2006
DOI: 10.1002/cmdc.200600029
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Enzyme Isoselective Inhibitors: A Tool for Binding‐Trend Analysis

Abstract: A transition-state analogue inhibitor that covalently reversibly binds to an enzyme formally consists of two parts: the chemical site, CS and the recognition site, RS. We have experimentally and theoretically demonstrated that the trend of binding affinity in a series of isoselective inhibitors (with identical RS and different CS fragments) depends mainly on their CS fragments. Isoselective inhibitors have the same affinity trend toward different enzymes of the same family with a common catalytic mechanism. Th… Show more

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Cited by 8 publications
(14 citation statements)
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“…The method uses series of isoselective RCA inhibitors, the relative binding affinities of which depend on the variation of their CS fragments only. The binding affinity trend is predicted on small molecular clusters representing the enzyme-inhibitor reaction core in the active site 12,13. The clusters are composed from the functional groups simulating the enzyme nucleophile (Nuc) and the CS fragment of the inhibitor (Inh) (Fig.…”
Section: Methodsmentioning
confidence: 99%
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“…The method uses series of isoselective RCA inhibitors, the relative binding affinities of which depend on the variation of their CS fragments only. The binding affinity trend is predicted on small molecular clusters representing the enzyme-inhibitor reaction core in the active site 12,13. The clusters are composed from the functional groups simulating the enzyme nucleophile (Nuc) and the CS fragment of the inhibitor (Inh) (Fig.…”
Section: Methodsmentioning
confidence: 99%
“…RCA inhibitor can be considered as formally comprised of two parts: the chemical site, CS , responsible for the covalent binding, and the recognition site, RS , dominating in the selectivity of the inhibitor towards the target enzyme 11,12. We have previously introduced a new method that allows a separate design of CS fragments of RCA inhibitors 12.…”
Section: Introductionmentioning
confidence: 99%
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“…[50] Two sets of the general formula RS-X (RS = carbobenzyloxy (Cbz)-Phe; X = OH, H, CH 3 , COCH 3 , CF 3 and RS = Cbz-Gly-Leu-Phe; X = OH, H, CH 3 , COCH 3 ) were examined with three serine proteases: chymotrypsin, subtilisin, and carboxypeptidase Y. Therefore, noncovalent enzymeÀRS interactions are different for different enzymes of the same family.…”
Section: Serine Protease Inhibition By Rca Inhibitorsmentioning
confidence: 99%