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FS36作为新型人源Hsp90抑制剂的发现
引用本文:李根,吕凯凯,李健,尹秀山,赵栋,张万忠. FS36作为新型人源Hsp90抑制剂的发现[J]. 生物化学与生物物理进展, 2018, 45(7): 736-744
作者姓名:李根  吕凯凯  李健  尹秀山  赵栋  张万忠
作者单位:沈阳化工大学制药与生物工程学院,沈阳 110142,中国科学院上海药物研究所,上海 201203,沈阳化工大学制药与生物工程学院,沈阳 110142;Department of Molecular & Cellular Biochemistry, College of Medicine, University of Kentucky, Lexington, KY 40536, USA,沈阳化工大学制药与生物工程学院,沈阳 110142;Karolinska Institutet (MTC), Science for Life Laboratory, Tomtebodavag, en 23A (Gamma5), 17165 Solna, Sweden,西安医学院基础与转化医学研究所,西安 710021,沈阳化工大学制药与生物工程学院,沈阳 110142
基金项目:国家自然科学基金(81402850)和陕西省教育厅专项科研计划项目(17JK0669)
摘    要:热休克蛋白90(Hsp90)通过对几百种蛋白质底物(客户蛋白质)进行合理的折叠、成熟其构象并且激活,在肿瘤细胞的生长和繁殖中发挥重要作用.因此,Hsp90成为非常有吸引力、有前途的抗肿瘤药物靶点,并且超过20种抑制剂已经进入临床实验阶段.我们在这里设计并合成了一个小分子抑制剂:FS36.收集了Hsp90N-FS36复合物晶体结构的X射线衍射实验数据.高分辨率X射线晶体结构表明,FS36在ATP结合位点上与Hsp90N相互作用,并且FS36可能替代核苷酸与Hsp90N结合.FS36和Hsp90N的复合物晶体结构和相互作用为后期设计和优化新型抗肿瘤药物奠定基础.

关 键 词:热休克蛋白90,抗肿瘤药物,抑制剂,X射线衍射,复合物晶体结构
收稿时间:2017-12-09
修稿时间:2018-04-16

Discovery of FS36 as a Novel Human Hsp90 Inhibitor
LI Gen,LV Kai-Kai,LI Jian,YIN Xiu-Shan,ZHAO Dong and ZHANG Wan-Zhong. Discovery of FS36 as a Novel Human Hsp90 Inhibitor[J]. Progress In Biochemistry and Biophysics, 2018, 45(7): 736-744
Authors:LI Gen  LV Kai-Kai  LI Jian  YIN Xiu-Shan  ZHAO Dong  ZHANG Wan-Zhong
Abstract:The heat shock protein 90 (Hsp90) plays an important role in growth and progression of tumor cells through the appropriate folding, conformational maturation and activation of several hundred protein substrates (client proteins). Thus, Hsp90 attracts a great many of interests as a promising target for antitumor drugs which results in more than 20 inhibitors advancing to clinical trials. Here, we designed and synthesized a small molecule inhibitor: FS36 and the X-ray diffraction data of the complex crystal of Hsp90N-FS36 is collected. High-resolution X-ray crystallography shows that FS36 interacts with Hsp90N at the ATP-binding pocket and this demonstrates that FS36 possibly substitutes nucleotides to bind to Hsp90N. The complex crystal structure and the interactions between FS36 and Hsp90N lay the foundation of the design and majorization of novel antitumor drugs.
Keywords:heat shock protein 90   antitumor drugs   inhibitor   X-ray diffraction   complex crystal structure
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