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首页> 外文期刊>Nature reviews. Clinical oncology >Advances in targeted therapies for hepatocellular carcinoma in the genomic era
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Advances in targeted therapies for hepatocellular carcinoma in the genomic era

机译:基因组时代肝细胞靶向治疗的研究进展

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Mortality owing to liver cancer has increased in the past 20 years, and the latest estimates indicate that the global health burden of this disease will continue to grow. Most patients with hepatocellular carcinoma (HCC) are still diagnosed at intermediate or advanced disease stages, where curative approaches are often not feasible. Among the treatment options available, the molecular targeted agent sorafenib is able to significantly increase overall survival in these patients. Thereafter, up to seven large, randomized phase III clinical trials investigating other molecular therapies in the first-line and second-line settings have failed to improve on the results observed with this agent. Potential reasons for this include intertumour heterogeneity, issues with trial design and a lack of predictive biomarkers of response. During the past 5 years, substantial advances in our knowledge of the human genome have provided a comprehensive picture of commonly mutated genes in patients with HCC. This knowledge has not yet influenced clinical decision-making or current clinical practice guidelines. In this Review the authors summarize the molecular concepts of progression, discuss the potential reasons for clinical trial failure and propose new concepts of drug development, which might lead to clinical implementation of emerging targeted agents.
机译:在过去的20年中,由于肝癌导致的死亡率增加了,最新估计表明,这种疾病的全球健康负担将继续增加。多数肝细胞癌(HCC)患者仍被诊断为处于中晚期疾病阶段,而通常无法采用治愈方法。在可用的治疗选择中,分子靶向药物索拉非尼能够显着提高这些患者的总体生存率。此后,多达七项大型的,随机的,涉及第一线和第二线环境中其他分子疗法研究的III期临床试验未能改善使用该药物观察到的结果。造成这种情况的潜在原因包括肿瘤间异质性,试验设计问题以及缺乏预测的反应性生物标志物。在过去的五年中,我们对人类基因组知识的实质性进步为HCC患者的常见突变基因提供了全面的了解。该知识尚未影响临床决策或当前的临床实践指南。在本综述中,作者总结了进展的分子概念,讨论了临床试验失败的潜在原因,并提出了药物开发的新概念,这可能会导致新兴的靶向药物在临床上得到应用。

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