Katalog Plus
Bibliothek der Frankfurt UAS
Bald neuer Katalog: sichern Sie sich schon vorab Ihre persönlichen Merklisten im Nutzerkonto: Anleitung.
Dieses Ergebnis aus BASE kann Gästen nicht angezeigt werden.  Login für vollen Zugriff.

Selective-inhibition of trypanosomal glyceraldehyde-3-phosphate dehydrogenase by protein structure-based design - toward new drugs for the treatment of sleeping sickness

Title: Selective-inhibition of trypanosomal glyceraldehyde-3-phosphate dehydrogenase by protein structure-based design - toward new drugs for the treatment of sleeping sickness
Authors: Verlinde, C.L.; Callens, M.; Van Calenbergh, Serge; Van Aerschot, Arthur; Herdewijn, Piet; Hannaert, V.; Michels, Pam; Opperdoes, F.R.; Hol, W.G.
Source: ISSN:0022-2623 ; ISSN:1520-4804 ; Journal of Medicinal Chemistry, vol. 37 (21), (3605-3613.
Publisher Information: Amer chemical soc
Publication Year: 1994
Subject Terms: glycolytic-enzymes; brucei-brucei; purine; metabolism; resolution; phosphate; Adenosine; Animals; Binding Sites; Deoxyadenosines; Drug Design; Glyceraldehyde-3-Phosphate Dehydrogenases; Humans; Hydrogen Bonding; Leishmania mexicana; Molecular Structure; NAD; Protein Conformation; Structure-Activity Relationship; Trypanosoma brucei brucei; Trypanosomiasis; African; Science & Technology; Life Sciences & Biomedicine; Chemistry; Medicinal; Pharmacology & Pharmacy; 0304 Medicinal and Biomolecular Chemistry; 0305 Organic Chemistry; 1115 Pharmacology and Pharmaceutical Sciences
Description: Within the framework of a project aimed at rational design of drugs against diseases caused by trypanosomes and related hemoflagellate parasites, selective inhibitors of trypanosomal glycolysis were designed, synthesized, and tested. The design was based upon the crystallographically determined structures of the NAD:glyceraldehyde-3-phosphate dehydrogenase complexes of humans and trypanosoma brucei, the causative agent of sleeping sickness. After one design cycle, using the adenosine part of the NAD cofactor as a lead, the following encouraging results were obtained: (1) a 2-methyl substitution, targeted at a small pocket near Val 36, improves inhibition of the parasite enzyme 12.5-fold; (2) an 8-(thien-2-yl) substitution, aimed at Leu 112 of the parasite enzyme, where the equivalent residue in the mammalian enzyme is Val 100, results in a 167-fold better inhibition of the trypanosomal enzyme, while the inhibition of the human enzyme is improved only 13-fold; (3) exploitation of a ''selectivity cleft'' created by a unique backbone conformation in the trypanosomal enzyme near the adenosine ribose yields a considerable improvement in selectivity: 2'-deoxy-2'-(3-methoxybenzamido)adenosine inhibits the human enzyme only marginally but enhances inhibition of the parasite enzyme 45-fold when compared with adenosine. The designed inhibitors are not only better inhibitors of T. brucei GAPDH but also of the enzyme from Leishmania mexicana. ; status: Published
Document Type: article in journal/newspaper
Language: English
Relation: https://lirias.kuleuven.be/handle/123456789/41445; https://doi.org/10.1021/jm00047a017; https://pubmed.ncbi.nlm.nih.gov/7932587
DOI: 10.1021/jm00047a017
Availability: https://lirias.kuleuven.be/handle/123456789/41445; https://doi.org/10.1021/jm00047a017; https://pubmed.ncbi.nlm.nih.gov/7932587
Rights: info:eu-repo/semantics/restrictedAccess ; intranet
Accession Number: edsbas.8564771C
Database: BASE