Design,synthesis and biological evaluation of novel human monoamine oxidase B inhibitors based on a fragment in an X-ray crystal structure |
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| Authors: | Kai Cheng Shiyu Li Xiao Lv Yongbin Tian Haiyan Kong Xufeng Huang Yajun Duan Jihong Han Zhouling Xie Chenzhong Liao |
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| Affiliation: | School of Food and Biological Engineering, Hefei University of Technology, Hefei, Anhui 230009, PR China |
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| Abstract: | Herein we report our efforts of developing reversible selective hMAO-B inhibitors based on isatin, a fragment in an X-ray crystal structure. Five different scaffolds were designed and many compounds were synthesized. Among them, compound A3 demonstrated very high potency and isoform selectivity against hMAO-B, 11 and 13 times more potent (IC50?=?3?nM) and 23.64 and 6.8 times more selective than the marked drugs, selegiline and safinamide. However, the endeavors to modify the polar 3-one group of isatin, that is in a hydrophobic environment in the binding site of hMAO-B, to small nonpolar hydrophobic groups did not bring about improved hMAO-B inhibitors, which may challenge our understanding of molecular interactions and molecular recognition in biological systems. |
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| Keywords: | hMAO-B Isatin Isoform selectivity Fragment-based drug design Structure activity relationship |
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