Exploring Aliphatic Sulfonamides As Multiclass Inhibitors of the Carbonic Anhydrases from the Pathogen Bacterium Vibrio Cholerae

Overview

Journal Arch Pharm (Weinheim)

Specialty Pharmacy

Date 2024 Dec 17

PMID 39686870

Authors

Niccolo Paoletti

Simone Giovannuzzi

Alessandro Bonardi

Viviana De Luca

Clemente Capasso

Alessio Nocentini

Paola Gratteri

Claudiu T Supuran

Affiliations

Soon will be listed here.

Abstract

This study investigates aliphatic sulfonamide derivatives as inhibitors of the α-, β-, and γ-class carbonic anhydrase (CA) isoforms from Vibrio cholerae (VchCAs). A series of 26 compounds bearing a triazole linker and urea- or ether-based tails were described and evaluated for their inhibitory action using a stopped-flow CO hydrase technique. These inhibitors demonstrated a preferential efficacy against VchCAβ. Specifically, the ureido derivatives showed the highest inhibitory potency with inhibition constants (Ks) in the submicromolar range (0.67-0.93 µM). Selectivity indices were calculated to assess the selective inhibition of VchCAβ over human CA I and II, as well as other VchCA isozymes. Urea-linked compounds demonstrated a significant 25- to 125-fold selectivity for VchCAβ over hCAs and 14- to 26-fold over other VchCAs. Molecular modeling elucidated the interactions contributing to the efficacy and selectivity of aliphatic sulfonamides as VchCA inhibitors, aligning with and reinforcing the experimental results. The latter suggests that aliphatic sulfonamides could serve as valid targeted therapeutics to treat V. cholerae infections.

Citing Articles

Exploring aliphatic sulfonamides as multiclass inhibitors of the carbonic anhydrases from the pathogen bacterium Vibrio cholerae.

Paoletti N, Giovannuzzi S, Bonardi A, De Luca V, Capasso C, Nocentini A Arch Pharm (Weinheim). 2024; 358(1):e2400814.

PMID: 39686870 PMC: 11650360. DOI: 10.1002/ardp.202400814.

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