4-Substituted Benzenesulfonamides Incorporating Bi/Tricyclic Moieties Act as Potent and Isoform-Selective Carbonic Anhydrase II/IX Inhibitors

Salerno, Silvia; Barresi, Elisabetta; Amendola, Giorgio; Berrino, Emanuela; Milite, Ciro; Marini, Anna María; Settimo, Federico Da; Novellino, Ettore; Cosconati, Sandro; Taliani, Sabrina

doi:10.1021/acs.jmedchem.8b00670

Cited by 19 publications

(17 citation statements)

References 25 publications

(51 reference statements)

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“…To clarify the reasons for the activities displayed by the newly designed compounds, molecular docking studies were attained. Docking calculations were performed using a protocol already successfully applied in our previous work on CA inhibitors 39 . Namely, AutoDock4.2 (AD4) 30 , 37 was employed together with the AutoDock4(Zn) forcefield 31 , which was specifically designed to accurately predict the binding interactions of ligands docking to zinc metalloproteins.…”

Section: Resultsmentioning

confidence: 99%

Novel 2-substituted-benzimidazole-6-sulfonamides as carbonic anhydrase inhibitors: synthesis, biological evaluation against isoforms I, II, IX and XII and molecular docking studies

Milite

Amendola

Nocentini

et al. 2019

Journal of Enzyme Inhibition and Medicinal Chemistry

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Inhibition of Carbonic Anhydrases (CAs) has been clinically exploited for many decades for a variety of therapeutic applications. Within a research project aimed at developing novel classes of CA inhibitors (CAIs) with a proper selectivity for certain isoforms, a series of derivatives featuring the 2-substituted-benzimidazole-6-sulfonamide scaffold, conceived as frozen analogs of Schiff bases and secondary amines previously reported in the literature as CAIs, were investigated. Enzyme inhibition assays on physiologically relevant human CA I, II, IX and XII isoforms revealed a number of potent CAIs, showing promising selectivity profiles towards the transmembrane tumor-associated CA IX and XII enzymes. Computational studies were attained to clarify the structural determinants behind the activities and selectivity profiles of the novel inhibitors.

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Section: Resultsmentioning

confidence: 99%

Novel 2-substituted-benzimidazole-6-sulfonamides as carbonic anhydrase inhibitors: synthesis, biological evaluation against isoforms I, II, IX and XII and molecular docking studies

Milite

Amendola

Nocentini

et al. 2019

Journal of Enzyme Inhibition and Medicinal Chemistry

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“…Due to the established role of CA IX/CA XII in cancer, many classes of potent and selective CA IX/CA XII inhibitors have been developed which have shown promising activity in in vitro as well as in vivo models. Many researchers have put their effort to develop potent CA IX/CA XII inhibitors, which selectively inhibit CA IX/CA XII or both over the cytosolic CA isoforms 269–316 …”

Section: Drug Design and Development Strategies For Selective Caismentioning

confidence: 99%

“…It was >1370‐, 577‐, and 990‐fold selective for hCA IX over hCA I, hCA II, and hCA IV. The molecular docking study indicated that pyrimidine ring nitrogen of compound 304 actively participated to establish H‐bond interaction with Q71 and Q92 side chains, which may be provided favorable binding with hCA IX led to achieving high affinity for hCA IX 311 . Bozdag et al developed 2‐aminophenol‐4‐sulfonamide and its urea analogues by modifying lead molecule SLC‐0111as potent hCA IX/hCA XII inhibitors.…”

Section: Drug Design and Development Strategies For Selective Caismentioning

confidence: 99%

“…The molecular docking study indicated that pyrimidine ring nitrogen of compound 304 actively participated to establish H-bond interaction with Q71 and Q92 side chains, which may be provided favorable binding with hCA IX led to achieving high affinity for hCA IX. 311 (Figure 21) was the most effective and selective derivative which displayed a K i value of 17.7 and 7.4 nM for hCA IX and hCA XII, respectively, a K i value of >10 000 nM was shown by this derivative for hCA I as well as hCA II. In psoralen-benzenesulfonamide series compound 308 (Figure 21) Figure 21) have demonstrated the most effective inhibition toward hCA IX (K i value of 8.2, 9.6, 8.5 nM, respectively) and hCA XII (K i value of 5.6, 5.8, and 7.1 nM, respectively).…”

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confidence: 97%

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Progress in the development of human carbonic anhydrase inhibitors and their pharmacological applications: Where are we today?

Mishra

Tiwari

Supuran

2020

Medicinal Research Reviews

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175

166

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Carbonic anhydrases (CAs, EC 4.2.1.1) are widely distributed metalloenzymes in both prokaryotes and eukaryotes. They efficiently catalyze the reversible hydration of carbon dioxide to bicarbonate and H + ions and play a crucial role in regulating many physiological processes. CAs are wellstudied drug target for various disorders such as glaucoma, epilepsy, sleep apnea, and high altitude sickness. In the past decades, a large category of diverse families of CA inhibitors (CAIs) have been developed and many of them showed effective inhibition toward specific isoforms, and effectiveness in pathological conditions in preclinical and clinical settings. The discovery of isoform-selective CAIs in the last decade led to diminished side effects associated with off-target isoforms inhibition. The many new classes of such compounds will be discussed in the review, together with strategies for their development. Pharmacological advances of the newly emerged CAIs in diseases not usually associated with CA inhibition (neuropathic pain, arthritis, cerebral ischemia, and cancer) will also be discussed.

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“…Each inhibitor was tested in triplicate, in serial dilutions starting from 0.01 to 0.1 mM. An incubation time of 15 min between inhibitor and enzyme has been used, as reported earlier, in order to be sure that the enzyme-inhibitor complex has been formed [2,25,27,[39][40][41][42][43][44][45][46][47][48][49][50]. The inhibition constants were obtained by using the Cheng-Prusoff equation [39,[51][52][53] and are the mean from three determinations.…”

Section: Ca Inhibitionmentioning

confidence: 99%

Benzylaminoethyureido-Tailed Benzenesulfonamides: Design, Synthesis, Kinetic and X-ray Investigations on Human Carbonic Anhydrases

Ali

Bozdağ

Farooq

et al. 2020

IJMS

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A drug design strategy of carbonic anhydrase inhibitors (CAIs) belonging to sulfonamides incorporating ureidoethylaminobenzyl tails is presented. A variety of substitution patterns on the ring and the tails, located on paraor metapositions with respect to the sulfonamide warheads were incorporated in the new compounds. Inhibition of human carbonic anhydrases (hCA) isoforms I, II, IX and XII, involving various pathologies, was assessed with the new compounds. Selective inhibitory profile towards hCA II was observed, the most active compounds being low nM inhibitors (K I s of 2.8-9.2 nM, respectively). Extensive X-ray crystallographic analysis of several sulfonamides in an adduct with hCA I allowed an in-depth understanding of their binding mode and to lay a detailed structure-activity relationship.

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4-Substituted Benzenesulfonamides Incorporating Bi/Tricyclic Moieties Act as Potent and Isoform-Selective Carbonic Anhydrase II/IX Inhibitors

Cited by 19 publications

References 25 publications

Novel 2-substituted-benzimidazole-6-sulfonamides as carbonic anhydrase inhibitors: synthesis, biological evaluation against isoforms I, II, IX and XII and molecular docking studies

Novel 2-substituted-benzimidazole-6-sulfonamides as carbonic anhydrase inhibitors: synthesis, biological evaluation against isoforms I, II, IX and XII and molecular docking studies

Progress in the development of human carbonic anhydrase inhibitors and their pharmacological applications: Where are we today?

Benzylaminoethyureido-Tailed Benzenesulfonamides: Design, Synthesis, Kinetic and X-ray Investigations on Human Carbonic Anhydrases

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