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EGF receptor as a therapeutic target: patient selection and mechanisms of resistance to receptor-targeted drugs.

机译:EGF受体作为治疗目标:患者选择和对受体靶向药物的耐药机制。

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摘要

Emerging results from clinical trials of epidermal growth factor receptor (EGFR) inhibitors indicate good tolerability and at best modest to no clinical activity in a variety of human carcinomas. The lack of molecular evidence to suggest a pathogenic role for the EGFR in most common solid tumors is not inconsistent with the modest clinical activity observed in these single-agent trials. In addition, the lack of enrollment of patients with EGFR-dependent tumors onto these trials leaves open the possibility that these studies may have included some tumors that benefited from these therapies but for which this benefit was diluted and thus not detected within the enrolled patient population at large. These considerations suggest that the enrollment of unselected patients onto trials with EGFR inhibitors should be revisited to identify a cohort of EGFR-dependent tumors against which EGFR inhibitors might exhibit clinical activity. This approach would also exclude patients for whom these drugs will not induce any clinical benefit.
机译:表皮生长因子受体(EGFR)抑制剂临床试验的最新结果表明,在多种人类癌症中,耐受性良好,至多没有或几乎没有临床活性。缺乏分子证据表明EGFR在大多数常见实体瘤中具有致病作用并不与这些单药试验中观察到的适度临床活动相矛盾。另外,缺乏EGFR依赖性肿瘤患者入组这些试验使这些研究可能包括一些受益于这些疗法但被稀释但因此在入组患者人群中未发现的肿瘤的可能性成为可能。大体上。这些考虑表明,应重新筛选未入选患者的EGFR抑制剂试验,以鉴定EGFR抑制剂可能针对其表现临床活性的EGFR依赖性肿瘤队列。这种方法还将排除这些药物不会为其带来任何临床益处的患者。

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