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Targeting RAF kinases for cancer therapy: BRAF-mutated melanoma and beyond

机译:靶向RAF激酶用于癌症治疗:BRAF突变的黑色素瘤及其他

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The identification of mutationally activated BRAF in many cancers altered our conception of the part played by the RAF family of protein kinases in oncogenesis. In this Review, we describe the development of BRAF inhibitors and the results that have emerged from their analysis in both the laboratory and the clinic. We discuss the spectrum of RAF mutations in human cancer and the complex interplay between the tissue of origin and the response to RAF inhibition. Finally, we enumerate mechanisms of resistance to BRAF inhibition that have been characterized and postulate how strategies of RAF pathway inhibition may be extended in scope to benefit not only the thousands of patients who are diagnosed annually with BRAF-mutated metastatic melanoma but also the larger patient population with malignancies harbouring mutationally activated RAF genes that are ineffectively treated with the current generation of BRAF kinase inhibitors.
机译:在许多癌症中,突变激活的BRAF的鉴定改变了我们对RAF蛋白激酶家族在肿瘤发生中所起的作用的认识。在本综述中,我们描述了BRAF抑制剂的开发以及从实验室和临床分析中得出的结果。我们讨论了人类癌症中RAF突变的谱以及起源组织与RAF抑制反应之间的复杂相互作用。最后,我们列举了已表征的对BRAF抑制的抗性机制,并提出了如何扩展RAF途径抑制策略的范围,不仅使每年诊断为BRAF突变的转移性黑色素瘤的数千名患者受益,而且使较大的患者受益携带具有突变激活的RAF基因的恶性肿瘤人群,目前无法使用目前的BRAF激酶抑制剂对其进行有效治疗。

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