| Literature DB >> 24321833 |
Makoto Hasegawa1, Yukari Yasuda2, Makoto Tanaka2, Kenya Nakata3, Eri Umeda3, Yanwen Wang3, Chihiro Watanabe3, Shoko Uetake3, Tatsuki Kunoh2, Masafumi Shionyu2, Ryuzo Sasaki2, Isamu Shiina4, Tamio Mizukami2.
Abstract
In a survey of nonpeptide noncovalent inhibitors of the human 20S proteasome, we found that a novel tamoxifen derivative, RID-F (compound 6), inhibits all three protease activities of the proteasome at submicromolar levels. Structure-activity relationship studies revealed that a RID-F analog (RID-F-S*4, compound 25) is the smallest derivative compound capable of inhibiting proteasome activity, with a potency similar to that of RID-F. Kinetic analyses of the inhibition mode and competition experiments involving biotin-belactosin A (a proteasome inhibitor) binding indicated that the RID-F derivatives interact with the protease subunits in a different manner. Culturing of human cells with these compounds resulted in accumulation of ubiquitinated proteins and induction of apoptosis. Thus, the RID-F derivatives may be useful lead chemicals for the generation of a new class of proteasome inhibitors.Entities:
Keywords: Docking studies; Proteasome inhibitors; Structure–activity relationship (SAR); Tamoxifen derivatives
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Year: 2013 PMID: 24321833 DOI: 10.1016/j.ejmech.2013.11.009
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514