PNAS:FGFR4 ,MAP3K9和PAK5可能成为非小细胞肺癌(NSCLC)的潜在治疗靶点

2013-07-13 MedSci MedSci原创

       肺癌是最难研究的癌症之一,有一半的非小细胞肺癌仍然不清楚其潜在遗传改变。当前科学家可以用药物或其他治疗靶向的遗传标记非常之少。而改善肺癌的生存是目前研究人员的当务之急。  日前,英国癌症研究中心的研究人员首次利用一种高效的新筛选策略,确定了最常见肺癌类型肿瘤细胞中的基因缺陷。这项研究为个体化治疗患者肿瘤,实时鉴别潜在的药物靶点提供了一种新方法。

肺癌
  

    
肺癌是最难研究的癌症之一,有一半的非小细胞肺癌仍然不清楚其潜在遗传改变。当前科学家可以用药物或其他治疗靶向的遗传标记非常之少。而改善肺癌的生存是目前研究人员的当务之急。

  日前,英国癌症研究中心的研究人员首次利用一种高效的新筛选策略,确定了最常见肺癌类型肿瘤细胞中的基因缺陷。这项研究为个体化治疗患者肿瘤,实时鉴别潜在的药物靶点提供了一种新方法。

  在这项刊登在PNAS杂志上的研究中,科学家们对实验室中培养的 6 种不同的非小细胞肺癌(NSCLC)细胞系进行了研究,每种细胞系已知携带了超过60个基因缺陷。为了确切地查明哪些缺陷驱动了癌症,科学家们特异采用依次关闭一个不同的缺陷基因的方法,来观察了它们对于细胞生长的影响。

  最终,研究小组发现有三个重要的基因: FGFR4 、 MAP3K9 和 PAK5 发生缺陷会导致生成过度活化的蛋白,由此向细胞发生信号导致其生长失控。

  研究人员表示,新技术使得研究人员能够开始绘制出最有可能驱动这些癌症生长的基因缺陷的图谱。这一重要的研究工作将推动更早实现肺癌患者个体化治疗。了解驱动个体患者癌症的遗传缺陷,将有助于确保研究人员在正确的时间得到正确的治疗。

原始出处:

Fawdar S, Trotter EW, Li Y, Stephenson NL, Hanke F, Marusiak AA, Edwards ZC, Ientile S, Waszkowycz B, Miller CJ, Brognard J. Targeted genetic dependency screen facilitates identification of actionable mutations in FGFR4, MAP3K9, and PAK5 in lung cancer.Proc Natl Acad Sci U S A. 2013 Jul 8.

PDF文件下载:1305207110.full.pdf

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    2013-08-21 drwjr
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    2013-07-14 liuyiping

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随着表皮生长因子受体酪氨酸激酶抑制剂(EGFR-TKIs)如:易瑞沙、特罗凯等广泛的应用,越来越多的研究表明EGFR突变与癌症家族史有着密切的关系。来自同济大学上海肺科医院的周彩存等针对中国地区的患者进行了一项前沿性分析实验,该研究结果发表在2013年5月30日的肺癌(Lung Cancer)杂志。该研究结果表明具有癌症家族史的非小细胞肺癌患者尤其是具有肺癌家族史的患者,具有较高的EGFR突变率。

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7月5日,记者在中科院广州生物医药与健康研究院获悉,该院科学家在克服非小细胞肺癌耐药研究方面获得新突破。相关结果在美国《药物化学杂志》和德国《应用化学》上在线发表。 肺癌是严重威胁人类健康的重大疾病,非小细胞肺癌则占所有类型肺癌的85%以上。目前,表皮生长因子(EGFR)受体抑制剂易瑞沙(吉非替尼)和特罗凯(埃罗替尼)等已在临床治疗非小细胞肺癌中获得巨大成功,但其耐药问题也日益突出。第二