转移性黑色素瘤个体化治疗提供新方案

2010-08-28 MedSci原创 MedSci原创

抑制转移性黑色素瘤中突变、活化的BRAF Inhibition of Mutated, Activated BRAF in Metastatic Melanoma   基思·T·弗莱厄蒂等 美国宾夕法尼亚大学艾布拉姆森癌症中心等 N Engl J Med 2010;363:809-19. August 26, 2010   背景 在大多数黑色素瘤中可检出丝氨酸—苏氨酸蛋白激酶B-RAF编

抑制转移性黑色素瘤中突变、活化的BRAF

Inhibition of Mutated, Activated BRAF in Metastatic Melanoma

  基思·T·弗莱厄蒂等 美国宾夕法尼亚大学艾布拉姆森癌症中心等

N Engl J Med 2010;363:809-19. August 26, 2010

  背景 在大多数黑色素瘤中可检出丝氨酸—苏氨酸蛋白激酶B-RAF编码基因(BRAF)的体细胞突变,这为检验针对这种肿瘤的癌基因靶向疗法提供了机会。

  方法 我们进行了一项有关PLX4032(又称RG7204,一种可以口服的突变BRAF的抑制剂)的多中心、Ⅰ期、剂量递增试验,并在随后的扩展期中检验不出现不良反应的最大可用剂量(推荐的Ⅱ期剂量)。病人接受PLX4032,每天2次,直到其病变进展。所有病人都接受了药代动力学分析和肿瘤疗效反应评估。部分病人在治疗前和治疗期间接受了肿瘤活检,以证实BRAF受抑。

  结果 共55例病人(其中49例有黑色素瘤)在剂量递增期被纳入研究,另外32例有BRAF V600E突变的转移性黑色素瘤病人,在扩展期被纳入研究。推荐的Ⅱ期剂量是960 mg,每天2次,当患者出现2级或3级皮疹、乏力和关节痛时,剂量不再增加。在剂量递增队列中,在16例肿瘤携带V600E BRAF突变和正在接受PLX4032≥240 mg(每天2次)治疗的黑色素瘤病人中,10例部分缓解,1例完全缓解。在扩展队列的32例病人中,24例部分缓解,2例完全缓解。所有病人中的估计无进展生存期中位数超过7个月。

  结论 对于肿瘤携带V600E BRAF突变的病人,采用PLX4032治疗转移性黑色素瘤,可使大部分病人的肿瘤完全或部分消退。

原始链接[PDF文件下载]:http://www.nejm.org/doi/pdf/10.1056/NEJMoa1002011


MedSci点评:

    实际上本文在2010年美国皮肤病年会上已公布了部分结果。而此篇文章是较为完整的I期临床研究的结果。PLX4032可以使BRAF原癌基因突变型转移性黑色素瘤患者带来治疗希望,而这类患者原来几乎是无药可治。

    本文有三大创新点:(1)从研究角度上看,这是典型的“个性化医疗”“基因组分型选择药物”的典型案例。它的发表,也将推动人类继续研究合适的基因型治疗药物,是具有重要意义的。(2)实验设计严谨。它是严格的I期临床试验的结果;(3)PLX4032是有一种极有希望的药物。它的巨大疗效也是吸引人的地方。这三点是促使文章发表在《新英格兰》杂志上的重要原因。

    PLX4032最初由加州伯克利的Plexxikon公司设计,之后罗氏公司也参与了研发。研究者表示,该药不是一种万灵药,对于部分患者而言,该药起效迅速,很明显这是一项重大突破,但还有很大一部分患者在用药后肿瘤还是发生了进展。

    未来,还会针对这一药物,有更多的文章出现。 

 

用Ipilimumab改善转移性黑色素瘤病人的生存

Improved Survival with Ipilimumab in Patients with Metastatic Melanoma

  F·斯蒂芬·霍迪等 美国波士顿市达纳—法伯癌症研究所等

N Engl J Med 2010; 363:711-23. August 19, 2010

  背景 改善转移性黑色素瘤病人的总体生存,一直是一个难以实现的目标。Ipilimumab可阻滞细胞毒性T淋巴细胞相关抗原4,以增强抗肿瘤T细胞应答。在这项Ⅲ期研究中,研究者在既往接受过治疗的转移性黑色素瘤病人中,对单用ipilimumab或加用糖蛋白100(gp100)肽疫苗的效果,与单用 gp100的效果进行了比较。

  方法 本研究共纳入676例HLA-A*0201阳性,有不可切除Ⅲ期或Ⅳ期黑色素瘤的患者,其病情在他们接受转移瘤治疗期间已发生进展,研究者按3:1:1的比例将患者随机分为3组:第1组接受ipilimumab加gp100治疗(403例病人),第2组仅接受ipilimumab治疗(137例),第3组接受单纯gp100治疗(136例)。Ipilimumab的剂量为3 mg/kg体重,加用或不加用gp100,每3周1次,最多进行4次治疗(诱导)。符合条件的病人可接受再诱导疗法。主要终点是总生存期。

  结果 总生存期中位数在接受ipilimumab加gp100治疗的病人中为10.0个月,相比之下,在接受单纯gp100治疗的病人中为6.4个月(死亡的风险比为0.68,P<0.001)。单纯使用ipilimumab(患者)的总生存期中位数为10.1个月(与单用gp100相比的死亡风险比是 0.66,P=0.003)。研究者发现,两个ipilimumab治疗组之间在总生存期上无(显著)差异(使用ipilimumab加gp100的风险比为1.04,P=0.76)。在10%~15%接受ipilimumab治疗的病人中,以及在3%接受单纯gp100治疗的病人中,发生了3级或4级免疫相关性不良事件。发生了14例(2.1%)与该研究药物相关的死亡,而且7例与免疫相关性不良事件有关。

  结论 在既往接受过治疗的转移性黑色素瘤病人中,与单用gp100相比,ipilimumab单用或与gp100肽疫苗联用,可改善其总生存期。不良事件可能是严重的和(或)持久的,但如果处理得当多数是可逆的。  


MedSci点评:

    这是上一期新英格兰杂志上的文章,与上一篇几乎完全类似,只是研究的药物不同,病例选择不同。本篇文章选择的是676例HLA-A*0201阳性,有不可切除Ⅲ期或Ⅳ期黑色素瘤的患者。同样,这也是个性化医疗的重要的代表。

    另外,在西方白人中,恶性黑色素瘤的发生率比较高,也是一直受到关注的对象。而本篇的特色之一在于ipilimumab药物与/不与gp100合作进行治疗。研究设计是十分严谨的。

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    2010-12-31 sunylz
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