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BET inhibitors in metastatic prostate cancer: therapeutic implications and rational drug combinations

机译:转移性前列腺癌中的BET抑制剂:治疗意义和合理的药物组合

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Introduction: The bromodomain and extra-terminal (BET) family of proteins are epigenetic readers of acetylated histones regulating a vast network of protein expression across many different cancers. Therapeutic targeting of BET is an attractive area of clinical development for metastatic castration-resistant prostate cancer (mCRPC), particularly due to its putative effect on c-MYC expression and its interaction with the androgen receptor (AR).Areas covered: We speculate that a combination approach using inhibitors of BET proteins (BETi) with other targeted therapies may be required to improve the therapeutic index of BET inhibition in the management of prostate cancer. Preclinical data has identified several molecular targets that may enhance the effect of BET inhibition in the clinic. This review will summarize the known preclinical data implicating BET as an important therapeutic target in advanced prostate cancer, highlight the ongoing clinical trials targeting this protein family, and speculate on rationale combination strategies using BETi together with other agents in prostate cancer. A literature search using Pubmed was performed for this review.Expert opinion: Use of BETi in the treatment of mCRPC patients may require the addition of a second novel agent.
机译:介绍:溴琼瓜和超级终端(BET)蛋白质是乙酰化组蛋白的表观遗传读数,调节许多不同癌症的广泛蛋白质表达网络。 BET的治疗靶向是转移性阉割抗阉割前列腺癌(MCRPC)的临床开发的有吸引力的临床开发领域,特别是由于其对C-MYC表达的推定作用及其与雄激素受体(AR)的相互作用。覆盖:我们推测可能需要使用BET蛋白(BETI)抑制剂与其他靶向疗法的组合方法,以改善前列腺癌管理中的BET抑制的治疗指标。临床前数据已鉴定出几种分子靶标,可以提高临床中的BET抑制的影响。本综述将使已知的临床前数据暗示投注作为晚期前列腺癌中的重要治疗目标,突出了靶向该蛋白质家族的持续临床试验,并推测使用Beti与前列腺癌中的其他药剂一起使用的理由组合策略。使用Pubmed进行了一个文献搜索,对该评论进行了.Pert意见:在治疗MCRPC患者的治疗中使用Beti可能需要添加第二种新试剂。

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