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Not just gRASping at flaws: Finding vulnerabilities to develop novel therapies for treating KRAS mutant cancers

机译：不仅探究缺陷：发现漏洞以开发新的疗法来治疗KRAS突变型癌症

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Mutations in Kirsten rat-sarcoma (KRAS) are well appreciated to be major drivers of human cancers through dysregulation of multiple growth and survival pathways. Similar to many other non-kinase oncogenes and tumor suppressors, efforts to directly target KRAS pharmaceutically have not yet materialized. As a result, there is broad interest in an alternative approach to develop therapies that induce synthetic lethality in cancers with mutant KRAS, therefore exposing the particular vulnerabilities of these cancers. Fueling these efforts is our increased understanding into the biology driving KRAS mutant cancers, in particular the important pathways that mutant KRAS governs to promote survival. In this mini-review, we summarize the latest approaches to treat KRAS mutant cancers and the rationale behind them.

机译：克尔斯滕大鼠肉瘤（KRAS）中的突变通过多种生长和生存途径的失调而被公认为是人类癌症的主要驱动因素。与许多其他非激酶癌基因和肿瘤抑制物相似，直接靶向KRAS药物的努力尚未实现。因此，人们对替代方法的开发产生了广泛的兴趣，这些方法可在具有突变KRAS的癌症中诱导合成致死性，从而暴露出这些癌症的特殊脆弱性。推动这些努力的是我们对驱动KRAS突变型癌症的生物学方法的了解日益加深，尤其是突变KRAS支配的促进生存的重要途径。在此小型审查中，我们总结了治疗KRAS突变型癌症的最新方法及其背后的原理。

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期刊名称 Cancer Science
作者
Hiromichi Ebi; Anthony C Faber; Jeffrey A Engelman; Seiji Yano;
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作者单位

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年(卷),期 2014(105),5
年度 2014
页码 499–505
总页数 7
原文格式 PDF
正文语种
中图分类肿瘤学;
关键词
Apoptosis Kirsten rat-sarcoma MEK phosphatidylinositol 3-kinase synthetic lethality;

机译：凋亡;克尔斯滕大鼠肉瘤;MEK;磷脂酰肌醇3-激酶;合成杀伤力;

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专利

1. KRAS G12C抑制剂联合其他药物治疗KRAS G12C突变型非小细胞肺癌的研究进展 [J] . 王雅丽, 陈秀琼, 郑琨, 癌症（英文版） . 2020,第009期
2. Not just gRASping at flaws: Finding vulnerabilities to develop novel therapies for treating KRAS mutant cancers [J] . Ebi Hiromichi, Faber Anthony C., Engelman Jeffrey A., Cancer science. . 2014,第5期

机译：不仅探究缺陷：发现漏洞以开发新的疗法来治疗KRAS突变型癌症
3. Not just gRASping at flaws: Finding vulnerabilities to develop novel therapies for treating KRAS mutant cancers [J] . Anthony C. Faber, Hiromichi Ebi, Jeffrey A. Engelman Cancer science. . 2014,第5期

机译：不仅探究缺陷：发现漏洞以开发新的疗法来治疗KRAS突变型癌症
4. Bevacizumab plus chemotherapy continued beyond first progression in patients with metastatic colorectal cancer previously treated with bevacizumab plus chemotherapy: ML18147 study KRAS subgroup findings [J] . Kubicka S., Greil R., Andre T., Annals of oncology: official journal of the European Society for Medical Oncology . 2013,第9期

机译：对于先前接受过贝伐单抗联合化疗治疗的转移性结直肠癌患者，贝伐单抗联合化疗继续超过首次进展：ML18147研究KRAS亚组发现
5. L-Ascorbic Acid Can Abrogate X Gene-Dependent Cetuximab Resistance Mediated by Mutant KRAS in Human Colon Cancer Cells [C] . Soo-A Jung, Jai-Hee Moon, Ih Yeon Hwang, International Molecular Medicine Tri-Conference. . 2016

机译：L-抗坏血酸可以消除突变克拉斯在人结肠癌细胞中介导的X基因依赖性的辛酸抗性
6. Targeting mutant KRAS in pancreatic cancer. [D] . Hayes, Tikvah Katheryn. 2016

机译：针对胰腺癌中的突变KRAS。
7. Relevance of Pharmacogenomics and Multidisciplinary Management in a Young-Elderly Patient With KRAS Mutant Colorectal Cancer Treated With First-Line Aflibercept-Containing Chemotherapy [O] . Gemma Bruera, Antonio DAndrilli, Maurizio Simmaco, 2020

机译：用含有含有含有一线含AFLibercept的化疗治疗的KRAS突变体结直肠癌幼年患者在幼年患者中的相关性
8. Not just gRASping at flaws: Finding vulnerabilities to develop novel therapies for treating KRAS mutant cancers [O] . Ebi, Hiromichi, Faber, Anthony C., Engelman, Jeffrey A., 2014

机译：不仅仅是缺陷：发现脆弱性，开发治疗KRas突变癌症的新疗法
9. In Vivo shRNA-Drug Screen to Identify Novel Targeted Therapy Combinations for KRAS Mutant Cancers. [R] . Corcoran, R. B. 2014

机译：在体内shRNa-药物筛选中鉴定用于KRas突变癌症的新型靶向治疗组合。

Not just gRASping at flaws: Finding vulnerabilities to develop novel therapies for treating KRAS mutant cancers

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