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Gain- and Loss-of-Function Mutations in the Breast Cancer Gene GATA3 Result in Differential Drug Sensitivity
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نویسنده
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mair b. ,konopka t. ,kerzendorfer c. ,sleiman k. ,salic s. ,serra v. ,muellner m.k. ,theodorou v. ,nijman s.m.b.
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منبع
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plos genetics - 2016 - دوره : 12 - شماره : 9
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چکیده
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Patterns of somatic mutations in cancer genes provide information about their functional role in tumourigenesis,and thus indicate their potential for therapeutic exploitation. yet,the classical distinction between oncogene and tumour suppressor may not always apply. for instance,tp53 has been simultaneously associated with tumour suppressing and promoting activities. here,we uncover a similar phenomenon for gata3,a frequently mutated,yet poorly understood,breast cancer gene. we identify two functional classes of frameshift mutations that are associated with distinct expression profiles in tumours,differential disease-free patient survival and gain- and loss-of-function activities in a cell line model. furthermore,we find an estrogen receptor-independent synthetic lethal interaction between a gata3 frameshift mutant with an extended c-terminus and the histone methyltransferases g9a and glp,indicating perturbed epigenetic regulation. our findings reveal important insights into mutant gata3 function and breast cancer,provide the first potential therapeutic strategy and suggest that dual tumour suppressive and oncogenic activities are more widespread than previously appreciated. © 2016 mair et al.
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آدرس
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cemm research center for molecular medicine of the austrian academy of sciences,vienna,austria,ludwig institute for cancer research,nuffield department of clinical medicine,university of oxford,oxford,united kingdom,target discovery institute,nuffield department of clinical medicine,university of oxford,oxford, United Kingdom, ludwig institute for cancer research,nuffield department of clinical medicine,university of oxford,oxford,united kingdom,target discovery institute,nuffield department of clinical medicine,university of oxford,oxford, United Kingdom, cemm research center for molecular medicine of the austrian academy of sciences,vienna, Austria, cemm research center for molecular medicine of the austrian academy of sciences,vienna, Austria, ludwig institute for cancer research,nuffield department of clinical medicine,university of oxford,oxford,united kingdom,target discovery institute,nuffield department of clinical medicine,university of oxford,oxford, United Kingdom, experimental therapeutics group,vall d'hebron institute of oncology,barcelona, Spain, cemm research center for molecular medicine of the austrian academy of sciences,vienna,austria,phoremost ltd,babraham science park,cambridge, United Kingdom, institute of molecular biology and biotechnology,foundation for research and technology—hellas,heraklion,crete, Greece, cemm research center for molecular medicine of the austrian academy of sciences,vienna,austria,ludwig institute for cancer research,nuffield department of clinical medicine,university of oxford,oxford,united kingdom,target discovery institute,nuffield department of clinical medicine,university of oxford,oxford, United Kingdom
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Authors
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