A combination therapy for KRAS -mutant lung cancer by targeting synthetic lethal partners of mutant KRAS

Xiufeng Pang; Mingyao Liu

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A combination therapy for KRAS -mutant lung cancer by targeting synthetic lethal partners of mutant KRAS

机译：通过靶向突变KRAS的致死性伴侣，对KRAS突变型肺癌进行联合治疗

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The KRAS gene is frequently mutated in multiple cancer types, but it fell off the drug discovery radar for many years because of its inherent “undruggable” structure and undefined biological properties. As reported in the paper entitled “Suppression of KRas-mutant cancer through the combined inhibition of KRAS with PLK1 and ROCK” in Nature Communications, we performed a synthetic lethal screening with a combinatorial strategy on a panel of clinical drugs; we found that combined inhibition of polo-like kinase 1 and RhoA/Rho kinase markedly suppressed tumor growth in mice. An increase in the expression of the tumor suppressor P21WAF1/CIP1 contributed to the synergistic mechanism of the combination therapy. These findings open a novel avenue for the treatment of KRAS-mutant lung cancer.

机译：KRAS基因经常在多种癌症类型中发生突变，但是由于其固有的“不可负担”的结构和不确定的生物学特性，它在药物研发雷达中失传了很多年。如《自然通讯》上题为“通过联合抑制KRAS与PLK1和ROCK抑制KRas突变型癌症”的论文所述，我们对一组临床药物进行了综合策略的合成致死筛选。我们发现联合抑制polo样激酶1和RhoA / Rho激酶可明显抑制小鼠的肿瘤生长。肿瘤抑制因子P21WAF1 / CIP1表达的增加有助于联合治疗的协同机制。这些发现为治疗KRAS突变型肺癌开辟了一条新途径。

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《Cancer Communications》 |2016年第1期|共页
作者
Xiufeng Pang; Mingyao Liu;
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中图分类肿瘤学;
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Synthetic lethalityKRASPolo-like kinase 1RhoA/Rho kinaseCombination therapy;

机译：合成致死性KRASPolo样激酶1RhoA / Rho激酶联合治疗;

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专利

1. A combination therapy for KRAS-mutant lung cancer by targeting synthetic lethal partners of mutant KRAS [J] . Xiufeng Pang, Mingyao Liu Chinese journal of cancer . 2016,第1期

机译：通过靶向突变KRAS的致死性伴侣，对KRAS突变型肺癌进行联合治疗
2. Cationic lipid-assisted polymeric nanoparticle mediated GATA2 siRNA delivery for synthetic lethal therapy of KRAS mutant non-small-cell lung carcinoma [J] . ShenS., MaoC.-Q., YangX.-Z., Molecular pharmaceutics . 2014,第8期

机译：阳离子脂质辅助聚合物纳米粒子介导的GATA2 siRNA递送，用于KRAS突变型非小细胞肺癌的合成致死性治疗
3. Synthetic lethal therapy for KRAS mutant non-small-cell lung carcinoma with nanoparticle-mediated CDK4 siRNA delivery [J] . MaoC.-Q., XiongM.-H., LiuY., Molecular therapy: the journal of the American Society of Gene Therapy . 2014,第5期

机译：纳米粒子介导的CDK4 siRNA递送对KRAS突变型非小细胞肺癌的合成致死治疗
4. 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
5. Targeting mutant KRAS in pancreatic cancer. [D] . Hayes, Tikvah Katheryn. 2016

机译：针对胰腺癌中的突变KRAS。
6. A combination therapy for KRAS-mutant lung cancer by targeting synthetic lethal partners of mutant KRAS [O] . Xiufeng Pang, Mingyao Liu 2016

机译：通过靶向突变KRAS的致死性伴侣对KRAS突变型肺癌进行联合治疗
7. A combination therapy for -mutant lung cancer by targeting synthetic lethal partners of mutant [O] . 2016

机译：以突变体的合成致死伴侣为靶点的突变肺癌联合疗法
8. Genomewide Screen for Synthetic Lethal Interactions with Mutant KRAS in Lung Cancer. [R] . Yin-Yuan, M. 2017

机译：全基因筛选与肺癌突变KRas合成致死性相互作用。

A combination therapy for KRAS -mutant lung cancer by targeting synthetic lethal partners of mutant KRAS

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