转移性或不能手术的BRAF v600阳性黑色素瘤:多活几个月。

Q4 Medicine
Prescrire International Pub Date : 2016-12-01
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引用次数: 0

摘要

约50%的变静态或不能手术的黑色素瘤患者携带BRAF V600突变的肿瘤。这些患者的首选药物是vemurafenib,一种BRAF抑制剂,似乎可以延长几个月的生存期。Dabrafenib是一种vemurafenib仿制药,其已知的不良反应略有不同。Trametinib是一种MEK抑制剂,现已在欧盟被批准用于这种情况,无论是作为单药治疗还是与dabrafenib联合使用(由同一家公司销售)。尚未将曲美替尼单药治疗与BRAF抑制剂单药治疗进行比较。在一项随机、非盲法试验中,322名患者与细胞毒性药物相比,两组间的中位生存时间无统计学差异(15.6个月对11.3个月;P = 0.09),但化疗组65%的患者在疾病进展后接受曲美替尼治疗,这使得更难检测组间差异。在一项无盲随机对照试验中,704例从未接受过转移性或不可手术性疾病治疗的患者,曲美替尼+达非尼联合治疗比vemurafenib延长中位生存期约8个月。在另一项423例患者的双盲随机对照试验中,曲美替尼+达非尼的中位生存期比安慰剂+达非尼的中位生存期长约6个月。在非比较性试验中,在BRAF抑制剂失效后,曲美替尼+达非尼联合治疗效果不佳,该试验包括几十例患者,其中唯一的终点是肿瘤反应。曲美替尼有许多不良反应,其中一些可能危及生命,如心力衰竭、深静脉血栓形成、出血(包括颅内出血)、中性粒细胞减少和胃肠道穿孔。曲美替尼还会引起视网膜疾病和肺炎。曲美替尼与达非尼联用可降低与达非尼相关的角化过度和皮肤癌的风险,但会增加发烧的频率(包括高热)。曲美替尼的相互作用主要包括加性作用或拮抗作用。在实践中,当患有转移性或无法手术的BRAF v600阳性黑色素瘤的患者愿意接受曲美替尼的显著毒性,希望获得额外几个月的生命时,曲美替尼+达非尼联合治疗是一线选择。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Trametinib (MEKINIST°) Metastatic or inoperable BRAF V600-positive melanoma: a few extra months of life.

About 50% of patients with meta- static or inoperable melanoma carry a tumour with BRAF V600 mutation.The drug of first choice for these patients is vemurafenib, a BRAF inhibitor, which appears to prolong survival by a few months. Dabrafenib is a vemurafenib me-too with a slightly different known profile of adverse effects. Trametinib, a MEK inhibitor, is now authorised in the European Union for use in this setting, either as monotherapy or in combination with dabrafenib (marketed by the same company). Trametinib monotherapy has not been compared to BRAF inhibitor monotherapy. In a randomised, unblinded trial versus cytotoxic drugs in 322 patients, the median survival time did not differ statistically between the groups (15.6 versus 11.3 months; p = 0.09), but 65% of patients in the chemotherapy group received trametinib after disease pro- gression, making it more difficult to detect a difference between the groups. In an unblinded randomised controlled trial in 704 patients who had never received treatment for metastatic or inoperable disease, the trametinib + dabrafenib combination prolonged median survival by about 8 months more than vemurafenib. In another double-blind randomised controlled trial in 423 patients, median survival was about 6 months longer with trametinib + dabrafenib than with placebo + dabrafenib. The trametinib+ dabrafenibcombination was poorly effective after BRAF inhibitor failure in non-comparative trials including a few dozen patients in which the only endpoint was tumour response. Trametinib has many adverse effects, some of which can be life-threatening, such as heart failure, deep vein thrombosis, bleeding (including intracranial haemorrhage), neutropenia, and gastrointestinal perforation. Trametinib also causes retinal disorders and pneumonitis. Combining trametinib with dabrafenib reduces the risk of hyperkeratosis and skin cancer associated with dabrafenib, but increases the frequency of fever (including very high fever). Trametinib interactions mainly involve additive effects or antagonism. In practice, when a patient with metastatic or inoperable BRAF V600-positive melanoma is willing to accept the significant toxicity of trametinib in the hope of gaining several extra months of life, the trametinib + dabrafenib combination is a first-line option.

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来源期刊
Prescrire International
Prescrire International Medicine-Pharmacology (medical)
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