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Identification by shape-based virtual screening and evaluation of new tyrosinase inhibitors.


ABSTRACT: Targeting tyrosinase is considered to be an effective way to control the production of melanin. Tyrosinase inhibitor is anticipated to provide new therapy to prevent skin pigmentation, melanoma and neurodegenerative diseases. Herein, we report our results in identifying new tyrosinase inhibitors. The shape-based virtual screening was performed to discover new tyrosinase inhibitors. Thirteen potential hits derived from virtual screening were tested by biological determinations. Compound 5186-0429 exhibited the most potent inhibitory activity. It dose-dependently inhibited the activity of tyrosinase, with the IC50 values 6.2 ± 2.0 µM and 10.3 ± 5.4 µM on tyrosine and L-Dopa formation, respectively. The kinetic study of 5186-0429 demonstrated that this compound acted as a competitive inhibitor. We believe the discoveries here could serve as a good starting point for further design of potent tyrosinase inhibitor.

SUBMITTER: Li Q 

PROVIDER: S-EPMC5788061 | biostudies-literature | 2018

REPOSITORIES: biostudies-literature

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Identification by shape-based virtual screening and evaluation of new tyrosinase inhibitors.

Li Qi Q   Yang Hongyu H   Mo Jun J   Chen Yao Y   Wu Yue Y   Kang Chen C   Sun Yuan Y   Sun Haopeng H  

PeerJ 20180126


Targeting tyrosinase is considered to be an effective way to control the production of melanin. Tyrosinase inhibitor is anticipated to provide new therapy to prevent skin pigmentation, melanoma and neurodegenerative diseases. Herein, we report our results in identifying new tyrosinase inhibitors. The shape-based virtual screening was performed to discover new tyrosinase inhibitors. Thirteen potential hits derived from virtual screening were tested by biological determinations. Compound 5186-0429  ...[more]

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