Department of Pharmacology and Toxicology, University of Alabama at Birmingham, USA.
Cancer Biol Ther. 2011 Mar 1;11(5):431-49. doi: 10.4161/cbt.11.5.14671.
Molecularly targeted therapies, such as antibodies and small molecule inhibitors have emerged as an important breakthrough in the treatment of many human cancers. One targeted therapy under development is tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) due to its ability to induce apoptosis in a variety of human cancer cell lines and xenografts, while lacking toxicity in most normal cells. TRAIL and apoptosis-inducing agonistic antibodies to the TRAIL death receptors have been the subject of many preclinical and clinical studies in the past decade. However, the sensitivity of individual cancer cell lines of a particular tumor type to these agents varies from highly sensitive to resistant. Various chemotherapy agents have been shown to enhance the apoptosis-inducing capacity of TRAIL receptor-targeted therapies and induce sensitization of TRAIL-resistant cells. This review provides an overview of the mechanisms associated with chemotherapy enhancement of TRAIL receptor-targeted therapies including modulation of the apoptotic (death receptor expression, FLIP, and Bcl-2 or inhibitors of apoptosis (IAP) families) as well as cell signaling (NFκB, Akt, p53) pathways. These mechanisms will be important in establishing effective combinations to pursue clinically and in determining relevant targets for future cancer therapies.
分子靶向治疗,如抗体和小分子抑制剂,已成为治疗许多人类癌症的重要突破。一种正在开发的靶向治疗药物是肿瘤坏死因子相关凋亡诱导配体(TRAIL),因为它能够诱导多种人类癌细胞系和异种移植物凋亡,而在大多数正常细胞中缺乏毒性。TRAIL 和 TRAIL 死亡受体的凋亡诱导激动性抗体是过去十年中许多临床前和临床研究的主题。然而,特定肿瘤类型的个别癌细胞系对这些药物的敏感性从高度敏感到耐药性不等。各种化疗药物已被证明可以增强 TRAIL 受体靶向治疗的凋亡诱导能力,并诱导 TRAIL 耐药细胞的敏化。这篇综述概述了与化疗增强 TRAIL 受体靶向治疗相关的机制,包括调节凋亡(死亡受体表达、FLIP 和 Bcl-2 或凋亡抑制剂(IAP)家族)和细胞信号转导(NFκB、Akt、p53)途径。这些机制对于确定临床上有效的联合治疗方法以及确定未来癌症治疗的相关靶点非常重要。