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中国临床药理学与治疗学 ›› 2021, Vol. 26 ›› Issue (9): 1005-1013.doi: 10.12092/j.issn.1009-2501.2021.09.005

• 基础研究 • 上一篇    下一篇

苍术苷靶向癌蛋白BORIS抑制癌细胞增殖的作用区域

刘宸,方梦蝶,徐昊,李超,任娟,左博文,张衍梅   

  1. 杭州医学院生物工程学院,杭州 310012,浙江
  • 收稿日期:2021-02-22 修回日期:2021-04-14 出版日期:2021-09-26 发布日期:2021-09-30
  • 通讯作者: 张衍梅,女,博士,副教授,研究方向:分子医学和基因组。 E-mail: yanmeizhang81@yahoo.com
  • 作者简介:刘宸,女,硕士研究生,研究方向:转化分子医学。 E-mail: sirius_lc@163.com
  • 基金资助:
    浙江省医药卫生科技计划(2019RC030);浙江省医学科学院青年基金(2019Y003)

Atractyloside targets the area of action of oncoprotein BORIS to inhibit cancer cell proliferation

LIU Chen, FANG Mengdie, XU Hao, LI Chao, REN Juan, ZUO Bowen, ZHANG Yanmei   

  1. School of Bioengineering, Hangzhou Medical College, Hangzhou 310012, Zhejiang, China
  • Received:2021-02-22 Revised:2021-04-14 Online:2021-09-26 Published:2021-09-30

摘要: 目的:探讨苍术苷靶向癌蛋白BORIS抑制癌细胞增殖的结合作用区域。方法:采用DNAMAN对比序列寻找BORIS保守区域,选择保守区域利用SWISS-MODEL结构预测,ChemBio3D Ultra进行结构最小量化,Autodocking进行分子对接。过表达相应区段的BORIS进行验证。结果:BORIS-N端在生物进化过程中有相对保守的区域并且有高级结构存在,人源BORIS的N端是我们推测的主要作用区域,重点是第70~97位氨基酸,分子对接后和苍术苷结合最好的位点为第96位的谷氨酰胺,该区域会抑制细胞增殖。 结论:BORIS-N端和苍术苷存在作用区域,且该区段对细胞增殖有重要作用,对今后筛选靶向药物有重要意义。

关键词: 苍术苷, BORIS, 蛋白结构, 分子相互作用, 分子靶向治疗

Abstract: AIM: To analyze the binding area of atractyloside targeting oncoprotein BORIS to inhibit cancer cell proliferation.  METHODS: DNAMAN comparison sequences were used to find the conserved regions of BORIS. Conservative regions were elected and the structure were predicted using SWISS-MODEL. ChemBio3D Ultra was used for minimum structure quantification, and Autodocking for molecular docking. The BORIS of the corresponding segment were overexpressed for verification. RESULTS: BORIS-N end had relatively conserved regions and high-level structures in the biological evolution process. The N-terminal of human-derived BORIS was the main action area we speculated, especially the 70th to 97th amino acids, and the site that binded preferentially to atractyloside after molecular docking was the 96th position (Glutamine), and this area would inhibit cell proliferation. CONCLUSION: BORIS-N terminal and atractyloside have an action area, and this segment has an important effect on cell proliferation, which is of great significance for the future screening of targeted drugs.

Key words: atractyloside, BORIS,  protein structure, molecular interaction, molecular targeted therapy

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