Unexpected Nanomolar Inhibition of Carbonic Anhydrase by COX-2-Selective Celecoxib:  New Pharmacological Opportunities Due to Related Binding Site Recognition

Weber, Alexander; Casini, Angela; Heine, A.; Kühn, Daniel; Supuran, Claudiu T.; Scozzafava, Andrea; Klebe, G.

doi:10.1021/jm030912m

Cited by 428 publications

(331 citation statements)

References 44 publications

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“…Similarly, valdecoxib, a sulphonamide-based coxib as well (Figure 1), was able to inhibit CAIX and CAXII with comparable potency, although its binding mode was entirely different from celecoxib (Di Fiore et al, 2006). In contrast, several non-sulphonamide COX inhibitors tested, including rofecoxib, a methylsulphone-type coxib (Figure 1), had no CA inhibitory activity (Knudsen et al, 2004;Weber et al, 2004). The ability of celecoxib and valdecoxib to inhibit CAs in vivo was confirmed in glaucomatous rabbits, where both drugs were able to lower intraocular pressure, suggesting that these agents may have utility in the treatment of this disorder (Weber et al, 2004).…”

Section: Carbonic Anhydrases As Targets For Celecoxibmentioning

confidence: 98%

“…Despite this telling chemical similarity, it came as a surprise when it was discovered that celecoxib displayed potent CA inhibitory activity in the low nanomolar range in vitro (Knudsen et al, 2004;Weber et al, 2004). In fact, its IC 50 towards the tumour-associated CAIX and CAXII enzymes was determined to be 16 and 18 nM, respectively (Di Fiore et al, 2006), and thus was more than double as potent than its inhibition of COX-2, where the IC 50 is 40 nM (Penning et al, 1997).…”

Section: Carbonic Anhydrases As Targets For Celecoxibmentioning

confidence: 99%

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Direct non-cyclooxygenase-2 targets of celecoxib and their potential relevance for cancer therapy

Schönthal

2007

Br J Cancer

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Celecoxib (Celebrex s ) was developed as a selective cyclooxygenase-2 (COX-2) inhibitor for the treatment of chronic pain. However, it now appears that this compound harbours additional pharmacologic activities that are entirely independent of its COX-2-inhibitory activity. This review presents the recently emerged direct non-COX-2 targets of celecoxib and their proposed role in mediating this drug's antitumour effects.

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Section: Carbonic Anhydrases As Targets For Celecoxibmentioning

confidence: 98%

Section: Carbonic Anhydrases As Targets For Celecoxibmentioning

confidence: 99%

Direct non-cyclooxygenase-2 targets of celecoxib and their potential relevance for cancer therapy

Schönthal

2007

Br J Cancer

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“…Literature evidence shows the CA inhibitory activity of celecoxib. 44 The 2D-similarity between these two molecules has a Tanimoto value of 0.12.…”

Section: Journal Of Chemical Information and Modelingmentioning

confidence: 99%

Exploring Polypharmacology Using a ROCS-Based Target Fishing Approach

AbdulHameed

Chaudhury

Singh

et al. 2012

J. Chem. Inf. Model.

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Polypharmacology has emerged as a new theme in drug discovery. In this paper, we studied polypharmacology using a ligand-based target fishing (LBTF) protocol. To implement the protocol, we first generated a chemogenomic database that links individual protein targets with a specified set of drugs or target representatives. Target profiles were then generated for a given query molecule by computing maximal shape/chemistry overlap between the query molecule and the drug sets assigned to each protein target. The overlap was computed using the program ROCS (Rapid Overlay of Chemical Structures). We validated this approach using the Directory of Useful Decoys (DUD). DUD contains 2950 active compounds, each with 36 property-matched decoys, against 40 protein targets. We chose a set of known drugs to represent each DUD target, and we carried out ligand-based virtual screens using data sets of DUD actives seeded into DUD decoys for each target. We computed Receiver Operator Characteristic (ROC) curves and associated area under the curve (AUC) values. For the majority of targets studied, the AUC values were significantly better than for the case of a random selection of compounds. In a second test, the method successfully identified off-targets for drugs such as rimantadine, propranolol, and domperidone that were consistent with those identified by recent experiments. The results from our ROCS-based target fishing approach are promising and have potential application in drug repurposing for single and multiple targets, identifying targets for orphan compounds, and adverse effect prediction.

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“…9 Hence new COX-2 inhibitors that are chemically different from the 1,2-diaryl class but at the same time possessing more enzyme specificity and less adverse side effects are required. The diaryl or aryl-heteroaryl ethers and thioethers are also known to be selective inhibitors of COX-2.…”

Section: Introductionmentioning

confidence: 99%

Chemical modifications of nimesulide

Pericherla¹,

Mareddy²,

P.³

et al. 2007

J. Braz. Chem. Soc.

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As modificações químicas da nimesulida via N-acilação direta ou através de um processo em duas etapas, envolvendo redução do grupo nitro seguida da acilação/sulfonilação regiosseletiva da arilamina resultante são descritas. A etapa da acilação do segundo método foi mais rápida do que a acilação da nimesulida. Uma série de derivados N-acilados e N-sulfonilados de N-(4-amino-2-fenóxi fenil)metanossulfonamida, obtidos a partir de nimesulida foram convenientemente preparados com bons a excelentes rendimentos. Alguns dos compostos sintetizados foram testados para inibição da ciclooxigenase e poucos mostraram seletividade para COX-2.We describe here the chemical modifications of nimesulide either via direct N-acylation or via a two-step process involving reduction of the nitro group followed by regioselective acylation/ sulfonylation of the resulting arylamine. The acylation step of the second approach was found to be faster than acylation of nimesulide. A number of N-acylated and N-sulfonylated derivatives of N-(4-amino-2-phenoxy phenyl)methanesulfonamide obtained from nimesulide were conveniently prepared in good to excellent yields. Some of the compounds synthesized were tested for cyclooxygenase inhibition and few of them showed selectivity for COX-2.

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Unexpected Nanomolar Inhibition of Carbonic Anhydrase by COX-2-Selective Celecoxib: New Pharmacological Opportunities Due to Related Binding Site Recognition

Cited by 428 publications

References 44 publications

Direct non-cyclooxygenase-2 targets of celecoxib and their potential relevance for cancer therapy

Direct non-cyclooxygenase-2 targets of celecoxib and their potential relevance for cancer therapy

Exploring Polypharmacology Using a ROCS-Based Target Fishing Approach

Chemical modifications of nimesulide

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