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首页> 外文期刊>Molecular cancer therapeutics >BGB-283, a Novel RAF Kinase and EGFR Inhibitor, Displays Potent Antitumor Activity in BRAF-Mutated Colorectal Cancers
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BGB-283, a Novel RAF Kinase and EGFR Inhibitor, Displays Potent Antitumor Activity in BRAF-Mutated Colorectal Cancers

机译:BGB-283,一种新型RAF激酶和EGFR抑制剂,在BRAF-突变的结肠直肠癌中显示有效的抗肿瘤活性

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摘要

Oncogenic BRAF, which drives cell transformation and proliferation, has been detected in approximately 50% of human malignant melanomas and 5% to 15% of colorectal cancers. Despite the remarkable clinical activities achieved by vemurafenib and dabrafenib in treating BRAF(V600E) metastatic melanoma, their clinical efficacy in BRAF(V600E) colorectal cancer is far less impressive. Prior studies suggested that feedback activation of EGFR and MAPK signaling upon BRAF inhibition might contribute to the relative unresponsiveness of colorectal cancer to the first-generation BRAF inhibitors. Here, we report characterization of a dual RAF kinase/EGFR inhibitor, BGB-283, which is currently under clinical investigation. In vitro, BGB-283 potently inhibits BRAF(V600E)-activated ERK phosphorylation and cell proliferation. It demonstrates selective cytotoxicity and preferentially inhibits proliferation of cancer cells harboring BRAF(V600E) and EGFR mutation/amplification. In BRAF(V600E) colorectal cancer cell lines, BGB-283 effectively inhibits the reactivation of EGFR and EGFR-mediated cell proliferation. In vivo, BGB-283 treatment leads to dose-dependent tumor growth inhibition accompanied by partial and complete tumor regressions in both cell line-derived and primary human colorectal tumor xenografts bearing BRAF(V600E) mutation. These findings support BGB-283 as a potent antitumor drug candidate with clinical potential for treating colorectal cancer harboring BRAF(V600E) mutation. (C) 2015 AACR.
机译:在大约50%的人恶性黑素瘤中检测到细胞转化和增殖的致癌BRAF和5%至15%的结肠直肠癌。尽管Vemurafenib和Dabrafenib在治疗BRAF(V600E)转移性黑色素瘤中实现了显着的临床活动,但它们在BRAF(V600E)结直肠癌中的临床疗效远不太令人印象深刻。结果表明,在BRAF抑制时EGFR和MAPK信号传导的反馈激活可能导致结直肠癌与第一代BRAF抑制剂的相对反应性。在此,我们报告目前正在临床研究的双RAF激酶/ EGFR抑制剂,BGB-283的表征。体外,BGB-283有效地抑制BRAF(V600E) - 活化的ERK磷酸化和细胞增殖。它证明了选择性细胞毒性,优先抑制患有BRAF(V600E)和EGFR突变/扩增的癌细胞的增殖。在BRAF(V600E)结直肠癌细胞系中,BGB-283有效地抑制EGFR和EGFR介导的细胞增殖的再活化。在体内,BGB-283处理导致剂量依赖性肿瘤生长抑制,其含有BRAF(V600E)突变的细胞系衍生和原发性人结晶瘤卵黄移植物中的部分和完全肿瘤回归。这些发现支持BGB-283作为一种有效的抗肿瘤药物候选者,其临床电位治疗含BRAF(V600E)突变的结肠直肠癌。 (c)2015年AACR。

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  • 来源
    《Molecular cancer therapeutics》 |2015年第10期|共11页
  • 作者

    Tang Zhiyu; Yuan Xi; Du Rong; Cheung Shing-Hu; Zhang Guoliang; Wei Jing; Zhao Yuan; Feng Yingcai; Peng Hao; Zhang Yi; Du Yunguang; Hu Xiaoxia; Gong Wenfeng; Liu Yong; Gao Yajuan; Liu Ye; Hao Rui; Li Shengjian; Wang Shaohui; Ji Jiafu; Zhang Lianhai; Li Shuangxi; Sutton David; Wei Min; Zhou Changyou; Wang Lai; Luo Lusong;

  • 作者单位

    BeiGene Beijing Co Ltd Dept In Vivo Pharmacol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Discovery Biol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Discovery Biol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Discovery Biol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Chem Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Discovery Biol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Discovery Biol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept In Vivo Pharmacol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept In Vivo Pharmacol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept In Vivo Pharmacol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept In Vivo Pharmacol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Chem Beijing 102206 Peoples R China;

    Peking Univ Canc Hosp &

    Inst Dept Surg Key Lab Carcinogenesis &

    Translat Res Minist Educ;

    Peking Univ Canc Hosp &

    Inst Dept Surg Key Lab Carcinogenesis &

    Translat Res Minist Educ;

    Peking Univ Canc Hosp &

    Inst Dept Surg Key Lab Carcinogenesis &

    Translat Res Minist Educ;

    BeiGene Beijing Co Ltd Dept In Vivo Pharmacol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Mol Sci Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Chem Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept In Vivo Pharmacol Beijing 102206 Peoples R China;

    BeiGene Beijing Co Ltd Dept Discovery Biol Beijing 102206 Peoples R China;

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  • 正文语种 eng
  • 中图分类 肿瘤学;
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