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. 2016 Jun 3;474(3):528-533.
doi: 10.1016/j.bbrc.2016.04.124. Epub 2016 Apr 24.

Discovery of novel selenium derivatives as Pin1 inhibitors by high-throughput screening

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Discovery of novel selenium derivatives as Pin1 inhibitors by high-throughput screening

Amit Subedi et al. Biochem Biophys Res Commun. .

Abstract

Peptidyl prolyl cis/trans isomerization by Pin1 regulates various oncogenic signals during cancer progression, and its inhibition through multiple approaches has established Pin1 as a therapeutic target. However, lack of simplified screening systems has limited the discovery of potent Pin1 inhibitors. We utilized phosphorylation-dependent binding of Pin1 to its specific substrate to develop a screening system for Pin1 inhibitors. Using this system, we screened a chemical library, and identified a novel selenium derivative as Pin1 inhibitor. Based on structure-activity guided chemical synthesis, we developed more potent Pin1 inhibitors that inhibited cancer cell proliferation.

Keywords: Cancer; High-throughput screening; PPIase; Pin1; Selenium.

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