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熊果酸通过抑制肺癌细胞中牛痘相关激酶1介导的损伤修复发挥抗癌活性。

Ursolic acid exerts anti-cancer activity by suppressing vaccinia-related kinase 1-mediated damage repair in lung cancer cells.

作者信息

Kim Seong-Hoon, Ryu Hye Guk, Lee Juhyun, Shin Joon, Harikishore Amaravadhi, Jung Hoe-Yune, Kim Ye Seul, Lyu Ha-Na, Oh Eunji, Baek Nam-In, Choi Kwan-Yong, Yoon Ho Sup, Kim Kyong-Tai

机构信息

Department of Life Sciences, Pohang University of Science and Technology, Pohang 790-784, Republic of Korea.

Division of Integrative Biosciences and Biotechnology, Pohang University of Science and Technology, Pohang 790-784, Republic of Korea.

出版信息

Sci Rep. 2015 Sep 28;5:14570. doi: 10.1038/srep14570.

Abstract

Many mitotic kinases have been targeted for the development of anti-cancer drugs, and inhibitors of these kinases have been expected to perform well for cancer therapy. Efforts focused on selecting good targets and finding specific drugs to target are especially needed, largely due to the increased frequency of anti-cancer drugs used in the treatment of lung cancer. Vaccinia-related kinase 1 (VRK1) is a master regulator in lung adenocarcinoma and is considered a key molecule in the adaptive pathway, which mainly controls cell survival. We found that ursolic acid (UA) inhibits the catalytic activity of VRK1 via direct binding to the catalytic domain of VRK1. UA weakens surveillance mechanisms by blocking 53BP1 foci formation induced by VRK1 in lung cancer cells, and possesses synergistic anti-cancer effects with DNA damaging drugs. Taken together, UA can be a good anti-cancer agent for targeted therapy or combination therapy with DNA damaging drugs for lung cancer patients.

摘要

许多有丝分裂激酶已成为抗癌药物开发的靶点,人们期望这些激酶的抑制剂在癌症治疗中表现良好。由于用于治疗肺癌的抗癌药物使用频率增加,因此尤其需要致力于选择良好靶点并找到针对这些靶点的特定药物。痘苗相关激酶1(VRK1)是肺腺癌中的主要调节因子,被认为是适应性通路中的关键分子,主要控制细胞存活。我们发现熊果酸(UA)通过直接结合VRK1的催化结构域来抑制VRK1的催化活性。UA通过阻断VRK1在肺癌细胞中诱导的53BP1病灶形成来削弱监测机制,并与DNA损伤药物具有协同抗癌作用。综上所述,UA可以成为肺癌患者靶向治疗或与DNA损伤药物联合治疗的良好抗癌剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cc21/4585938/0cfd0e4a8577/srep14570-f1.jpg

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