Use of an Additional Hydrophobic Binding Site, the Z Site, in the Rational Drug Design of a New Class of Stronger Trypanothione Reductase Inhibitor, Quaternary Alkylammonium Phenothiazines

Khan, Madeeha; Austin, S. E.; Chan, Cecil; Yin, Hong; Marks, David L.; Vaghjiani, S. N.; Kendrick, Howard; Yardley, Vanessa; Croft, S. L.; Douglas, Kenneth T.

doi:10.1021/jm000156+

Cited by 108 publications

(121 citation statements)

References 41 publications

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“…Most of them include nitrogen heterocycle rings such as quinolines 9 , quinazolines 10 , acridines 11 , pyrimidines 12 , pyrazols 13 , pyridines 8 , benzothiazoles 14 , imidazoles 15 , thiadiazoles 16 and include functional structures such as alkyl phospholipids 17 , ether phospholipids 18 , chalcones 19 , amidines 20 , oximes 21 , amidoxime 22 , hydrazones 23 and hydrazides 24,25 . On the other hand, a number of quaternized amine derivatives such as thiadiazolium-phenylamine 26,27 , arylisoquinolinium 28 , imidazo-pyridinium 29 , alkylammonium-phenothiazines 30 , indolo-quinolinium 31 and naphthalimide-amonnium 32 were previously reported to exert antiprotozoal properties. Antiprotozoal activity of quaternary ammonium compounds against Acanthamoeba spp.…”

Section: Introductionmentioning

confidence: 99%

Synthesis and antileishmanial activity of novel pyridinium-hydrazone derivatives

Alptüzün

Cakiroglu

Limoncu

et al. 2012

Journal of Enzyme Inhibition and Medicinal Chemistry

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Section: Introductionmentioning

confidence: 99%

Synthesis and antileishmanial activity of novel pyridinium-hydrazone derivatives

Alptüzün

Cakiroglu

Limoncu

et al. 2012

Journal of Enzyme Inhibition and Medicinal Chemistry

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“…A number of groups have reported on the successful design of inhibitors directed against trypanosomal (2,4,(15)(16), leishmanial (6), malarial (19), and tritrichomonal (3, 27) targets active in the 10 nM to 50 M range. However, with the number of compounds that could be generated by combinatorial chemistry growing exponentially, it has become apparent that chemical diversity has surpassed the capacity of high-throughput screening.…”

mentioning

confidence: 99%

Virtual Screening of Combinatorial Libraries across a Gene Family: in Search of Inhibitors of Giardia lamblia Guanine Phosphoribosyltransferase

Aronov

Munagala

Kuntz

et al. 2001

Antimicrob Agents Chemother

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Parasitic protozoa lack the ability to synthesize purine nucleotides de novo, relying instead on purine salvage enzymes for their survival. Guanine phosphoribosyltransferase (GPRT) from the protozoan parasite Giardia lamblia is a potential target for rational antiparasitic drug design, based on the experimental evidence, which indicates the lack of interconversion between adenine and guanine nucleotide pools. The present study is a continuation of our efforts to use three-dimensional structures of parasitic phosphoribosyltransferases (PRTs) to design novel antiparasitic agents. Two micromolar phthalimide-based GPRT inhibitors were identified by screening the in-house phthalimide library. A combination of structure-based scaffold selection using virtual library screening across the PRT gene family and solid phase library synthesis led to identification of smaller (molecular weight, <300) ligands with moderate to low specificity for GPRT; the best inhibitors, GP3 and GP5, had K i values in the 23 to 25 M range. These results represent significant progress toward the goal of designing potent inhibitors of purine salvage in Giardia parasites. As a second step in this process, altering the phthalimide moiety to optimize interactions in the guanine-binding pocket of GPRT is expected to lead to compounds with promising activity against G. lamblia PRT.Computer-aided drug design in combination with combinatorial chemistry approaches, whereby focused or diverse combinatorial libraries can be designed using computational methods, is becoming increasingly important in the process of drug discovery for parasitic targets (7,11). A number of groups have reported on the successful design of inhibitors directed against trypanosomal (2,4,(15)(16), leishmanial (6), malarial (19), and tritrichomonal (3, 27) targets active in the 10 nM to 50 M range. However, with the number of compounds that could be generated by combinatorial chemistry growing exponentially, it has become apparent that chemical diversity has surpassed the capacity of high-throughput screening. In the case of antiparasitics research, which is concentrated in a limited number of mostly academic labs, the need for more rapid ligand screening tools has become apparent. Recently, in silico methods for database screening have come to the forefront of drug discovery (30). By accelerating the screening process, these methods are able to capitalize on the potential of virtual combinatorial libraries. While a number of recent reports have focused on structure-based pruning of the virtual combinatorial libraries built around a given preselected scaffold, there has been a growing trend toward combinatorial scaffold evaluation against a number of biological targets. Evaluation of binding preferences for combinatorial libraries across a range of targets could, in principle, provide information about scaffold generality or selectivity as related to the target selection (M. L. Lamb, K. W. Burdick, S. Toba, M. M. Young, A. G. Skillman, X. Zou, J. R. Arnold, and I. D. Kuntz, unpubl...

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“…Although potent inhibitors of TR could be developed by means of molecular modeling and quantitative docking techniques (22), it was found that several different modes of binding of such compounds to TR are energetically allowed. The authors conclude that with inhibitors not docked to a unique locus, it may be difficult to obtain good X-ray diffraction data for their binding to TR.…”

Section: Inhibitors Of Trypanothione Metabolismmentioning

confidence: 99%

Thiol Metabolism of the Trypanosomatids as Potential Drug Targets

Steenkamp

2002

IUBMB Life

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Use of an Additional Hydrophobic Binding Site, the Z Site, in the Rational Drug Design of a New Class of Stronger Trypanothione Reductase Inhibitor, Quaternary Alkylammonium Phenothiazines

Cited by 108 publications

References 41 publications

Synthesis and antileishmanial activity of novel pyridinium-hydrazone derivatives

Synthesis and antileishmanial activity of novel pyridinium-hydrazone derivatives

Virtual Screening of Combinatorial Libraries across a Gene Family: in Search of Inhibitors of Giardia lamblia Guanine Phosphoribosyltransferase

Thiol Metabolism of the Trypanosomatids as Potential Drug Targets

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