论文
论文题目: Skp1 in lung cancer: Clinical significance and therapeutic efficacy of its small molecule inhibitors
论文题目英文:
作者: 刘永强①,王晓璐①,程昕①,#Yong-Zhi Lu①,王桂珍①,李新春,#Jian Zhang,#Zhe-Sheng Wen,#Zhi-Liang Huang,#Qin-Lei Gao,#Li-Na Yang,#程永现*,#Sheng-Ce Tao,#刘劲松*,周光飚*
论文出处:
年: 2015
卷: 6
期: 33
页: 34953-34967
联系作者: #程永现,#刘劲松,周光飚
发表期刊: Oncotarget
ISSN:
第一作者所在部门:
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论文连接 http://www.impactjournals.com/oncotarget/index.php? journal=oncotarget&page=article&op=view&path[]=5547&path[]=15041
影响因子:
摘要: Skp1 is an essential adaptor protein of the Skp1-Cul1-F-box protein complex and is able to stabilize the conformation of some ubiquitin E3 ligases. However, the role Skp1 plays during tumorigenesis remains unclear and Skp1-targeting agent is lacking. Here we showed that Skp1 was overexpressed in 36/64 (56.3%) of non-small cell lung cancers, and elevated Skp1 was associated with poor prognosis. By structure-based high-throughput virtual screening, we found some Skp1-targeting molecules including a natural compound 6-O-angeloylplenolin (6-OAP). 6-OAP bound Skp1 at sites critical to Skp1-Skp2 interaction, leading to dissociation and proteolysis of oncogenic E3 ligases NIPA, Skp2, and β-TRCP, and accumulation of their substrates Cyclin B1, P27 and E-Cadherin. 6-OAP induced prometaphase arrest and exerted potent anti-lung cancer activity in two murine models and showed low adverse effect. These results indicate that Skp1 is critical to lung cancer pathogenesis, and Skp1 inhibitor inactivates crucial oncogenic E3 ligases and exhibits significant therapeutic potentials.
英文摘要:
外单位作者单位: