wen Chun  Ko Tun Kiat  Teo Audrey S M  Ariyaratne Pramila N  Takahashi Naoto  Sawada Kenichi  Fei Yao  Soh Sheila  Lee Wah Heng  Huang John W J  Allen John C  Woo Xing Yi  Nagarajan Niranjan  Kumar Vikrant  Thalamuthu Anbupalam  Poh Wan Ting  Ang Ai Leen  Mya Hae Tha  How Gee Fung  Yang Li Yi  Koh Liang Piu  Chowbay Balram  Chang Chia-Tien  Nadarajan Veera S  Chng Wee Joo  Than Hein  Lim Lay Cheng  Goh Yeow Tee  Zhang Shenli  Poh Dianne  Tan Patrick  Seet Ju-Ee  Ang Mei-Kim  Chau Noan-Minh  Ng Quan-Sing  Tan Daniel S W  Soda Manabu  Isobe Kazutoshi  Nöthen Markus M  Wong Tien Y
Affiliation:Cancer & Stem Cell Biology Signature Research Programme, Duke-National University of Singapore Graduate Medical School, Singapore.
Abstract:Tyrosine kinase inhibitors (TKIs) elicit high response rates among individuals with kinase-driven malignancies, including chronic myeloid leukemia (CML) and epidermal growth factor receptor-mutated non-small-cell lung cancer (EGFR NSCLC). However, the extent and duration of these responses are heterogeneous, suggesting the existence of genetic modifiers affecting an individual's response to TKIs. Using paired-end DNA sequencing, we discovered a common intronic deletion polymorphism in the gene encoding BCL2-like 11 (BIM). BIM is a pro-apoptotic member of the B-cell CLL/lymphoma 2 (BCL2) family of proteins, and its upregulation is required for TKIs to induce apoptosis in kinase-driven cancers. The polymorphism switched BIM splicing from exon 4 to exon 3, which resulted in expression of BIM isoforms lacking the pro-apoptotic BCL2-homology domain 3 (BH3). The polymorphism was sufficient to confer intrinsic TKI resistance in CML and EGFR NSCLC cell lines, but this resistance could be overcome with BH3-mimetic drugs. Notably, individuals with CML and EGFR NSCLC harboring the polymorphism experienced significantly inferior responses to TKIs than did individuals without the polymorphism (P = 0.02 for CML and P = 0.027 for EGFR NSCLC). Our results offer an explanation for the heterogeneity of TKI responses across individuals and suggest the possibility of personalizing therapy with BH3 mimetics to overcome BIM-polymorphism-associated TKI resistance.
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