个人信息
教师姓名:刘接卿

学位:理学博士学位

学历:博士研究生

职称:教授

所在单位:JieQing Liu, Professor, Huaqiao University

学术荣誉:
泉州市引进高层次创业创新人才
泉州市高端海洋人才引进资助项目中的海洋课题研究项目
福建省引进高层次人才
曾获荣誉:
个人简介

  于2003年获吉林大学药学学士,2006年获吉林大学药物化学硕士,2009年获首都师范大学遗传学博士,2009-2011年于中国科学院昆明植物研究所完成博士后研究工作。2018-2019年以高级访问学者赴香港大学交流学习。20151月入职华侨大学医学院,现任华侨大学医学院副院长。福建省高层次人才,龙岩市首批创新人才,泉州市高层次(第三层次)人才,云南省中青年学术和技术带头人后备人才,华侨大学学生最喜爱的教师师德模范。泉州市中医药研究促进会会长,福建省中医药研究促进会第六届理事会常务理事,泉州市中医药学会中药分会副会长/常委,福建省微生物学会药用真菌专业委员会常委。

 

  长期从事中药现代化应用研究,药膳与大健康研究,天然药物研究与开发。先后主持国家自然科学基金面上项目、福建省自然科学基金面上项目、福建省高校青年自然基金重点项目、泉州市高端海洋人才资助项目、泉州市科技局项目、福建省高校产学合作项目、校企横向合作项目等。以第一作者或通讯作者在Communications Biology, BMC Cancer, Bioorganic & Medicinal Chemistry, Phytotherapy Research, Journal of Ethnopharmacology, Food & Function, Food Chemistry, Organic Biomolecular Chemistry, Steroids等国际杂志上发表SCI论文60余篇,申请中国发明专利十余项。指导学生获得校级及以上各类科创竞赛或创新项目20余项,包括全国大学生生命科学竞赛一等奖2个、二等奖1个、三等奖2个,第11届全国大学生电子商务创新、创意及创业挑战赛三等奖、第七届全国青年科普创新实验暨作品大赛(生物环境组)福建赛区一等奖和三等奖各1个,2023福建省基础医学研究生创新大赛三等奖2个,华侨大学第28挑战杯赛特等奖等。


论文成果
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Cui, C.; Dwyer, B. G.; Liu, C.; Abegg, D.; Cai, Z.-J.; Hoch, D. G.; Yin, X.; Qiu, N.; Liu, J.-Q.; Adibekian, A.; Dai, M., Total Synthesis and Target Identification of the Curcusone Diterpenes. Journal of the American Chemical Society 2021, 143 (11), 4379-4386.


发表刊物:Journal of the American Chemical Society

摘要:The curcusone natural products are complex diterpenes featuring a characteristic [6-7-5] tricyclic carbon skeleton similar to the daphnane and tigliane diterpenes. Among them, curcusones A-D demonstrated potent anticancer activity against a broad spectrum of human cancer cell lines. Prior to this study, no total synthesis of the curcusones was achieved and their anticancer mode of action remained unknown. Herein, we report our synthetic and chemoproteomics studies of the curcusone diterpenes which culminate in the first total synthesis of several curcusone natural products and identification of BRCA1-associated ATM activator 1 (BRAT1) as a cellular target. Our efficient synthesis is highly convergent, builds upon cheap and abundant starting materials, features a thermal [3,3]-sigmatropic rearrangement and a novel FeCl3-promoted cascade reaction to rapidly construct the critical cycloheptadienone core of the curcusones, and led us to complete the first total synthesis of curcusones A and B in only 9 steps, C and D in 10 steps, and dimericursone A in 12 steps. The chemical synthesis of dimericursone A from curcusones C and D provided direct evidence to support the proposed Diels-Alder dimerization and cheletropic elimination biosynthetic pathway. Using an alkyne-tagged probe molecule, BRAT1, an important but previously "undruggable" oncoprotein, was identified as a key cellular target via chemoproteomics. We further demonstrate for the first time that BRAT1 can be inhibited by curcusone D, resulting in impaired DNA damage response, reduced cancer cell migration, potentiated activity of the DNA damaging drug etoposide, and other phenotypes similar to BRAT1 knockdown.

论文类型:基础研究

是否译文:

发表时间:2021-03-24


上一条: Huang, J.-D.#; Zhang, C.#; Xu, W.-J.; Lian, C.-L.; Liu, X.-M.; Wang, C.-F.; Liu, J.-Q.*, New lathyrane diterpenoids with anti-inflammatory activity isolated from the roots of Jatropha curcas L. J Ethnopharmacol 2021, 113673.

下一条: Huang, J.-D.; Wang, C.-F.; Lian, C.-L.; Huang, M.-Y.; Zhang, C.; Liu, J.-Q.*, Isolation and identification of five new diterpenoids from Jatropha curcas. Phytochem. Lett. 2020, 40, 37-41.


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