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A Small‐Molecule Protein–Protein Interaction Inhibitor of PARP1 That Targets Its BRCT Domain
Authors:Zhenkun Na  Bo Peng  Shukie Ng  Sijun Pan  Prof. Dr. Jun‐Seok Lee  Prof. Dr. Han‐Ming Shen  Prof. Dr. Shao Q. Yao
Affiliation:1. Department of Chemistry, National University of Singapore, 3 Science Drive 3, Singapore 117543 (Singapore) http://staff.science.nus.edu.sg/~syao;2. Molecular Recognition Research Center, Korea Institute of Science and Technology (KIST), 39‐1 Hawolgok‐dong, Seoul, 136‐791 (Republic of Korea);3. Department of Biological Chemistry, University of Science and Technology (UST), 113 Gawhank‐ro, Yuseong‐gu, Daejeon, 305‐333 (Republic of Korea);4. Department of Physiology, National University of Singapore, 16 Medical Drive, Singapore 11794 (Singapore)
Abstract:Poly(ADP‐ribose)polymerase‐1 (PARP1) is a BRCT‐containing enzyme (BRCT=BRCA1 C‐terminus) mainly involved in DNA repair and damage response and a validated target for cancer treatment. Small‐molecule inhibitors that target the PARP1 catalytic domain have been actively pursued as anticancer drugs, but are potentially problematic owing to a lack of selectivity. Compounds that are capable of disrupting protein–protein interactions of PARP1 provide an alternative by inhibiting its activities with improved selectivity profiles. Herein, by establishing a high‐throughput microplate‐based assay suitable for screening potential PPI inhibitors of the PARP1 BRCT domain, we have discovered that (±)‐gossypol, a natural product with a number of known biological activities, possesses novel PARP1 inhibitory activity both in vitro and in cancer cells and presumably acts through disruption of protein–protein interactions. As the first known cell‐permeable small‐molecule PPI inhibitor of PAPR1, we further established that (?)‐gossypol was likely the causative agent of PARP1 inhibition by promoting the formation of a 1:2 compound/PARP1 complex by reversible formation of a covalent imine linkage.
Keywords:cancer  inhibitors  microarrays  PARP1  protein–  protein interactions
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