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首页> 外文期刊>Cancer: A Journal of the American Cancer Society >Enhancing endocrine response with novel targeted therapies: why have the clinical trials to date failed to deliver on the preclinical promise?
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Enhancing endocrine response with novel targeted therapies: why have the clinical trials to date failed to deliver on the preclinical promise?

机译:通过新型靶向疗法增强内分泌反应:为什么迄今为止的临床试验未能实现临床前承诺?

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摘要

Acquired resistance to endocrine therapies has severely limited their long-term effectiveness in breast cancer. In recent years a clear rationale has developed for combining signal transduction inhibitors (STIs) with endocrine therapies to delay the emergence of acquired resistance and enhance endocrine responsiveness. A variety of biologic agents have been developed to target key proteins along the EGFR, HER2, MAPK, and P13K/Akt signal transduction cascades. While several of these agents have shown early promise in selected breast cancer models, translating these data into convincing clinical results has been generally disappointing to date. By applying more rigorous trial design and tumor selection criteria to future trials, it is much more likely that adding the new generation of targeted therapies can fulfill its promise in enhancing endocrine responsiveness and our ability to treat breast cancer patients.
机译:获得的对内分泌疗法的抵抗力严重限制了它们在乳腺癌中的长期有效性。近年来,人们已经明确提出将信号转导抑制剂(STIs)与内分泌治疗相结合以延缓获得性耐药的出现并增强内分泌反应性的基本原理。已经开发出多种生物制剂来靶向EGFR,HER2,MAPK和P13K / Akt信号转导级联反应中的关键蛋白。尽管这些药物中的几种已在选定的乳腺癌模型中显示出早期希望,但迄今为止,将这些数据转化为令人信服的临床结果一直令人失望。通过将更严格的试验设计和肿瘤选择标准应用于未来的试验中,增加新一代靶向疗法的可能性更有可能实现其在增强内分泌反应性和我们治疗乳腺癌患者能力方面的承诺。

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