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

Seong‐Hoon Kim(Pohang University of Science and Technology), Hye Guk Ryu(Pohang University of Science and Technology), Juhyun Lee(Pohang University of Science and Technology), Joon Shin(Nanyang Technological University), Amaravadhi Harikishore(Nanyang Technological University), Hoe‐Yune Jung(Pohang University of Science and Technology), Ye Seul Kim(Pohang University of Science and Technology), Ha-Na Lyu(Pohang University of Science and Technology), Eun-Ji Oh(Kyung Hee University), Nam‐In Baek(Kyung Hee University), Kwan-Yong Choi(Pohang University of Science and Technology), Ho Sup Yoon(University of Suwon), Kyong‐Tai Kim(Pohang University of Science and Technology)
Scientific Reports
September 28, 2015
Cited by 49Open Access
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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.


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