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Potential Therapeutic Strategies to Overcome Acquired Resistance to BRAF or MEK Inhibitors in BRAF Mutant Cancers

机译：克服BRAF突变型癌症对BRAF或MEK抑制剂获得性耐药的潜在治疗策略

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Recent clinical trials with selective inhibitors of the BRAF and MEK kinases have shown promising results in patients with tumors harboring BRAF V600 mutations. However, as has been observed previously with similarly successful targeted therapies, acquired resistance to these agents is an emerging problem that limits their clinical benefit. Several recent studies from our laboratory and others have investigated the causes of acquired resistance to BRAF and MEK inhibitors, and multiple resistance mechanisms have been identified. Here, we review these mechanisms and suggest that they can be broadly grouped into two main classes: ERK-dependent and ERK-independent. We also propose distinct therapeutic strategies that might be employed to overcome each class of acquired resistance.

机译：最近使用BRAF和MEK激酶选择性抑制剂的临床试验显示，在患有携带BRAF V600突变的肿瘤患者中，结果令人鼓舞。然而，如先前在类似的成功靶向治疗中所观察到的，对这些药物的后天耐药性是一个正在出现的问题，限制了它们的临床益处。我们实验室和其他研究机构最近进行的一些研究已经调查了对BRAF和MEK抑制剂获得抗药性的原因，并确定了多种抗药性机制。在这里，我们回顾这些机制，并建议将它们大致分为两大类：ERK依赖性和ERK依赖性。我们还提出了独特的治疗策略，可以用来克服获得性耐药的每一类。

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Corcoran, Ryan B.; Settleman, Jeffrey; Engelman, Jeffrey A.;
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年度 2011
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原文格式 PDF
正文语种 {"code":"en","name":"English","id":9}
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专利

1. Combinations of BRAF, MEK, and PI3K/mTOR Inhibitors Overcome Acquired Resistance to the BRAF Inhibitor GSK2118436 Dabrafenib, Mediated by NRAS or MEK Mutations. [J] . James G Greger, Stephen D Eastman, Vivian Zhang, Molecular cancer therapeutics . 2012,第4期

机译：由NRAS或MEK突变介导的BRAF，MEK和PI3K / mTOR抑制剂的组合克服了对BRAF抑制剂GSK2118436 Dabrafenib的获得性耐药。
2. The Novel ATP-Competitive MEK/Aurora Kinase Inhibitor BI-847325 Overcomes Acquired BRAF Inhibitor Resistance through Suppression of Mcl-1 and MEK Expression [J] . Phadke Manali S., Sini Patrizia, Smalley Keiran S. M. Molecular cancer therapeutics . 2015,第6期

机译：新型ATP竞争性MEK / Aurora激酶抑制剂BI-847325通过抑制MCL-1和MEK表达来克服获得的BRAF抑制剂抗性
3. Inhibition of HSP90 by AT13387 Delays the Emergence of Resistance to BRAF Inhibitors and Overcomes Resistance to Dual BRAF and MEK Inhibition in Melanoma Models [J] . Smyth Tomoko, Paraiso Kim H. T., Hearn Keisha, Molecular cancer therapeutics . 2014,第12期

机译：AT13387对HSP90的抑制作用会延迟对BRAF抑制剂的耐药性出现，并克服黑色素瘤模型对BRAF和MEK双重抑制的耐药性
4. Gene Expression Models of BRAF Inhibitor Resistance in Melanoma Predict Drug Repurposing Candidates for Novel Combination Therapies [C] . Kelly Regan, Andrew R. Stiff, William E. Carson, International Molecular Medicine Tri-Conference. . 2016

机译：黑色素瘤中BRAF抑制剂抗性的基因表达模型预测了新型组合疗法的药物重新培养候选者
5. Optimizing MEK Inhibitors in NRAS Mutant Melanoma - Overcoming Resistance and Combination Strategies [D] . Nguyen, Mai. 2021

机译：优化NRAS突变体黑素瘤耐久性和组合策略中的MEK抑制剂
6. Potential Therapeutic Strategies to Overcome Acquired Resistance to BRAF or MEK Inhibitors in BRAF Mutant Cancers [O] . Ryan B. Corcoran, Jeffrey Settleman, Jeffrey A. Engelman 2011

机译：克服BRAF突变型癌症对BRAF或MEK抑制剂获得性耐药的潜在治疗策略
7. Combinations of BRAF, MEK, and PI3K/mTOR Inhibitors Overcome Acquired Resistance to the BRAF Inhibitor GSK2118436 Dabrafenib, Mediated by NRAS or MEK Mutations [O] . James G. Greger, Stephen D. Eastman, Vivian Zhang, 2012

机译：BRAF，MEK和PI3K / MTOR抑制剂的组合克服了由NRAS或MEK突变介导的BRAF抑制剂GSK2118436 Dabrafenib的获得性抗性

Potential Therapeutic Strategies to Overcome Acquired Resistance to BRAF or MEK Inhibitors in BRAF Mutant Cancers

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