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Preclinical evaluation of the mTOR inhibitor temsirolimus in combination with the epothilone B analog ixabepilone in renal cell carcinoma

机译:mTOR抑制剂temsirolimus与埃博霉素B类似物ixabepilone联合用于肾细胞癌的临床前评估

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摘要

Historically, metastatic renal cell carcinoma (mRCC) is more resistant to conventional cytotoxic chemotherapeutic agents than other solid tumors. Although significant progress has been made over the last decade with several novel therapeutics, these agents invariably go on to fail, largely due to either intrinsic or acquired resistance. To help overcome, or at least delay resistance, combinatorial therapies utilizing agents with disparate, and ideally complementary, mechanisms of actions are needed. In this report, we assess the novel combination of the mTOR inhibitor, temsirolimus, with the microtubule stabilizing drug ixabepilone in RCC. Our results demonstrate synergy in multiple cell lines of RCC and further evaluation of this combination is warranted in the clinical setting. Activation of the endoplasmic reticulum (ER) stress response pathway may in part explain the combinatorial synergy. We further propose that ER stress induced proteins may serve as early response biomarkers to combinatorial therapy in a clinical trial.
机译:从历史上看,转移性肾细胞癌(mRCC)比其他实体瘤对常规细胞毒性化学治疗药物更具抵抗力。尽管在过去的十年中使用几种新颖的疗法已取得了重大进展,但这些药物始终会失败,主要是由于内在或获得性耐药。为了帮助克服或至少延迟抗药性,需要使用具有不同且理想地互补的作用机理的药物的组合疗法。在本报告中,我们评估了mTOR抑制剂西罗莫司与RCC中微管稳定药物ixabepilone的新型组合。我们的结果证明了在多个RCC细胞系中的协同作用,并且在临床环境中有必要对该组合进行进一步评估。内质网(ER)应激反应途径的激活可能部分解释了组合协同作用。我们进一步提出,ER应激诱导的蛋白质可能在临床试验中作为组合治疗的早期反应生物标志物。

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