Heterocyclic periphery in the design of carbonic anhydrase inhibitors: 1,2,4-Oxadiazol-5-yl benzenesulfonamides as potent and selective inhibitors of cytosolic hCA II and membrane-bound hCA IX isoforms

A series of novel aromatic primary sulfonamides decorated with diversely substituted 1,2,4-oxadiazole periphery groups has been prepared using a parallel chemistry approach. The compounds displayed a potent inhibition of cytosolic hCA II and membrane-bound hCA IX isoforms. Due to a different cellular localization of the two target enzymes, the compounds can be viewed as selective inhibition tools for either isoform, depending on the cellular permeability profile. The SAR findings revealed in this study has been well rationalized by docking simulation of the key compounds against the crystal structures of the relevant hCA isoforms. © 2017

Авторы
Krasavin M.1 , Shetnev A. 2, 3 , Sharonova T.3 , Baykov S.3 , Tuccinardi T.4 , Kalinin S.1 , Angeli A.5 , Supuran C.T.5
Журнал
Издательство
Academic Press Inc.
Язык
Английский
Страницы
88-97
Статус
Опубликовано
Том
76
Год
2018
Организации
  • 1 Saint Petersburg State University, Saint Petersburg, 199034, Russian Federation
  • 2 Department of Organic Chemistry, Faculty of Science, RUDN University117198, Russian Federation
  • 3 The Ushinsky Yaroslavl State Pedagogical University, Yaroslavl, 150000, Russian Federation
  • 4 Department of Pharmacy, University of Pisa, Pisa, 56126, Italy
  • 5 Neurofarba Department, Universita degli Studi di Firenze, Florence, Italy
Ключевые слова
1,2,4-Oxadiazole; Acylation; Carbonic anhydrase; Cyclodehydration; Isoform-selective inhibitors; Nanomolar inhibition; Periphery groups; Primary sulfonamides; Superbase
Дата создания
19.10.2018
Дата изменения
19.10.2018
Постоянная ссылка
https://repository.rudn.ru/ru/records/article/record/6881/
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