化疗提高晚期非小细胞肺癌的生存率和降低毒性:一个现实的目标?

Fiona H Blackhall, Frances A Shepherd, Kathy S Albain
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引用次数: 36

摘要

化疗在晚期非小细胞肺癌(NSCLC)治疗中的作用已经争论了30多年,但直到最近,化疗才成为这种疾病的标准治疗方法。除了延长生存期,化疗还能缓解令人痛苦的症状。对化疗的副作用可能超过其益处的担忧在很大程度上没有得到表现良好的患者的生活质量数据的证实。在以铂为基础的化疗方案中,顺铂或卡铂与第三代细胞毒性药物(如吉西他滨、紫杉醇或长春瑞滨)联合使用,具有相似的活性和疗效,但在不良反应方面有所不同。预期有效率为30-40%,中位和1年生存率分别为8-10个月和30-40%。在二线治疗中,多西紫杉醇化疗已被证明明显优于单用最佳支持治疗。在最近的一项试验中,将多西他赛与新型抗叶酸药培美曲塞进行比较,反应率和生存率没有差异,但毒性谱偏向培美曲塞。总的来说,这些数据表明,在不增加进一步毒性发生率的情况下,化疗在提高NSCLC患者生存率方面取得了进展。在过去,存活1年的可能性非常小,而现在更多的患者达到了这一里程碑和2年。然而,现有的细胞毒性药物可能已经达到平台期,人们普遍认为,NSCLC治疗的下一个重大进展将来自于在标准化疗方案中按顺序添加靶向特定分子途径的药物。
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Improving survival and reducing toxicity with chemotherapy in advanced non-small cell lung cancer : a realistic goal?

The role of chemotherapy in the treatment of advanced non-small cell lung cancer (NSCLC) has been debated over three decades, but it is only relatively recently that chemotherapy has become a standard of care for this disease. In addition to prolonging survival, chemotherapy can palliate distressing symptoms. Concerns that the adverse effects of chemotherapy are likely to outweigh its benefits have largely not been confirmed by quality-of-life data reported among patients with good performance status. Platinum-based chemotherapy regimens in which cisplatin or carboplatin are partnered by a third-generation cytotoxic drug such as gemcitabine, paclitaxel or vinorelbine, have similar activity and efficacy, but differ in adverse effect profiles. Response rates of 30-40% should be expected with median and 1-year survival of 8-10 months and 30-40%, respectively. In the second-line setting chemotherapy with docetaxel has been shown to be significantly superior to best supportive care alone. In a recent trial that compared docetaxel to the novel antifolate, pemetrexed the response rates and survival rates did not differ, but the toxicity profile favored pemetrexed. Overall, these data demonstrate that progress has been made in the use of chemotherapy to improve survival in patients with NSCLC without increasing the incidence of further toxicity. In the past, the potential to survive 1 year was extremely small, whereas now many more patients reach this milestone as well as the 2-year point. However, a plateau has probably been reached with existing cytotoxic drugs and there is a general belief that the next significant advance in the treatment of NSCLC will come from the addition of drugs that target specific molecular pathways in sequence with standard chemotherapy regimens.

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