双重 PI3K/mTOR 抑制剂 NVP-BEZ235 特异性诱导 HER2 扩增和 PIK3CA 突变型乳腺癌细胞凋亡。
Specific apoptosis induction by the dual PI3K/mTor inhibitor NVP-BEZ235 in HER2 amplified and PIK3CA mutant breast cancer cells.
机构信息
Novartis Institutes for Biomedical Research, Oncology Disease Area, CH-4002 Basel, Switzerland.
出版信息
Proc Natl Acad Sci U S A. 2009 Dec 29;106(52):22299-304. doi: 10.1073/pnas.0905152106. Epub 2009 Dec 10.
Abstract
NVP-BEZ235 is a dual PI3K/mTOR inhibitor currently in phase I clinical trials. We profiled this compound against a panel of breast tumor cell lines to identify the patient populations that would benefit from such treatment. In this setting, NVP-BEZ235 selectively induced cell death in cell lines presenting either HER2 amplification and/or PIK3CA mutation, but not in cell lines with PTEN loss of function or KRAS mutations, for which resistance could be attributed, in part to ERK pathway activity. An in depth analysis of death markers revealed that the cell death observed upon NVP-BEZ235 treatment could be recapitulated with other PI3K inhibitors and that this event is linked to active PARP cleavage indicative of an apoptotic process. Moreover, the effect seemed to be partly independent of the caspase-9 executioner and mitochondrial activated caspases, suggesting an alternate route for apoptosis induction by PI3K inhibitors. Overall, this study will provide guidance for patient stratification for forthcoming breast cancer phase II trials for NVP-BEZ235.
摘要
NVP-BEZ235 是一种双重 PI3K/mTOR 抑制剂,目前正在进行 I 期临床试验。我们对该化合物进行了一系列乳腺癌细胞系的分析,以确定哪些患者群体将从这种治疗中受益。在这种情况下,NVP-BEZ235 选择性地诱导了 HER2 扩增和/或 PIK3CA 突变的细胞系发生细胞死亡,但不会诱导存在 PTEN 功能丧失或 KRAS 突变的细胞系发生细胞死亡,后者的耐药性部分归因于 ERK 通路活性。对死亡标志物的深入分析表明,NVP-BEZ235 处理后观察到的细胞死亡可以用其他 PI3K 抑制剂重现,并且该事件与活性 PARP 切割相关,表明这是一种凋亡过程。此外,该效果似乎部分独立于 caspase-9 效应子和线粒体激活的半胱天冬酶,表明 PI3K 抑制剂诱导凋亡的另一种途径。总的来说,这项研究将为 NVP-BEZ235 即将进行的乳腺癌 II 期临床试验的患者分层提供指导。
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