Your search keyword '"Acetazolamide chemistry"' showing total 152 results

51. Linker stability influences the anti-tumor activity of acetazolamide-drug conjugates for the therapy of renal cell carcinoma.

Author

Cazzamalli S, Corso AD, and Neri D

Subjects

Acetazolamide chemistry, Acetazolamide therapeutic use, Animals, Antineoplastic Agents chemistry, Antineoplastic Agents therapeutic use, Carbonic Anhydrase IX antagonists & inhibitors, Carbonic Anhydrase IX metabolism, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrase Inhibitors therapeutic use, Carcinoma, Renal Cell enzymology, Carcinoma, Renal Cell pathology, Cell Line, Tumor, Female, Humans, Kidney drug effects, Kidney enzymology, Kidney pathology, Kidney Neoplasms enzymology, Kidney Neoplasms pathology, Mice, Mice, Inbred BALB C, Mice, Nude, Oligopeptides chemistry, Oligopeptides therapeutic use, Acetazolamide administration & dosage, Antineoplastic Agents administration & dosage, Carbonic Anhydrase Inhibitors administration & dosage, Carcinoma, Renal Cell drug therapy, Drug Delivery Systems, Kidney Neoplasms drug therapy, Oligopeptides administration & dosage

Abstract

Small molecule-drug conjugates (SMDCs) are increasingly being considered as an alternative to antibody-drug conjugates (ADCs) for the selective delivery of anticancer agents to the tumor site, sparing normal tissues. Carbonic anhydrase IX (CAIX) is a membrane-bound enzyme, which is over-expressed in the majority of renal cell carcinomas and which can be efficiently targeted in vivo, using charged derivatives of acetazolamide, a small heteroaromatic sulfonamide. Here, we show that SMDC products, obtained by the coupling of acetazolamide with monomethyl auristatin E (MMAE) using dipeptide linkers, display a potent anti-tumoral activity in mice bearing xenografted SKRC-52 renal cell carcinomas. A comparative evaluation of four dipeptides revealed that SMDCs featuring valine-citrulline and valine-alanine linkers exhibited greater serum stability and superior therapeutic activity, compared to the counterparts with valine-lysine or valine-arginine linkers. The most active products substantially inhibited tumor growth over a prolonged period of time, in a tumor model for which sunitinib and sorafenib do not display therapeutic activity. However, complete tumor eradication was not possible even after ten intravenous injection. Macroscopic near-infrared imaging procedures confirmed that ligands had not lost the ability to selectively localize at the tumor site at the end of therapy and that the neoplastic masses continued to express CAIX. The findings are of mechanistic and of therapeutic significance, since CAIX is a non-internalizing membrane-associated antigen, which can be considered for targeted drug delivery applications in kidney cancer patients., Competing Interests: of potential conflict of interest: D.N. is a co-founder and shareholder of Philogen SpA, a company which develops antibody therapeutics and small molecule-drug conjugates, (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2017

52. Interrelation of the dissolution behavior and solid-state features of acetazolamide cocrystals.

Author

Arenas-García JI, Herrera-Ruiz D, Morales-Rojas H, and Höpfl H

Subjects

Crystallization, Solubility, X-Ray Diffraction methods, Acetazolamide chemistry, Acetazolamide metabolism

Abstract

The thermal behavior, phase stability, indicative stability and intrinsic dissolution rates of a series of cocrystals and cocrystal hydrates derived from the pharmaceutically active ingredient acetazolamide (ACZ) and 2-aminobenzamide (2ABAM), 2,3-dihydroxybenzoic acid (23DHBA), 2-hydroxybenzamide (2HBAM), 4-hydroxybenzoic acid (4HBA), nicotinamide (NAM) and picolinamide (PAM) as cocrystal formers have been evaluated. Upon heating in an inert atmosphere most of the cocrystals tested demonstrated first the elimination of the crystal former, followed by ACZ degradation. Only in cocrystals with NAM was melting observed. Under controlled temperature and relative humidity conditions all cocrystals tested were stable. However, phase stability tests in a medium simulating physiological conditions (HCl 0.01N, pH2.0) indicated that cocrystals ACZ-NAM-H 2 O and ACZ-PAM gradually transform into ACZ. All cocrystals examined gave enhanced intrinsic dissolution rates when compared to pure ACZ and the largest dissolution rate constants were measured for the cocrystals that transformed in the phase stability test (approximate two-fold increase of the dissolution rate constants). The series of cocrystals examined herein exhibits an inverse correlation between the intrinsic dissolution rates and the melting/decomposition temperatures as well as the dimension of the hydrogen-bonded ACZ aggregates found in the corresponding crystal structure, indicating that solid-state stability is the major influence on dissolution performance., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2017

53. Acetazolamide Serves as Selective Delivery Vehicle for Dipeptide-Linked Drugs to Renal Cell Carcinoma.

Author

Cazzamalli S, Dal Corso A, and Neri D

Subjects

Animals, Antineoplastic Agents pharmacokinetics, Carcinoma, Renal Cell drug therapy, Carcinoma, Renal Cell pathology, Cell Line, Tumor, Cell Survival drug effects, Disease Models, Animal, Dose-Response Relationship, Drug, Female, Humans, Ligands, Mice, Molecular Targeted Therapy, Tissue Distribution, Tumor Burden drug effects, Xenograft Model Antitumor Assays, Acetazolamide chemistry, Antineoplastic Agents administration & dosage, Dipeptides chemistry, Drug Carriers chemistry

Abstract

In most cases, cytotoxic drugs do not preferentially accumulate at the tumor site, causing unwanted toxicities and preventing dose escalation to therapeutically active regimens. Here, we show that acetazolamide derivatives, which bind to carbonic anhydrase IX (CAIX) on the surface of kidney cancer cells, selectively deliver payloads at the site of disease, sparing normal organs. Biodistribution studies, performed in tumor-bearing mice with acetazolamide derivatives bearing a technetium-99m chelator complex or a red fluorophore as payload, revealed a preferential tumor accumulation of the compound at doses up to 560 nmol/kg. The percentage of injected dose per gram in the tumor was dose-dependent and revealed optimal tumor:organ ratios at 140 nmol/kg, with a tumor:blood ratio of 80:1 at 6 hours. Acetazolamide, coupled to potent cytotoxic drugs via a dipeptide linker, exhibited a potent antitumor activity in nude mice bearing SKRC-52 renal cell carcinomas, whereas drug derivatives devoid of the acetazolamide moiety did not exhibit any detectable anticancer activity at the same doses. The observation of tumor regression with a noninternalizing ligand and with different cytotoxic moieties (MMAE and PNU-159682) indicates a general mechanism of action, based on the selective accumulation of the product on tumor cells, followed by the extracellular proteolytic release of the cytotoxic payload at the neoplastic site and the subsequent drug internalization into tumor cells. Acetazolamide-based drug conjugates may represent a promising class of targeted agents for the treatment of metastatic kidney cancer, as the majority of human clear cell renal cell carcinomas are strongly positive for CAIX. Mol Cancer Ther; 15(12); 2926-35. ©2016 AACR., Competing Interests: of potential conflict of interest: D.N. is a co-founder and shareholder of Philogen SpA, (©2016 American Association for Cancer Research.)

Published

2016

54. Inhibition of carbonic anhydrase IX in glioblastoma multiforme.

Author

Amiri A, Le PU, Moquin A, Machkalyan G, Petrecca K, Gillard JW, Yoganathan N, and Maysinger D

Subjects

Acetazolamide administration & dosage, Acetazolamide chemistry, Antineoplastic Agents administration & dosage, Brain Neoplasms enzymology, Carbonic Anhydrase Inhibitors administration & dosage, Caspase 3 metabolism, Cell Death, Cell Line, Tumor, Cell Proliferation drug effects, Combined Modality Therapy methods, Dacarbazine administration & dosage, Dacarbazine chemistry, Drug Carriers chemistry, Glioblastoma enzymology, Humans, Micelles, Spheroids, Cellular, Temozolomide, Time Factors, Tumor Cells, Cultured drug effects, Antineoplastic Agents chemistry, Brain Neoplasms pathology, Carbonic Anhydrase IX antagonists & inhibitors, Carbonic Anhydrase Inhibitors chemistry, Dacarbazine analogs & derivatives, Glioblastoma pathology

Abstract

Carbonic anhydrase IX (CAIX) is a transmembrane enzyme upregulated in several types of tumors including glioblastoma multiforme (GBM). GBM is among the most aggressive tumors among gliomas. Temozolomide (TMZ) therapy combined with surgical or radiation approaches is the standard treatment but not effective in long term. In this study we tested the treatment with acetazolamide (ATZ), an inhibitor of CAIX, alone or combined with TMZ. The experiments were performed in 2D and 3D cultures (spheroids) using glioblastoma U251N and human brain tumor stem cells (BTSCs). Several proteins implicated in tumor cell death were also investigated. The key results from these studies suggest the following: (1) Cell death of human glioblastoma spheroids and BTSC is significantly increased with combined treatment after 7 days, and (2) the effectiveness of ATZ is significantly enhanced against BTSC and U251N when incorporated into nano-carriers. Collectively, these results point toward the usefulness of nano-delivery of CAIX inhibitors and their combination with chemotherapeutics for glioblastoma treatment., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

55. Novel Water-Soluble Mucoadhesive Carbosilane Dendrimers for Ocular Administration.

Author

Bravo-Osuna I, Vicario-de-la-Torre M, Andrés-Guerrero V, Sánchez-Nieves J, Guzmán-Navarro M, de la Mata FJ, Gómez R, de Las Heras B, Argüeso P, Ponchel G, Herrero-Vanrell R, and Molina-Martínez IT

Subjects

Acetazolamide chemistry, Administration, Ophthalmic, Animals, Cell Line, Cell Survival drug effects, Dendrimers administration & dosage, Dendrimers pharmacology, Humans, Male, Rabbits, Silanes administration & dosage, Silanes pharmacology, Surface Plasmon Resonance, Dendrimers chemistry, Dendrimers pharmacokinetics, Silanes chemistry, Silanes pharmacokinetics

Abstract

The purpose of this research was to determine the potential use of water-soluble anionic and cationic carbosilane dendrimers (generations 1-3) as mucoadhesive polymers in eyedrop formulations. Cationic carbosilane dendrimers decorated with ammonium -NH3(+) groups were prepared by hydrosylilation of Boc-protected allylamine and followed by deprotection with HCl. Anionic carbosilane dendrimers with terminal carboxylate groups were also employed in this study. In vitro and in vivo tolerance studies were performed in human ocular epithelial cell lines and rabbit eyes respectively. The interaction of dendrimers with transmembrane ocular mucins was evaluated with a surface biosensor. As proof of concept, the hypotensive effect of a carbosilane dendrimer eyedrop formulation containing acetazolamide (ACZ), a poorly water-soluble drug with limited ocular penetration, was tested after instillation in normotensive rabbits. The methodology used to synthesize cationic dendrimers avoids the difficulty of obtaining neutral -NH2 dendrimers that require harsher reaction conditions and also present high aggregation tendency. Tolerance studies demonstrated that both prototypes of water-soluble anionic and cationic carbosilane dendrimers were well tolerated in a range of concentrations between 5 and 10 μM. Permanent interactions between cationic carbosilane dendrimers and ocular mucins were observed using biosensor assays, predominantly for the generation-three (G3) dendrimer. An eyedrop formulation containing G3 cationic carbosilane dendrimers (5 μM) and ACZ (0.07%) (289.4 mOsm; 5.6 pH; 41.7 mN/m) induced a rapid (onset time 1 h) and extended (up to 7 h) hypotensive effect, and led to a significant increment in the efficacy determined by AUC0(8h) and maximal intraocular pressure reduction. This work takes advantage of the high-affinity interaction between cationic carbosilane dendrimers and ocular transmembrane mucins, as well as the tensioactive behavior observed for these polymers. Our results indicate that low amounts of cationic carbosilane dendrimers are well tolerated and able to improve the hypotensive effect of an acetazolamide solution. Our results suggest that carbosilane dendrimers can be used in a safe range of concentrations to enhance the bioavailability of drugs topically administered in the eye.

Published

2016

56. Microwave assisted synthesis of novel acridine-acetazolamide conjugates and investigation of their inhibition effects on human carbonic anhydrase isoforms hCA I, II, IV and VII.

Author

Ulus R, Aday B, Tanç M, Supuran CT, and Kaya M

Subjects

Carbonic Anhydrase Inhibitors chemistry, Humans, Spectrum Analysis methods, Acetazolamide chemistry, Acetazolamide pharmacology, Carbonic Anhydrase Inhibitors pharmacology, Isoenzymes drug effects, Microwaves

Abstract

4-Amino-N-(5-sulfamoyl-1,3,4-thiadiazol-2-yl)benzamide was condensed with cyclic-1,3-diketones (dimedone and cyclohexane-1,3-dione) and aromatic aldehydes under microwave irradiation, leading to a series of acridine-acetazolamide conjugates. The new compounds were investigated as inhibitors of carbonic anhydrases (CA, EC 4.2.1.1), and more precisely cytosolic isoforms hCA I, II, VII and membrane-bound one hCA IV. All investigated isoforms were inhibited in low micromolar and nanomolar range by the new compounds. hCA IV and VII were inhibited with KIs in the range of 29.7-708.8nM (hCA IV), and of 1.3-90.7nM (hCA VII). For hCA I and II the KIs were in the range of 6.7-335.2nM (hCA I) and of 0.5-55.4nM (hCA II). The structure-activity relationships (SAR) for the inhibition of these isoforms with the acridine-acetazolamide conjugates reported here were delineated., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

57. Molecular dynamics study of human carbonic anhydrase II in complex with Zn(2+) and acetazolamide on the basis of all-atom force field simulations.

Author

Wambo TO, Chen LY, McHardy SF, and Tsin AT

Subjects

Acetazolamide chemistry, Carbonic Anhydrase II chemistry, Humans, Kinetics, Models, Molecular, Protein Binding, Thermodynamics, Zinc chemistry, Acetazolamide metabolism, Carbonic Anhydrase II metabolism, Molecular Dynamics Simulation, Zinc metabolism

Abstract

Human carbonic anhydrase II (hCAII) represents an ultimate example of the perfectly efficient metalloenzymes, which is capable of catalyzing the hydration of carbon dioxide with a rate approaching the diffusion controlled limit. Extensive experimental studies of this physiologically important metalloprotein have been done to elucidate the fundamentals of its enzymatic actions: what residues anchor the Zn(2+) (or another divalent cation) at the bottom of the binding pocket; how the relevant residues work concertedly with the divalent cation in the reversible conversions between CO2 and HCO3(-); what are the protonation states of the relevant residues and acetazolamide, an inhibitor complexed with hCAII, etc. In this article, we present a detailed computational study on the basis of the all-atom CHARMM force field where Zn(2+) is represented with a simple model of divalent cation using the transferrable parameters available from the current literature. We compute the hydration free energy of Zn(2+), the characteristics of hCAII-Zn(2+) complexation, and the absolute free energy of binding acetazolamide to the hCAII-Zn(2+) complex. In each of these three problems, our computed results agree with the experimental data within the known margin of error without making any case-by-case adjustments to the parameters. The quantitatively accurate insights we gain in this all-atom molecular dynamics study should be helpful in the search and design of more specific inhibitors of this and other carbonic anhydrases., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

58. A 99mTc-Labeled Ligand of Carbonic Anhydrase IX Selectively Targets Renal Cell Carcinoma In Vivo.

Author

Krall N, Pretto F, Mattarella M, Müller C, and Neri D

Subjects

Acetazolamide chemistry, Acetazolamide metabolism, Acetazolamide pharmacokinetics, Animals, Carcinoma, Renal Cell diagnostic imaging, Cell Line, Tumor, Gene Expression Regulation, Neoplastic, Humans, Isotope Labeling, Kidney Neoplasms diagnostic imaging, Ligands, Mice, Tissue Distribution, Tomography, Emission-Computed, Single-Photon, Carbonic Anhydrase IX metabolism, Carcinoma, Renal Cell metabolism, Kidney Neoplasms metabolism, Technetium chemistry

Abstract

Unlabelled: Small organic ligands, selective for tumor-associated antigens, are increasingly being considered as alternatives to monoclonal antibodies for the targeted delivery of diagnostic and therapeutic payloads such as radionuclides and drugs into neoplastic masses. We have previously described a novel acetazolamide derivative, a carbonic anhydrase ligand with high affinity for the tumor-associated isoform IX (CAIX), which can transport highly potent cytotoxic drugs into CAIX-expressing solid tumors. The aim of the present study was to quantitatively investigate the biodistribution properties of said ligand and understand whether acetazolamide conjugates merit further development as drug carriers and radioimaging agents., Methods: The conjugate described in this study, consisting of a derivative of acetazolamide, a spacer, and a peptidic (99m)Tc chelator, was labeled using sodium pertechnetate under reducing conditions and injected intravenously into CAIX-expressing SKRC-52 xenograft-bearing mice. Animals were sacrificed, and organ uptake as percentage injected activity of radiolabeled ligand per gram of tissues (%IA/g) was evaluated between 10 min and 24 h. Additionally, postmortem imaging by SPECT was performed., Results: The acetazolamide conjugate described in this study could be labeled to high radiochemical purity (>95%, 2.2-4.5 MBq/nmol). Analysis of organ uptake at various time points revealed that the ligand displayed a maximal tumor accumulation 3 h after intravenous injection (22 %IA/g), with an excellent tumor-to-blood ratio of 70:1 at the same time point. The ligand accumulation in the tumor was more efficient than in any other organ, but a residual uptake in the kidney, lung, and stomach (9, 16, and 10 %IA/g, respectively) was also observed, in line with patterns of carbonic anhydrase isoform expression in those tissues. Interestingly, tumor-to-organ ratios improved on administration of higher doses of radiolabeled ligand, suggesting that certain binding sites in normal organs can be saturated in vivo., Conclusion: The (99m)Tc-labeled acetazolamide conjugate exhibits high tumor uptake and favorable tumor-to-kidney ratios of up to 3 that may allow imaging of tumors in the kidney and distant sites at earlier time points than commonly possible with antibody-based products. These data suggest that the described molecule merit further development as a radioimaging agent for CAIX-expressing renal cell carcinoma., (© 2016 by the Society of Nuclear Medicine and Molecular Imaging, Inc.)

Published

2016

59. Acetazolamide polymorphism: a case of hybridization induced polymorphism?

Author

Sarkar S, Pavan MS, Cherukuvada S, and Guru Row TN

Subjects

Crystallization, Models, Chemical, Molecular Conformation, Molecular Structure, X-Ray Diffraction, Acetazolamide chemistry, Diuretics chemistry

Abstract

The unusual phenomenon of the formation of the kinetic form as against the thermodynamic form upon slow cooling of boiling aqueous solution in the case of diuretic drug acetazolamide is rationalized in terms of "hybridization induced polymorphism" based on extensive experimental and theoretical investigations.

Published

2016

60. Development of a mechanism and an accurate and simple mathematical model for the description of drug release: Application to a relevant example of acetazolamide-controlled release from a bio-inspired elastin-based hydrogel.

Author

Fernández-Colino A, Bermudez JM, Arias FJ, Quinteros D, and Gonzo E

Subjects

Animals, Delayed-Action Preparations chemistry, Delayed-Action Preparations pharmacokinetics, Delayed-Action Preparations pharmacology, Humans, Kinetics, Acetazolamide chemistry, Acetazolamide pharmacokinetics, Acetazolamide pharmacology, Models, Chemical

Abstract

Transversality between mathematical modeling, pharmacology, and materials science is essential in order to achieve controlled-release systems with advanced properties. In this regard, the area of biomaterials provides a platform for the development of depots that are able to achieve controlled release of a drug, whereas pharmacology strives to find new therapeutic molecules and mathematical models have a connecting function, providing a rational understanding by modeling the parameters that influence the release observed. Herein we present a mechanism which, based on reasonable assumptions, explains the experimental data obtained very well. In addition, we have developed a simple and accurate “lumped” kinetics model to correctly fit the experimentally observed drug-release behavior. This lumped model allows us to have simple analytic solutions for the mass and rate of drug release as a function of time without limitations of time or mass of drug released, which represents an important step-forward in the area of in vitro drug delivery when compared to the current state of the art in mathematical modeling. As an example, we applied the mechanism and model to the release data for acetazolamide from a recombinant polymer. Both materials were selected because of a need to develop a suitable ophthalmic formulation for the treatment of glaucoma. The in vitro release model proposed herein provides a valuable predictive tool for ensuring product performance and batch-to-batch reproducibility, thus paving the way for the development of further pharmaceutical devices.

Published

2016

61. Sulfonamide inhibition studies of the β-carbonic anhydrase from the newly discovered bacterium Enterobacter sp. B13.

Author

Eminoğlu A, Vullo D, Aşık A, Çolak DN, Çanakçı S, Beldüz AO, and Supuran CT

Subjects

Acetazolamide chemistry, Acetazolamide pharmacology, Carbonic Anhydrase I metabolism, Enterobacter drug effects, Enterobacteriaceae Infections microbiology, Humans, Methazolamide analogs & derivatives, Methazolamide pharmacology, Structure-Activity Relationship, Benzenesulfonamides, Carbonic Anhydrase I antagonists & inhibitors, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrase Inhibitors pharmacology, Enterobacter enzymology, Enterobacteriaceae Infections drug therapy, Sulfonamides chemistry, Sulfonamides pharmacology

Abstract

The genome of the newly identified bacterium Enterobacter sp. B13 encodes for a β-class carbonic anhydrases (CAs, EC 4.2.1.1), EspCA. This enzyme was recently cloned, and characterized kinetically by this group (J. Enzyme Inhib. Med. Chem. 2016, 31). Here we report an inhibition study with sulfonamides and sulfamates of this enzyme. The best EspCA inhibitors were some sulfanylated sulfonamides with elongated molecules, metanilamide, 4-aminoalkyl-benzenesulfonamides, acetazolamide, and deacetylated methazolamide (KIs in the range of 58.7-96.5nM). Clinically used agents such as methazolamide, ethoxzolamide, dorzolamide, brinzolamide, benzolamide, zonisamide, sulthiame, sulpiride, topiramate and valdecoxib were slightly less effective inhibitors (KIs in the range of 103-138nM). Saccharin, celecoxib, dichlorophenamide and many simple benzenesulfonamides were even less effective as EspCA inhibitors, with KIs in the range of 384-938nM. Identification of effective inhibitors of this bacterial enzyme may lead to pharmacological tools useful for understanding the physiological role(s) of the β-class CAs in bacterial pathogenicity/virulence., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

62. XModeScore: a novel method for accurate protonation/tautomer-state determination using quantum-mechanically driven macromolecular X-ray crystallographic refinement.

Author

Borbulevych O, Martin RI, Tickle IJ, and Westerhoff LM

Subjects

Humans, Acetazolamide chemistry, Carbonic Anhydrase II antagonists & inhibitors, Carbonic Anhydrase II chemistry, Crystallography, X-Ray methods, Software

Abstract

Gaining an understanding of the protein-ligand complex structure along with the proper protonation and explicit solvent effects can be important in obtaining meaningful results in structure-guided drug discovery and structure-based drug discovery. Unfortunately, protonation and tautomerism are difficult to establish with conventional methods because of difficulties in the experimental detection of H atoms owing to the well known limitations of X-ray crystallography. In the present work, it is demonstrated that semiempirical, quantum-mechanics-based macromolecular crystallographic refinement is sensitive to the choice of a protonation-state/tautomer form of ligands and residues, and can therefore be used to explore potential states. A novel scoring method, called XModeScore, is described which enumerates the possible protomeric/tautomeric modes, refines each mode against X-ray diffraction data with the semiempirical quantum-mechanics (PM6) Hamiltonian and scores each mode using a combination of energetic strain (or ligand strain) and rigorous statistical analysis of the difference electron-density distribution. It is shown that using XModeScore it is possible to consistently distinguish the correct bound protomeric/tautomeric modes based on routine X-ray data, even at lower resolutions of around 3 Å. These X-ray results are compared with the results obtained from much more expensive and laborious neutron diffraction studies for three different examples: tautomerism in the acetazolamide ligand of human carbonic anhydrase II (PDB entries 3hs4 and 4k0s), tautomerism in the 8HX ligand of urate oxidase (PDB entries 4n9s and 4n9m) and the protonation states of the catalytic aspartic acid found within the active site of an aspartic protease (PDB entry 2jjj). In each case, XModeScore applied to the X-ray diffraction data is able to determine the correct protonation state as defined by the neutron diffraction data. The impact of QM-based refinement versus conventional refinement on XModeScore is also discussed.

Published

2016

63. Inhibition of carbonic anhydrase isoforms I, II, IV, VII and XII with carboxylates and sulfonamides incorporating phthalimide/phthalic anhydride scaffolds.

Author

El-Azab AS, Abdel-Aziz AA, Ayyad RR, Ceruso M, and Supuran CT

Subjects

Acetazolamide chemistry, Carbonic Anhydrase Inhibitors chemical synthesis, Humans, Isoenzymes antagonists & inhibitors, Phthalic Anhydrides chemical synthesis, Phthalimides chemical synthesis, Sulfonamides chemical synthesis, ortho-Aminobenzoates chemical synthesis, Carbonic Anhydrase Inhibitors chemistry, Phthalic Anhydrides chemistry, Phthalimides chemistry, Sulfonamides chemistry, ortho-Aminobenzoates chemistry

Abstract

We report a panel of carboxylates and sulfonamides incorporating phthalic anhydride and phthalimide moieties in their structure and their interaction with the metalloenzyme carbonic anhydrase (CA, EC 4.2.1.1). They were synthesized from substituted anthranilic acids and trimellitic anhydride chloride, followed by reaction with primary amines and were tested for the inhibition of five physiologically relevant CA isoforms, the human (h) hCA I, II, IV, VII and XII, some of which are involved in serious pathologies (CA II, IV and XII in glaucoma; CA VII in epilepsy; CA XII in some solid tumors). The carboxylic acids were generally poor inhibitors of isoforms hCA I, II and IV but were highly effective, low nanomolar inhibitors of hCA VII and XII. The sulfonamides inhibited all isoforms significantly, and some of them were sub-nanomolar hCA VII inhibitors, although their isoform selectivity was lower compared to the carboxylates. This study proves that carboxylic acids incorporating a phthalic anhydride/phthalimide based scaffold may lead to isoform-selective inhibitors by applying the tail approach, mostly used up until now for obtaining sulfonamide, sulfamide and sulfamate CA inhibitors., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2016

64. Esterase activity of carbonic anhydrases serves as surrogate for selecting antibodies blocking hydratase activity.

Author

Uda NR, Seibert V, Stenner-Liewen F, Müller P, Herzig P, Gondi G, Zeidler R, van Dijk M, Zippelius A, and Renner C

Subjects

Acetazolamide chemistry, Acetazolamide pharmacology, Aconitate Hydratase metabolism, Antibodies, Monoclonal chemistry, Carbonic Anhydrase IX, Dose-Response Relationship, Drug, Enzyme Inhibitors chemistry, Humans, Molecular Structure, Structure-Activity Relationship, Aconitate Hydratase antagonists & inhibitors, Antibodies, Monoclonal pharmacology, Antigens, Neoplasm metabolism, Carbonic Anhydrases metabolism, Enzyme Inhibitors pharmacology, Esterases metabolism

Abstract

Carbonic anhydrase 9 (CA9) and carbonic anhydrase 12 (CA12) were proposed as potential targets for cancer therapy more than 20 years ago. However, to date, there are only very few antibodies that have been described to specifically target CA9 and CA12 and also block the enzymatic activity of their targets. One of the early stage bottlenecks in identifying CA9- and CA12-inhibiting antibodies has been the lack of a high-throughput screening system that would allow for rapid assessment of inhibition of the targeted carbon dioxide hydratase activity of carbonic anhydrases. In this study, we show that measuring the esterase activity of carbonic anhydrase offers a robust and inexpensive screening method for identifying antibody candidates that block both hydratase and esterase activities of carbonic anhydrase's. To our knowledge, this is the first implementation of a facile surrogate-screening assay to identify potential therapeutic antibodies that block the clinically relevant hydratase activity of carbonic anhydrases.

Published

2015

65. S···O chalcogen bonding in sulfa drugs: insights from multipole charge density and X-ray wavefunction of acetazolamide.

Author

Thomas SP, Jayatilaka D, and Guru Row TN

Subjects

Crystallography, X-Ray, Molecular Conformation, Static Electricity, Acetazolamide chemistry, Oxygen chemistry, Sulfur chemistry

Abstract

Experimental charge density analysis combined with the quantum crystallographic technique of X-ray wavefunction refinement (XWR) provides quantitative insights into the intra- and intermolecular interactions formed by acetazolamide, a diuretic drug. Firstly, the analysis of charge density topology at the intermolecular level shows the presence of exceptionally strong interaction motifs such as a DDAA-AADD (D-donor, A-acceptor) type quadruple hydrogen bond motif and a sulfonamide dimer synthon. The nature and strength of intra-molecular S···O chalcogen bonding have been characterized using descriptors from the multipole model (MM) and XWR. Although pure geometrical criteria suggest the possibility of two intra-molecular S···O chalcogen bonded ring motifs, only one of them satisfies the "orbital geometry" so as to exhibit an interaction in terms of an electron density bond path and a bond critical point. The presence of 'σ-holes' on the sulfur atom leading to the S···O chalcogen bond has been visualized on the electrostatic potential surface and Laplacian isosurfaces close to the 'reactive surface'. The electron localizability indicator (ELI) and Roby bond orders derived from the 'experimental wave function' provide insights into the nature of S···O chalcogen bonding.

Published

2015

66. Investigating the Selectivity of Metalloenzyme Inhibitors in the Presence of Competing Metalloproteins.

Author

Chen Y and Cohen SM

Subjects

Acetazolamide chemistry, Dose-Response Relationship, Drug, Humans, Metalloproteins metabolism, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Acetazolamide pharmacology, Metalloproteins antagonists & inhibitors

Abstract

Metalloprotein inhibitors (MPi) are an important class of therapeutics for the treatment of a variety of diseases, including hypertension, cancer, and HIV/AIDS. However, despite their clinical success, there is an apprehension that MPi may be less selective than other small-molecule therapeutics and more prone to inhibit off-target metalloenzymes. We examined the issue of MPi specificity by investigating the selectivity of a variety of MPi against a representative panel of metalloenzymes in the presence of competing metalloproteins (metallothionein, myoglobin, carbonic anhydrase, and transferrin). Our findings reveal that a wide variety of MPi do not exhibit a decrease in inhibitory activity in the presence of large excesses of competing metalloproteins, suggesting that the competing proteins do not titrate the MPi away from its intended target. This study represents a rudimentary but important means to mimic the biological milieu, which contains other metalloproteins that could compete the MPi away from its target. The strategy used in this study may be a useful approach to examine the selectivity of other MPi in development., (© 2015 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2015

67. Phosphate Chemical Probes Designed for Location Specific Inhibition of Intracellular Carbonic Anhydrases.

Author

Rankin GM, Vullo D, Supuran CT, and Poulsen SA

Subjects

Acetazolamide chemistry, Carbonic Anhydrase Inhibitors chemical synthesis, Cell Membrane Permeability, Glucose-6-Phosphate chemical synthesis, Glucose-6-Phosphate chemistry, Humans, Hydrogen-Ion Concentration, Intracellular Space enzymology, Isoenzymes antagonists & inhibitors, Isoenzymes chemistry, Molecular Probes chemical synthesis, Prodrugs chemical synthesis, Saccharin analogs & derivatives, Saccharin chemistry, Structure-Activity Relationship, Sulfonamides chemical synthesis, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases chemistry, Glucose-6-Phosphate analogs & derivatives, Molecular Probes chemistry, Prodrugs chemistry, Sulfonamides chemistry

Abstract

Chemical probes are small molecules designed to bind to a specific protein and disrupt the proteins function. Although many inhibitors are reported for human carbonic anhydrase (CA) enzymes, few may be considered useful as chemical probes as they exhibit broad action against the 12 catalytically active CA isozymes. In addition, most do not possess an appropriate physicochemical profile to discriminate intracellular CA activity from either global or extracellular CA activity. We report herein the synthesis of three monophosphate CA proinhibitors (compounds 2, 3, and 5) that are derived from cyclosaligenyl (cycloSal) phosphate and S-acyl-2-thioethyl (SATE) phosphate as protecting groups. The proinhibitors are designed as neutral, membrane-permeable compounds that once inside the cell may be hydrolyzed by pH-driven or enzymatic-driven mechanisms to release a negatively charged monophosphate. The resulting monophosphate compound is trapped intracellularly and available for locality specific inhibition of intracellular CAs.

Published

2015

68. Biochemical characterization of recombinant β-carbonic anhydrase (PgiCAb) identified in the genome of the oral pathogenic bacterium Porphyromonas gingivalis.

Author

Del Prete S, Vullo D, De Luca V, AlOthman Z, Osman SM, Supuran CT, and Capasso C

Subjects

Acetazolamide chemistry, Acetazolamide pharmacology, Amino Acid Sequence, Biocatalysis, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases chemistry, Carbonic Anhydrases isolation & purification, Dose-Response Relationship, Drug, Molecular Sequence Data, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins isolation & purification, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacology, Carbonic Anhydrases genetics, Carbonic Anhydrases metabolism, Porphyromonas gingivalis enzymology, Porphyromonas gingivalis genetics, Recombinant Proteins metabolism

Abstract

Carbonic anhydrases (CAs, EC 4.2.1.1) belonging to the α-, β-, γ-, δ- and ζ-CAs are ubiquitous metalloenzymes present in prokaryotes and eukaryotes. CAs started to be investigated in detail only recently in pathogenic bacteria, in the search for antibiotics with a novel mechanism of action, since it has been demonstrated that in many such organisms they are essential for the life cycle of the organism. CA inhibition leads to growth impairment or growth defects in several pathogenic bacteria. The microbiota of the human oral mucosa consists of a myriad of bacterial species, Porphyromonas gingivalis being one of them and the major pathogen responsible for the development of chronic periodontitis. The genome of P. gingivalis encodes for a β- and a γ-CAs. Recently, our group purified the recombinant γ-CA (named PgiCA) which was shown to possess a significant catalytic activity for the reaction that converts CO2 to bicarbonate and protons, with a kcat of 4.1 × 10(5 )s(-1) and a kcat/Km of 5.4 × 10(7 )M(-1 )× s(-1). We have also investigated its inhibition profile with a range of inorganic anions such as thiocyanate, cyanide, azide, hydrogen sulfide, sulfamate and trithiocarbonate. Here, we describe the cloning, purification and kinetic parameters of the other class of CA identified in the genome of P. gingivalis, the β-CA, named PgiCAb. This enzyme has a good catalytic activity, with a kcat of 2.8 × 10(5 )s(-1) and a kcat/Km of 1.5 × 10(7 )M(-1 )× s(-1). PgiCAb was also inhibited by the clinically used sulfonamide acetazolamide, with an inhibition constant of 214 nM. The role of CAs as possible virulence factors of P. gingivalis is poorly understood at the moment but their good catalytic activity and the fact that they might be inhibited by a large number of compounds, which may pave the way for finding inhibitors with antibacterial activity that may elucidate these phenomena and lead to novel antibiotics.

Published

2015

69. Optimal ligand descriptor for pocket recognition based on the Beta-shape.

Author

Kim JK, Won CI, Cha J, Lee K, and Kim DS

Subjects

Benchmarking, Binding Sites, Calcitriol chemistry, Drug Discovery, High-Throughput Screening Assays, Humans, Ligands, Principal Component Analysis, Protein Binding, Protein Conformation, Structure-Activity Relationship, User-Computer Interface, Acetazolamide chemistry, Algorithms, Calcitriol analogs & derivatives, Carbonic Anhydrases chemistry, Receptors, Calcitriol chemistry

Abstract

Structure-based virtual screening is one of the most important and common computational methods for the identification of predicted hit at the beginning of drug discovery. Pocket recognition and definition is frequently a prerequisite of structure-based virtual screening, reducing the search space of the predicted protein-ligand complex. In this paper, we present an optimal ligand shape descriptor for a pocket recognition algorithm based on the beta-shape, which is a derivative structure of the Voronoi diagram of atoms. We investigate six candidates for a shape descriptor for a ligand using statistical analysis: the minimum enclosing sphere, three measures from the principal component analysis of atoms, the van der Waals volume, and the beta-shape volume. Among them, the van der Waals volume of a ligand is the optimal shape descriptor for pocket recognition and best tunes the pocket recognition algorithm based on the beta-shape for efficient virtual screening. The performance of the proposed algorithm is verified by a benchmark test.

Published

2015

70. Cerenkov-specific contrast agents for detection of pH in vivo.

Author

Czupryna J, Kachur AV, Blankemeyer E, Popov AV, Arroyo AD, Karp JS, and Delikatny EJ

Subjects

Acetazolamide chemistry, Animals, Disease Models, Animal, Fluorodeoxyglucose F18, Hydrogen-Ion Concentration, Mice, Models, Chemical, Multimodal Imaging, Optics and Photonics, Phenolphthalein chemistry, Phenolsulfonphthalein chemistry, Photons, Positron-Emission Tomography, Radiopharmaceuticals, Contrast Media chemistry, Fluorine Radioisotopes chemistry, Phenolsulfonphthalein analogs & derivatives, Radioisotopes chemistry

Abstract

Unlabelled: We report the design, testing, and in vivo application of pH-sensitive contrast agents designed specifically for Cerenkov imaging. Radioisotopes used for PET emit photons via Cerenkov radiation. The multispectral emission of Cerenkov radiation allows for selective bandwidth quenching, in which a band of photons is quenched by absorption by a functional dye. Under acidic conditions, (18)F-labeled derivatives emit the full spectrum of Cerenkov light. Under basic conditions, the dyes change color and a wavelength-dependent quenching of Cerenkov emission is observed., Methods: Mono- and di-(18)F-labeled derivatives of phenolsulfonphthalein (phenol red) and meta-cresolsulfonphthalein (cresol purple) were synthesized by electrophilic fluorination. Cerenkov emission was measured at different wavelengths as a function of pH in vitro. Intramolecular response was measured in fluorinated probes and intermolecular quenching by mixing phenolphthalein with (18)F-FDG. Monofluorocresol purple (MFCP) was tested in mice treated with acetazolamide to cause urinary alkalinization, and Cerenkov images were compared with PET images., Results: Fluorinated pH indicators were produced with radiochemical yields of 4%-11% at greater than 90% purity. Selective Cerenkov quenching was observed intramolecularly with difluorophenol red or monofluorocresol purple and intermolecularly in phenolphthalein (18)F-FDG mixtures. The probes were selectively quenched in the bandwidth closest to the indicator's absorption maximum (λmax) at pHs above the indicator pKa (the negative logarithm of the acid dissociation constant). Addition of acid or base to the probes resulted in reversible switching from unquenched to quenched emission. In vivo, the bladders of acetazolamide-treated mice exhibited a wavelength-dependent quenching in Cerenkov emission, with the greatest reduction occurring near the λmax. Ratiometric imaging at 2 wavelengths showed significant decreases in Cerenkov emission at basic pH and allowed the estimation of absolute pH in vivo., Conclusion: We have created contrast agents that selectively quench photons emitted during Cerenkov radiation within a given bandwidth. In the presence of a functional dye, such as a pH indicator, this selective quenching allows for a functional determination of pH in vitro and in vivo. This method can be used to obtain functional information from radiolabeled probes using multimodal imaging. This approach allows for the imaging of nonfluorescent chromophores and is generalizable to any functional dye that absorbs at suitable wavelengths., (© 2015 by the Society of Nuclear Medicine and Molecular Imaging, Inc.)

Published

2015

71. Investigation of arenesulfonyl-2-imidazolidinones as potent carbonic anhydrase inhibitors.

Author

Abdel-Aziz AA, El-Azab AS, Ekinci D, Şentürk M, and Supuran CT

Subjects

Acetazolamide chemistry, Carbonic Anhydrase Inhibitors chemical synthesis, Enzyme Assays, Humans, Imidazolidines chemical synthesis, Kinetics, Nitrophenols chemistry, Recombinant Proteins chemistry, Structure-Activity Relationship, Carbonic Anhydrase I chemistry, Carbonic Anhydrase II chemistry, Carbonic Anhydrase Inhibitors chemistry, Imidazolidines chemistry

Abstract

A series of arenesulfonyl-2-imidazolidinones incorporating methyl, isopropyl, methoxy, halogen and phenyl moieties were prepared and tested as possible inhibitors of two members of the pH regulatory enzyme family, carbonic anhydrase (CA; EC 4.2.1.1). The inhibitory potencies of the compounds against human isoforms hCA I and hCA II were analyzed by an esterase assay with 4-nitrophenyl acetate as substrate, and the inhibition constants (KI) were calculated. Most compounds investigated here exhibited micromolar inhibition constants against the two isoenzymes. KI values were in the range of 10.2-40.6 μM for hCA I and of 13.1-31.4 μM for hCA II, respectively. Most of the imidazolidinones showed interesting CA inhibitory efficacy, some of them having comparable affinity (for hCA I) as the clinically used sulfonamide acetazolamide (AZA), but their efficacy against hCA II was much lower compared to AZA.

Published

2015

72. Synthesis and biological activity of novel thiourea derivatives as carbonic anhydrase inhibitors.

Author

Korkmaz N, Obaidi OA, Senturk M, Astley D, Ekinci D, and Supuran CT

Subjects

Acetazolamide chemistry, Carbonic Anhydrase Inhibitors chemical synthesis, Enzyme Assays, Humans, Kinetics, Nitrophenols chemistry, Phenol chemistry, Recombinant Proteins chemistry, Structure-Activity Relationship, Thiourea chemical synthesis, Amino Acids chemistry, Benzimidazoles chemistry, Carbonic Anhydrase I chemistry, Carbonic Anhydrase II chemistry, Carbonic Anhydrase Inhibitors chemistry, Thiourea analogs & derivatives

Abstract

A new series of chiral thiourea derivatives (5a-5c) and thiourea containing benzimidazole moieties (9b-9e) were synthesized from different amino acids (l-valine, l-isoleucine, l-methionine, l-phenylalanine, and d-phenylglycine). The compounds were characterized and tested against the two most studied members of the pH regulatory enzyme family, carbonic anhydrase (CA, EC 4.2.1.1). KI values of the novel compounds were measured in the range of 3.4-73.6 μM for hCA I isozyme and 8.7-1.44.2 μM for hCA II isozyme, respectively. Phenol was also tested as standard in order to understand the structure activity relationship and the clinically used sulfonamide acetazolamide was tested for comparison reasons. All of the compounds exhibited competitive inhibition with 4-nitrophenylacetate as substrate.

Published

2015

73. Intestinal uptake and toxicity evaluation of acetazolamide and its multicomponent complexes with hidroxypropyl-β-cyclodextrin in rats.

Author

Mora MJ, Petiti JP, Longhi MR, Torres AI, and Granero GE

Subjects

2-Hydroxypropyl-beta-cyclodextrin, Animals, Calcium administration & dosage, Calcium chemistry, Calcium pharmacokinetics, Calcium toxicity, Duodenum drug effects, Duodenum pathology, Duodenum ultrastructure, Ethanolamines administration & dosage, Ethanolamines chemistry, Ethanolamines pharmacokinetics, Ethanolamines toxicity, Intestinal Absorption, Intestinal Mucosa drug effects, Intestinal Mucosa pathology, Intestinal Mucosa ultrastructure, Male, Microscopy, Electron, Transmission, Rats, Wistar, Acetazolamide administration & dosage, Acetazolamide chemistry, Acetazolamide pharmacokinetics, Acetazolamide toxicity, beta-Cyclodextrins administration & dosage, beta-Cyclodextrins chemistry, beta-Cyclodextrins pharmacokinetics, beta-Cyclodextrins toxicity

Abstract

Large oral doses of ACZ lower the intraocular pressure (IOP), but usually lead to a multitude of systemic side effects, including gastrointestinal upset. The present study was undertaken to evaluate the effect of ACZ on the histological structure of rat duodenal mucosa and to assess a possible protective role of the complex formation of ACZ with HP-β-CD, either separately or in combination with a third compound, on the gut epithelial layer by histological and ultrastructural examinations of sections of rat duodenum exposed to ACZ or its formulations. In addition, the transport process of ACZ and its binary or ternary complexes across the duodenal mucosa by means of the single-pass intestinal perfusion (SPIP) method in rats was evaluated. Evidence was found that ACZ alters intestinal permeability and induces damage to the rat small intestine. In contrast, ACZ-induced intestinal injury may be abrogated by ACZ complexation. In addition, the complexation of ACZ with HP-β-CD, alone or in combination with a third compound, facilitated significant levels of ACZ uptake across the rat duodenal segment. Ternary complexes of ACZ with HP-β-CD in combination with TEA (triethanolamine) or calcium ions were found to provide an excellent approach that enabled an increased apparent permeability of ACZ across the duodenal epithelium, with a concomitant ability to preserve the integrity of the gut epithelium from ACZ-induced injury. These results could be useful for the design and development of novel ACZ formulations that can reduce GI toxicity, while still maintaining their essential therapeutic efficacies., (Copyright © 2014. Published by Elsevier B.V.)

Published

2015

74. Synthesis and Biological Potential Assessment of 2-Substituted Quinazolin-4(3H)-ones as Inhibitors of Phosphodiesterase-I and Carbonic Anhydrase-II.

Author

Saad SM, Saleem M, Perveen S, Alam MT, Khan KM, and Choudhary MI

Subjects

Acetazolamide chemistry, Animals, Carbonic Anhydrase II chemistry, Carbonic Anhydrase II isolation & purification, Carbonic Anhydrase Inhibitors chemistry, Drug Design, Edetic Acid chemistry, Enzyme Assays, Molecular Structure, Phosphodiesterase I chemistry, Phosphodiesterase I isolation & purification, Phosphodiesterase Inhibitors chemistry, Quinazolinones chemistry, Small Molecule Libraries chemistry, Snakes metabolism, Solutions, Structure-Activity Relationship, Carbonic Anhydrase II antagonists & inhibitors, Carbonic Anhydrase Inhibitors chemical synthesis, Phosphodiesterase I antagonists & inhibitors, Phosphodiesterase Inhibitors chemical synthesis, Quinazolinones chemical synthesis, Small Molecule Libraries chemical synthesis

Abstract

A library of twenty-five derivatives of 2-substituted quinazolin-4(3H)-ones 1-25 was synthesized and evaluated against phosphodiesterase-I (PDE) and carbonic anhydrase-II (CA). Compounds 17 (IC50 = 210.7 ± 2.62 µM), 16 (IC50 = 301.6 ± 1.18 µM), and 13 (IC50 = 458.13 ± 3.60 µM), selectively exhibited PDE inhibition while compounds 22 (IC50 = 61.33 ± 2.38 µM), 1 (IC50 = 108.30 ± 0.93 µM), and 21 (IC50 = 191.93 ± 2.72 µM), discriminatingly exhibited CA inhibition as compared to standards EDTA (IC50 = 277.69 ± 2.52 µM) and acetazolamide (IC50 = 0.12 ± 0.03 µM), for PDE and CA inhibitions, respectively. However, compound 15 was found to be active against both enzymes with the IC50 values 344.33 ± 4.32 µM and 20.94 ± 0.58 µM, for PDE and CA inhibitions, respectively. Remaining compounds were found to be inactive against both the enzymes. Structure-activity relationship studies are discussed herein.

Published

2015

75. Acetazolamide for the treatment of idiopathic intracranial hypertension.

Author

Supuran CT

Subjects

Acetazolamide chemistry, Acetazolamide pharmacology, Animals, Brain drug effects, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrase Inhibitors pharmacology, Humans, Acetazolamide therapeutic use, Carbonic Anhydrase Inhibitors therapeutic use, Pseudotumor Cerebri drug therapy

Abstract

Idiopathic intracranial hypertension (IIH) is characterized by an increase of intracranial pressure in the absence of neurologic tumors. The sulfonamide carbonic anhydrase (CA, EC 4.2.1.1) inhibitor (CAI) acetazolamide (AAZ), a compound developed in the 1950s as a diuretic drug and presently used as an antiglaucoma, antiepileptic and diuretic agent, is effective in the treatment of IIH. AAZ is a low nanomolar inhibitor of CA isoforms involved in cerebrospinal fluid (CSF) secretion. Inhibition of brain/choroid plexus CA II, IV, VA and XII leads to a decreased CSF fluid secretion and control of the intracranial pressure. Although many sulfonamide/sulfamate CAIs are in clinical use for decades, apparently only AAZ is being currently used clinically for IIH. We speculate that more lipophilic CAIs such as methazolamide, zonisamide or topiramate should lead to a more effective control of increased intracranial pressure, thus having the opportunity to become useful in the management of IIH.

Published

2015

76. Effectiveness of spray congealing to obtain physically stabilized amorphous dispersions of a poorly soluble thermosensitive API.

Author

Kulthe VV and Chaudhari PD

Subjects

Aerosols, Calorimetry, Differential Scanning, Chemistry, Pharmaceutical, Colloids, Crystallography, X-Ray, Drug Stability, Kinetics, Microscopy, Electron, Scanning, Powder Diffraction, Solubility, Solvents chemistry, Spectroscopy, Fourier Transform Infrared, Technology, Pharmaceutical methods, Acetazolamide chemistry, Plasticizers chemistry, Poloxamer chemistry, Temperature

Abstract

An amorphous phase produced by micronization up to the molecular or colloidal level of a poorly soluble drug having low lipophilicity can distinctly enhance its solubility characteristics. However, though dispersing the molten mass of a poorly water-soluble drug within polymeric matrix has been found to be most effective in formation of molecular dispersions, the drug molecules which melt at high temperature also accompanied by decomposition, such as acetazolamide, are difficult to formulate as molecular dispersions. Hence, a method is proposed to obtain molecular dispersions of acetazolamide with poloxamer-237 by spray congealing under optimal heat treatment. Uniform molecular and/or colloidal dispersions of the drug were achieved with instantaneous solvent evaporation by mixing a drug solution with molten mass of the plasticizer matrix. Immobilization of dispersed drug molecules was effected subsequently through rapid solidification by spray congealing. Initial characterization of 1:1, 1:1.5, and 1:2 ratios of solid dispersions and devitrification study of an optimized (1:2) ratio ensured efficacy of the proposed method in formation of physically stabilized amorphous systems without thermal degradation and hence resulted in more than ninefold rise in solubility and more than 90% dissolution within initial 10 min. With 1:2 ratio, molecular dispersions could be achieved by initial solvent evaporation stage, which when subjected to spray congealing produced physically stable amorphous systems, without signs of thermal degradation. This study also proposes an opportunity for selection of those polymers with which the drug is immiscible in their fluid state, yet obtaining molecular dispersions.

Published

2014

77. Carbonic anhydrase inhibition by 1-aroyl-3-(4-aminosulfonylphenyl)thioureas.

Author

Saeed A, Al-Rashida M, Hamayoun M, Mumtaz A, and Iqbal J

Subjects

Acetazolamide chemistry, Animals, Carbonic Anhydrase Inhibitors chemical synthesis, Cattle, Isothiocyanates chemistry, Molecular Docking Simulation, Molecular Structure, Solutions, Structure-Activity Relationship, Sulfanilamide, Sulfanilamides chemistry, Thiourea analogs & derivatives, Thiourea chemical synthesis, Carbonic Anhydrase II chemistry, Carbonic Anhydrase Inhibitors chemistry, Thiourea chemistry

Abstract

A series of 1-aroyl-3-(4-aminosulfonylphenyl)thioureas containing free sulfonamide group has been evaluated for their ability to inhibit bovine carbonic anhydrase II (bCA, EC 4.2.1.1). All compounds in the series were able to inhibit bCA II, the most active inhibitor had IC50 value of 0.26 ± 0.01 µM. Molecular docking studies and detailed structure-activity relationship studies were carried out. The absorption, distribution, metabolism, excretion (ADME) properties, as a predictor of oral absorption, were computationally calculated and compared with the clinically used drug acetazolamide.

Published

2014

78. The structure of a tetrameric α-carbonic anhydrase from Thermovibrio ammonificans reveals a core formed around intermolecular disulfides that contribute to its thermostability.

Author

James P, Isupov MN, Sayer C, Saneei V, Berg S, Lioliou M, Kotlar HK, and Littlechild JA

Subjects

Acetazolamide chemistry, Bacteria chemistry, Bacterial Proteins chemistry, Bacterial Proteins genetics, Bacterial Proteins metabolism, Carbon Dioxide metabolism, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrase Inhibitors metabolism, Carbonic Anhydrases genetics, Catalytic Domain, Cloning, Molecular, Crystallography, X-Ray, Disulfides chemistry, Enzyme Stability, Kinetics, Models, Molecular, Nitrophenols metabolism, Protein Conformation, Sulfanilamide, Sulfanilamides chemistry, Temperature, Carbonic Anhydrases chemistry, Carbonic Anhydrases metabolism

Abstract

Carbonic anhydrase enzymes catalyse the reversible hydration of carbon dioxide to bicarbonate. A thermophilic Thermovibrio ammonificans α-carbonic anhydrase (TaCA) has been expressed in Escherichia coli and structurally and biochemically characterized. The crystal structure of TaCA has been determined in its native form and in two complexes with bound inhibitors. The tetrameric enzyme is stabilized by a unique core in the centre of the molecule formed by two intersubunit disulfides and a single lysine residue from each monomer that is involved in intersubunit ionic interactions. The structure of this core protects the intersubunit disulfides from reduction, whereas the conserved intrasubunit disulfides are not formed in the reducing environment of the E. coli host cytosol. When oxidized to mimic the environment of the periplasmic space, TaCA has increased thermostability, retaining 90% activity after incubation at 70°C for 1 h, making it a good candidate for industrial carbon-dioxide capture. The reduction of all TaCA cysteines resulted in dissociation of the tetrameric molecule into monomers with lower activity and reduced thermostability. Unlike other characterized α-carbonic anhydrases, TaCA does not display esterase activity towards p-nitrophenyl acetate, which appears to result from the increased rigidity of its protein scaffold.

Published

2014

79. Development of acetazolamide-loaded, pH-triggered polymeric nanoparticulate in situ gel for sustained ocular delivery: in vitro. ex vivo evaluation and pharmacodynamic study.

Author

Singh J, Chhabra G, and Pathak K

Subjects

Acetazolamide chemistry, Animals, Chemistry, Pharmaceutical methods, Cornea drug effects, Delayed-Action Preparations chemistry, Drug Delivery Systems methods, Gels chemistry, Glaucoma drug therapy, Hydrogen-Ion Concentration, Intraocular Pressure drug effects, Nanoparticles chemistry, Ophthalmic Solutions chemistry, Particle Size, Permeability, Polymers chemistry, Rabbits, Suspensions administration & dosage, Suspensions classification, Acetazolamide administration & dosage, Delayed-Action Preparations administration & dosage, Gels administration & dosage, Nanoparticles administration & dosage, Ophthalmic Solutions administration & dosage, Polymers administration & dosage

Abstract

The objective of research was to develop a novel pH-triggered polymeric nanoparticulate in situ gel (NP-ISG) for ophthalmic delivery of acetazolamide (ACZ) to enhance the conjunctival permeation and precorneal residence time of the formulation by overcoming the limitations of protective ocular barriers. Nanoparticles (NP1--NP12) were developed by nanoprecipitation method and evaluated for pharmacotechnical characteristics including transmission electron microscopy. The optimized formulation, NP10 was dispersed in carbopol 934 P to form nanoparticulate in situ gels (NP-ISG1--NP-ISG5). NP-ISG5 was selected as optimized formulation on the basis of gelation ability and residence time. Ex vivo transcorneal permeation study exhibited significantly higher ACZ permeation from NP-ISG5 (74.50 ± 2.20 mg/cm(2)) and NP10 (93.5 ± 2.25 mg/cm(2)) than eye drops (20.08 ± 3.12 mg/cm(2)) and ACZ suspension (16.03 ± 2.14). Modified Draize test with zero score indicated nonirritant property of NP-ISG5. Corneal toxicity study revealed no visual signs of tissue damage. Further, NP-ISG5 when tested for hypotensive effect on intraocular pressure (IOP) in rabbits revealed that NP-ISG5 caused significant decrease in IOP (p < 0.05) in comparison to eye drops. Conclusively, NP-ISG5 may offer intensive management of glaucoma via higher permeation, prolonged precorneal residence time and sustained drug release along with higher in vitro efficacy, safety and patient compliance.

Published

2014

80. Freeze-dried amorphous dispersions for solubility enhancement of thermosensitive API having low molecular lipophilicity.

Author

Kulthe VV, Chaudhari PD, and Aboul-Enein HY

Subjects

Acetazolamide chemistry, Chemistry, Pharmaceutical methods, Drug Compounding, Drug Liberation, Drug Stability, Freeze Drying, Solubility, Solvents chemistry, Temperature, Acetazolamide administration & dosage, Drug Carriers chemistry, Mannitol chemistry

Abstract

The present study focuses on the development of an alternative 'thermally gentle' strategy such as freeze-drying to obtain not only solubility enhanced but also physically stabilised amorphous solid dispersions of acetazolamide, which melt with decomposition (M.P.~260°C). The solid dispersions were prepared by freeze-drying an aqueous dispersion of acetazolamide containing a lyoprotectant as sugar alcohol (mannitol) in 1:0.5, 1:1 and 1:2 proportions by weight. All the proportions of solid dispersions reported a marked increase in solubility characteristics compared to those of pure drug; with outstanding performance by 1:1 ratio of about 6 folds rise in saturation solubility and 90% drug release in about initial 30 minutes. This could be attributed to the formation amorphous molecular dispersions, cosolvent effect of mannitol on dispersed acetazolamide as well as its local solubilisation effect at the diffusion layer. During stability study also, 1:1 ratio of solid dispersions reported an insignificant change in solubility characteristics subjected to an unchanged amorphous nature. Such physical stability could be attributed to decreased molecular mobility of the drug molecules in amorphous carrier because of weaker drug-carrier interactions. Thus, it was demonstrated that freeze-drying is an effective method of forming dissolution-enhanced, amorphous solid dispersions of thermally degradable APIs., (© Georg Thieme Verlag KG Stuttgart · New York.)

Published

2014

81. Arylamino bisphosphonates: potent and selective inhibitors of the tumor-associated carbonic anhydrase XII.

Author

Tauro M, Loiodice F, Ceruso M, Supuran CT, and Tortorella P

Subjects

Acetazolamide chemistry, Acetazolamide pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Carbonic Anhydrase Inhibitors chemistry, Diphosphonates chemistry, Drug Delivery Systems, Enzyme Activation drug effects, Humans, Imidazoles chemistry, Imidazoles pharmacology, Inhibitory Concentration 50, Molecular Structure, Protein Isoforms chemistry, Structure-Activity Relationship, Zoledronic Acid, Antineoplastic Agents chemical synthesis, Carbonic Anhydrase Inhibitors chemical synthesis, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases chemistry, Diphosphonates chemical synthesis, Diphosphonates pharmacology

Abstract

A set of matrix metalloproteinases (MMPs) inhibitors, containing a bisphosphonate moiety (BP), has been evaluated for the inhibitory activity of carbonic anhydrases (CAs, EC 4.2.1.1). Human (h) isoforms hCA I, II, IX, XII and XIV were included in the study due to their involvement in crucial physiologic and pathologic processes. Some of these molecules selectively inhibited CA XII in the nanomolar range, showing an attractive dual mechanism (anti-MMP and anti-CA) of action as potential antitumor agents. The BP inhibitors investigated in this study are also excellent leads for obtaining even more effective compounds able to selectively target membrane-bound CA XII and having the potential to be used as tools for understanding physiologic processes regulated by this isoform., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

82. Pulmonary vasodilation by acetazolamide during hypoxia: impact of methyl-group substitutions and administration route in conscious, spontaneously breathing dogs.

Author

Pickerodt PA, Francis RC, Höhne C, Neubert F, Telalbasic S, Boemke W, and Swenson ER

Subjects

Acetazolamide chemistry, Administration, Inhalation, Administration, Oral, Animals, Arterial Pressure drug effects, Carbonic Anhydrase Inhibitors administration & dosage, Carbonic Anhydrase Inhibitors chemistry, Disease Models, Animal, Dogs, Female, Hypoxia enzymology, Infusions, Intravenous, Methylation, Pulmonary Artery physiopathology, Structure-Activity Relationship, Time Factors, Vascular Resistance drug effects, Vasodilator Agents chemistry, Acetazolamide administration & dosage, Hypoxia physiopathology, Pulmonary Artery drug effects, Respiration, Vasodilation drug effects, Vasodilator Agents administration & dosage

Abstract

Acetazolamide (ACZ) prevents hypoxic pulmonary vasoconstriction (HPV) in isolated lungs, animals, and humans, but not by carbonic anhydrase (CA) inhibition. We studied administration routes in, and certain structural aspects of, ACZ critical to HPV inhibition. Analogs of ACZ during acute hypoxia were tested in unanesthetized dogs. Dogs breathed normoxic gas for 1 h (inspired O2 fraction = 0.21), followed by 10% O2 for 2 h (hypoxia) in these protocols: 1) controls; 2) ACZ intravenously (2 mg · kg(-1) · h(-1)); 3) ACZ orally (5 mg/kg, 12 and 1 h before the experiment); 4) inhaled ACZ (750 mg); 5) methazolamide (MTZ) intravenously (3 mg · kg(-1) · h(-1)); and 6) N-methyl-acetazolamide (NMA) intravenously (10 mg · kg(-1) · h(-1)). In controls, mean pulmonary arterial pressure (MPAP) increased 7 mmHg, and pulmonary vascular resistance (PVR) 224 dyn · s · cm(-5) with hypoxia (P < 0.05). With intravenous and inhaled ACZ, MPAP and PVR did not change during hypoxia. With oral ACZ, HPV was only slightly suppressed; MPAP increased 5 mmHg and PVR by 178 dyn · s · cm(-5) during hypoxia. With MTZ and NMA, the MPAP rise (4 ± 2 mmHg) was reduced, and PVR did not increase during hypoxia compared with normoxia (MTZ intravenous: 81 ± 77 and 68 ± 82 dyn · s · cm(-5) with NMA intravenous). Inhaled ACZ prevents HPV, but not without causing systemic CA inhibition. NMA, a compound lacking CA inhibiting effects by methylation at the sulfonamide moiety, and MTZ, a CA-inhibiting analog methylated at the thiadiazole ring, are only slightly less effective than ACZ in reducing HPV.

Published

2014

83. Probing influence of methodological variation on active loading of acetazolamide into nanoliposomes: biophysical, in vitro, ex vivo, in vivo and rheological investigation.

Author

Pisal PB, Joshi MA, Padamwar MN, Patil SS, and Pokharkar VB

Subjects

Acetazolamide chemistry, Acetazolamide pharmacology, Administration, Ophthalmic, Animals, Carbonic Anhydrase Inhibitors chemistry, Chemistry, Pharmaceutical methods, Drug Compounding methods, Drug Delivery Systems, Drug Stability, Glaucoma drug therapy, Glaucoma physiopathology, Liposomes, Male, Particle Size, Rabbits, Rheology, Acetazolamide administration & dosage, Carbonic Anhydrase Inhibitors administration & dosage, Intraocular Pressure drug effects, Nanoparticles

Abstract

In the present work comparative evaluation of acetate and pH gradient techniques for effective drug loading in liposomes has been investigated. The acetazolamide (ACZ) loaded liposomes prepared by two methods were analyzed by vesicle size analysis, zeta potential, percent encapsulation efficiency, in vitro drug release studies and intraocular pressure lowering activity. ICH guidelines were followed for determining stability of the prepared liposomes. The superiority of acetate gradient method for active loading of acetazolamide has been established. The prepared acetate gradient positive liposomes showed extended hypotensive effect when compared to other liposomal formulations. Thus ACZ loaded liposomes prepared by acetate gradient technique may serve as promising ocular delivery system in the treatment of glaucoma. The current work emphasizes the fact that the techniques used for active drug loading into liposomes strongly influence the pharmaceutical performance of the final formulation., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2014

84. Carbonic anhydrase inhibitors and high altitude illnesses.

Author

Swenson ER

Subjects

Acetazolamide chemistry, Alkalosis metabolism, Alkalosis pathology, Altitude, Altitude Sickness classification, Altitude Sickness pathology, Carbonic Anhydrase Inhibitors chemistry, Humans, Hypoxia metabolism, Hypoxia pathology, Acetazolamide therapeutic use, Altitude Sickness drug therapy, Carbonic Anhydrase Inhibitors therapeutic use, Carbonic Anhydrases chemistry

Abstract

Carbonic anhydrase (CA) inhibitors, particularly acetazolamide, have been used at high altitude for decades to prevent or reduce acute mountain sickness (AMS), a syndrome of symptomatic intolerance to altitude characterized by headache, nausea, fatigue, anorexia and poor sleep. Principally CA inhibitors act to further augment ventilation over and above that stimulated by the hypoxia of high altitude by virtue of renal and endothelial cell CA inhibition which oppose the hypocapnic alkalosis resulting from the hypoxic ventilatory response (HVR), which acts to limit the full expression of the HVR. The result is even greater arterial oxygenation than that driven by hypoxia alone and greater altitude tolerance. The severity of several additional diseases of high attitude may also be reduced by acetazolamide, including high altitude cerebral edema (HACE), high altitude pulmonary edema (HAPE) and chronic mountain sickness (CMS), both by its CA-inhibiting action as described above, but also by more recently discovered non-CA inhibiting actions, that seem almost unique to this prototypical CA inhibitor and are of most relevance to HAPE. This chapter will relate the history of CA inhibitor use at high altitude, discuss what tissues and organs containing carbonic anhydrase play a role in adaptation and maladaptation to high altitude, explore the role of the enzyme and its inhibition at those sites for the prevention and/or treatment of the four major forms of illness at high altitude.

Published

2014

85. New mucoadhesive polymeric film for ophthalmic administration of acetazolamide.

Author

Tártara LI, Palma SD, Allemandi D, Ahumada MI, and Llabot JM

Subjects

Acetazolamide chemistry, Adhesives chemistry, Animals, Chemistry, Pharmaceutical, Polymers chemistry, Rabbits, Acetazolamide administration & dosage, Adhesives administration & dosage, Administration, Ophthalmic, Drug Delivery Systems trends, Polymers administration & dosage

Abstract

This article reports the results concerning the design and manufacture of a novel polymeric film for ocular administration of acetazolamide (AZM), and a patent document presented to INPI- National Institute of Industrial/Intelectual Property. The system was designed using mucoadhesive polymers, such as carbomer (CB974P) and sodium carboxymethylcellulose (NaCMC), combined with the poloxamer (POL407) which behaves as a swelling modulator, surfactant and slightly plasticizer. The maximum amount of AZM to be incorporated without loss of homogeneity or precipitation of the drug, was 0.04 mg AZM/mg of the film. The addition of a polymeric coating based on Eudragit RSPO (cationic permeable polymethacrylate polymer) allowed optimizing drug release. The coating in a proportion of 10% (determined as percentage of total weight of the film) seemed to be the most adequate, since 80% of controlled drug release was achieved along 240 minutes. This coating membrane did not affect the mucoadhesive properties of the swellable polymers. Thus, the system obtained, showed good efficiency and the intra ocular pressure (IOP) decreased according to the results derived from in vivo studies performed on normotensive rabbits. Finally, irritation scored studies demonstrated that these systems were not irritant for rabbit´s ocular mucosa.

Published

2014

86. Ligand binding analysis and screening by chemical denaturation shift.

Author

Schön A, Brown RK, Hutchins BM, and Freire E

Subjects

Calorimetry, Humans, Hydrogen-Ion Concentration, Kinetics, Ligands, Protein Binding, Protein Conformation, Protein Denaturation, Spectrometry, Fluorescence, Temperature, Thermodynamics, Acetazolamide chemistry, Carbonic Anhydrase I chemistry, HIV Protease chemistry, Mesylates chemistry, Oxalates chemistry, Piperidines chemistry, Urea chemistry

Abstract

The identification of small molecule ligands is an important first step in drug development, especially drugs that target proteins with no intrinsic activity. Toward this goal, it is important to have access to technologies that are able to measure binding affinities for a large number of potential ligands in a fast and accurate way. Because ligand binding stabilizes the protein structure in a manner dependent on concentration and binding affinity, the magnitude of the protein stabilization effect elicited by binding can be used to identify and characterize ligands. For example, the shift in protein denaturation temperature (Tm shift) has become a popular approach to identify potential ligands. However, Tm shifts cannot be readily transformed into binding affinities, and the ligand rank order obtained at denaturation temperatures (≥60°C) does not necessarily coincide with the rank order at physiological temperature. An alternative approach is the use of chemical denaturation, which can be implemented at any temperature. Chemical denaturation shifts allow accurate determination of binding affinities with a surprisingly wide dynamic range (high micromolar to sub nanomolar) and in situations where binding changes the cooperativity of the unfolding transition. In this article, we develop the basic analytical equations and provide several experimental examples., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

87. Cloning, purification and preliminary crystallographic analysis of the complex of Helicobacter pylori α-carbonic anhydrase with acetazolamide.

Author

Modak JK, Revitt-Mills SA, and Roujeinikova A

Subjects

Cloning, Molecular, Crystallography, X-Ray, Recombinant Proteins chemistry, Acetazolamide chemistry, Bacterial Proteins chemistry, Carbonic Anhydrases chemistry, Helicobacter pylori enzymology

Abstract

Helicobacter pylori infection of the stomach can lead to severe gastroduodenal diseases such as gastritis, peptic ulcers and gastric cancers. Periplasmic H. pylori α-carbonic anhydrase (HpαCA) is essential for the acclimatization of the bacterium to the acidity of the stomach. Through the action of urease and carbonic anhydrases, the H. pylori periplasmic pH is maintained at around 6 in an environment with a pH as low as 2, which in turn facilitates the maintenance of a cytoplasmic pH close to neutral, allowing growth in the gastric niche. Crystals of HpαCA in complex with the inhibitor acetazolamide have been grown by the hanging-drop vapour-diffusion method using polyethylene glycol as a precipitating agent. The crystals have the symmetry of space group P2(1)2(1)2(1), with unit-cell parameters a = 37.0, b = 82.4, c = 150.8 Å. An X-ray diffraction data set was collected from a single crystal to 1.7 Å resolution. Calculation of the self-rotation function using this data and molecular replacement showed that the asymmetric unit contains an HpαCA dimer.

Published

2013

88. Characterization, dissolution and in vivo evaluation of solid acetazolamide complexes.

Author

Mora MJ, Tártara LI, Onnainty R, Palma SD, Longhi MR, and Granero GE

Subjects

2-Hydroxypropyl-beta-cyclodextrin, Animals, Ethanolamines chemistry, Intraocular Pressure drug effects, Rabbits, Temperature, beta-Cyclodextrins chemistry, Acetazolamide chemistry, Acetazolamide pharmacology

Abstract

The effects of binary and ternary systems of acetazolamide (ACZ) with hydroxypropyl-β-cyclodextrin (HP-β-CD) alone or with triethanolamine (TEA) on the crystalline properties, dissolution and intraocular pressure (IOP)-lowering effect were investigated. It was found that the crystal structure of ACZ powder could be modified by the processing conditions. Freeze-drying ACZ powder affected not only the particle morphology but also its polymorphic form and the starting ACZ was converted to pure form A upon freeze-drying treatment. Results provided by DSC/TGA, XRPD, SEM and FT-IR suggested the formation of inclusion complexes between ACZ with HP-β-CD alone or with TEA, obtained by the freeze-drying method and the conversion of the drug into the amorphous state. Binary and ternary systems of ACZ obtained by freeze-drying exhibited significantly enhanced ACZ dissolution rates. The IOP-lowering effects of ACZ and its complexes with HP-β-CD alone or with TEA were studied in normotensive rabbits. Whereas the maximum IOP-lowering effect (~4 mmHg, ~33%), obtained with these binary and ternary lyophilized ACZ systems occurred at around 90 min, the ternary system exhibited a longer maximum IOP-lowering effect peak compared with that of the binary system. These results are in line with those obtained from the dissolution studies, where the ternary system exhibited longer dissolution times compared to the lyophilized binary one. Results obtained from the dissolution studies, also showed that freeze-drying the native crystalline form of ACZ significantly increased the dissolution rate of ACZ, thus improving the IOP-lowering effect of this drug., (Copyright © 2013. Published by Elsevier Ltd.)

Published

2013

89. Effect of incorporating a thiophene tail in the scaffold of acetazolamide on the inhibition of human carbonic anhydrase isoforms I, II, IX and XII.

Author

Biswas S, McKenna R, and Supuran CT

Subjects

Antigens, Neoplasm metabolism, Binding Sites, Carbonic Anhydrase I metabolism, Carbonic Anhydrase II metabolism, Carbonic Anhydrase IX, Carbonic Anhydrases metabolism, Catalytic Domain, Crystallography, X-Ray, Humans, Molecular Conformation, Molecular Docking Simulation, Acetazolamide chemistry, Antigens, Neoplasm chemistry, Carbonic Anhydrase I antagonists & inhibitors, Carbonic Anhydrase II antagonists & inhibitors, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases chemistry, Thiophenes chemistry

Abstract

The high resolution crystal structure of 5-(2-thienylacetamido)-1,3,4-thiadiazole-2-sulfonamide complexed to human (h) carbonic anhydrase (CA, EC 4.2.1.1) isoform hCA II is reported. The compound binds in a similar manner with acetazolamide when the sulfamoyl-thiadiazolyl-acetamido fragment of the two compounds is considered, but the thienyl tail was positioned in the subpocket 2, rarely observed by other investigated CA inhibitors. This positioning allows interaction with amino acid residues (such as Asn67, Ile91, Gln92 and Val121 which are variable in other isoforms of medicinal chemistry interest, such as hCA I, IX and XII. Indeed, the investigated sulfonamide was a medium potency hCA I and II inhibitor but was highly effective as a hCA IX and XII inhibitor. This different behavior with respect to acetazolamide (a promiscuous inhibitor of all these isoforms) has been explained by resolving the crystal structure, and may be used to design more isoform-selective compounds., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

90. Interaction of antihypertensive acetazolamide with nonsteroidal anti-inflammatory drugs.

Author

Jabeen E, Qureshi R, and Shah A

Subjects

Computer Simulation, Drug Interactions, Hydrogen-Ion Concentration, Models, Molecular, Acetazolamide chemistry, Anti-Inflammatory Agents, Non-Steroidal chemistry, Antihypertensive Agents chemistry

Abstract

The binding of antihypertensive acetazolamide with eleven nonsteroidal anti-inflammatory drugs (NSAIDs) was investigated at pH 3, 7 and 9.5 with the objective of monitoring their interactive pharmacokinetics during digestion and absorption in human body. The results of UV-Vis spectroscopy and cyclic voltammetry revealed two NSAIDs (acetaminophen and dichlofenic sodium) to interact with acetazolamide in stomach fluid conditions forming complexes of 1:1 and 1:2 stoichiometry. The complexation ratio was also verified by computational methods. The strong binding propensity of acetaminophen and dichlofenic sodium with acetazolamide prohibited their combined therapy. However, the poor binding affinity of aspirin and mefinamic acid suggested these drugs as preferred NSAIDs to be prescribed with acetazolamide., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2013

91. Hypoxia induced CA9 inhibitory targeting by two different sulfonamide derivatives including acetazolamide in human glioblastoma.

Author

Said HM, Hagemann C, Carta F, Katzer A, Polat B, Staab A, Scozzafava A, Anacker J, Vince GH, Flentje M, and Supuran CT

Subjects

Antigens, Neoplasm genetics, Brain Neoplasms drug therapy, Brain Neoplasms enzymology, Carbonic Anhydrase IX, Carbonic Anhydrases genetics, Cell Hypoxia, Cell Line, Tumor, Down-Regulation drug effects, Gene Expression Regulation, Neoplastic drug effects, Glioblastoma drug therapy, Glioblastoma enzymology, Humans, Models, Molecular, RNA, Messenger genetics, RNA, Small Interfering genetics, Acetazolamide chemistry, Acetazolamide pharmacology, Antigens, Neoplasm metabolism, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases metabolism, Sulfonamides chemistry, Sulfonamides pharmacology

Abstract

HIF-1α regulated genes are mainly responsible for tumour resistance to radiation- and chemo-therapy. Among these genes, carbonic anhydrase isoform IX (CA9) is highly over expressed in many types of cancer especially in high grade brain cancer like Glioblastoma (GBM). Inhibition of the enzymatic activity by application of specific chemical CA9 inhibitor sulphonamides (CAI) like Acetazolamide (Aza.), the new sulfonamide derivative carbonic anhydrase inhibitor (SU.D2) or indirect inhibitors like the HIF-1α inhibitor Chetomin or molecular inhibitors like CA9-siRNA are leading to an inhibition of the functional role of CA9 during tumorigenesis. Human GBM cells were treated with in vitro hypoxia (1, 6, or 24 h at 0.1%, O2). Aza. application was at a range between 250 and 8000 nM and the HIF-1α inhibitor Chetomin at a concentration range of 150-500 nM. Cell culture plates were incubated for 24 h under hypoxia (0.1% O2). Further, CA9-siRNA constructs were transiently transfected into GBM cells exposed to extreme hypoxic aeration conditions. CA9 protein expression level was detectable in a cell-type specific manner under normoxic conditions. Whereas U87-MG exhibited a strong aerobic expression, U251 and U373 displayed moderate and GaMG very weak normoxic CA9 protein bands. Aza. as well as SU.D2 displayed inhibitory characteristics to hypoxia induced CA9 expression in the four GBM cell lines for 24 h of hypoxia (0.1% O2) at concentrations between 3500 and 8000 nM, on both the protein and mRNA level. Parallel experiments using CA9-siRNA confirmed these results. Application of 150-500 nM of the glycolysis inhibitor Chetomin under similar oxygenation conditions led to a sharply reduced expression of both CA IX protein and CA9 mRNA levels, indicating a clear glucose availability involvement for the hypoxic HIF-1α and CA9 expression in GBM cells. Hypoxia significantly influences the behaviour of human tumour cells by activation of genes involved in the adaptation to hypoxic stress. The main objective in malignant GBM therapy is either to eradicate the tumour or to convert it into a controlled, quiescent chronic disease. Aza., SU.D2, Chetomin or CA9-siRNA possesses functional CA9 inhibitory characteristics when applied against human cancers with hypoxic regions like GBM. They may be used as alternative or in conjunction with other direct inhibitors possessing similar functionality, thereby rendering them as potential optimal tools for the development of an optimized therapy in human brain cancer treatment., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

92. Evaluation of enhanced thermostability and operational stability of carbonic anhydrase from Micrococcus species.

Author

Bhattacharya A, Shrivastava A, and Sharma A

Subjects

Acetazolamide chemistry, Bacterial Proteins isolation & purification, Cadmium chemistry, Calcium Carbonate chemistry, Carbon Dioxide chemistry, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases chemistry, Enzyme Activation, Enzyme Stability, Ethoxzolamide chemistry, Hydrogen-Ion Concentration, Molecular Weight, Temperature, Zinc chemistry, Bacterial Proteins chemistry, Carbonic Anhydrases isolation & purification, Micrococcus luteus enzymology

Abstract

Carbonic anhydrase (CA) was purified from Micrococcus lylae and Micrococcus luteus with 49.90 and 53.8 % yield, respectively, isolated from calcium carbonate kilns. CA from M. lylae retained 80 % stability in the pH and temperature range of 6.0-8.0 and 35-45 °C, respectively. However, CA from M. luteus was stable in the pH and temperature range of 7.5-10.0 and 35-55 °C, respectively. Cross-linked enzyme aggregates (CLEAs) raised the transition temperature of M. lylae and M. luteus CA up to 67.5 and 74.0 °C, while the operational stability (T(1/20) of CA at 55 °C was calculated to be 7.7 and 12.0 h, respectively. CA from both the strains was found to be monomeric in nature with subunit molecular weight and molecular mass of 29 kDa. Ethoxozolamide was identified as the most potent inhibitor based on both IC(50) values and inhibitory constant measurement (K(i)). The K(m) and V(max) for M. lylae CA (2.31 mM; 769.23 μmol/mg/min) and M. luteus CA (2.0 mM; 1,000 μmol/mg/min) were calculated from Lineweaver-Burk plots in terms of esterase activity. Enhanced thermostability of CLEAs alleviates its role in operational stability for application at an on-site scrubber. The characteristic profile of purified CA from Micrococcus spp. advocates its effective application in biomimetic CO(2) sequestration.

Published

2013

93. Effects of cryoprotectants on the structure and thermostability of the human carbonic anhydrase II-acetazolamide complex.

Author

Aggarwal M, Boone CD, Kondeti B, Tu C, Silverman DN, and McKenna R

Subjects

Calorimetry, Differential Scanning, Carbonic Anhydrase II antagonists & inhibitors, Carbonic Anhydrase II metabolism, Catalytic Domain, Cryoprotective Agents chemistry, Crystallography, X-Ray, Glycerol chemistry, Glycerol metabolism, Glycerol pharmacology, Humans, Kinetics, Models, Molecular, Protein Conformation, Sucrose chemistry, Temperature, Acetazolamide chemistry, Carbonic Anhydrase II chemistry, Carbonic Anhydrase Inhibitors chemistry, Cryoprotective Agents pharmacology, Enzyme Stability drug effects

Abstract

Protein X-ray crystallography has seen a progressive shift from data collection at cool/room temperature (277-298 K) to data collection at cryotemperature (100 K) because of its ease of crystal preparation and the lessening of the detrimental effects of radiation-induced crystal damage, with 20-25%(v/v) glycerol (GOL) being the preferred choice of cryoprotectant. Here, a case study of the effects of cryoprotectants on the kinetics of carbonic anhydrase II (CA II) and its inhibition by the clinically used inhibitor acetazolamide (AZM) is presented. Comparative studies of crystal structure, kinetics, inhibition and thermostability were performed on CA II and its complex with AZM in the presence of either GOL or sucrose. These results suggest that even though the cryoprotectant GOL was previously shown to be directly bound in the active site and to interact with AZM, it affects neither the thermostability of CA II nor the binding of AZM in the crystal structure or in solution. However, addition of GOL does affect the kinetics of CA II, presumably as it displaces the water proton-transfer network in the active site.

Published

2013

94. Carbonic anhydrase inhibitors: inhibition of the β-class enzyme from the pathogenic yeast Candida glabrata with sulfonamides, sulfamates and sulfamides.

Author

Vullo D, Leewattanapasuk W, Mühlschlegel FA, Mastrolorenzo A, Capasso C, and Supuran CT

Subjects

Acetazolamide chemistry, Amino Acid Sequence, Antifungal Agents chemical synthesis, Antifungal Agents metabolism, Carbonic Anhydrase Inhibitors chemical synthesis, Carbonic Anhydrase Inhibitors metabolism, Carbonic Anhydrases classification, Carbonic Anhydrases metabolism, Humans, Kinetics, Molecular Sequence Data, Phylogeny, Protein Binding, Sequence Alignment, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides metabolism, Sulfonic Acids chemical synthesis, Sulfonic Acids metabolism, Antifungal Agents chemistry, Candida glabrata enzymology, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases chemistry, Sulfonamides chemistry, Sulfonic Acids chemistry

Abstract

The fungal pathogen Candida glabrata encodes for a β-carbonic anhydrase (CA, EC 4.2.1.1), CgNce103, recently discovered. Only anions have been investigated as CgNce103 inhibitors up until now. Here we report the first sulfonamides inhibition study of this enzyme. Simple sulfonamides showed weak or moderate CgNce103 inhibitory properties, whereas acetazolamide, and a series of 4-substituted ureido-benzene-sulfonamides, sulfamates and sulfamides showed effective CgNce103 inhibitory properties, with KIs in the range of 4.1-115 nM, being also ineffective as human CA II inhibitors. As there is significant resistance of C. glabrata clinical isolates to many classical antifungal agents, inhibition of the β-CA from this organism may allow an interesting means of controlling the pathogen growth, eventually leading to antifungals with a novel mechanism of action., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

95. o-Benzenedisulfonimido-sulfonamides are potent inhibitors of the tumor-associated carbonic anhydrase isoforms CA IX and CA XII.

Author

Güzel-Akdemir Ö, Akdemir A, Isik S, Vullo D, and Supuran CT

Subjects

Acetazolamide chemistry, Acetazolamide metabolism, Antigens, Neoplasm metabolism, Binding Sites, Carbonic Anhydrase IX, Carbonic Anhydrase Inhibitors chemical synthesis, Carbonic Anhydrase Inhibitors metabolism, Carbonic Anhydrases metabolism, Catalytic Domain, Humans, Kinetics, Molecular Docking Simulation, Protein Binding, Sulfonamides chemical synthesis, Sulfonamides metabolism, Antigens, Neoplasm chemistry, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases chemistry, Imides chemistry, Sulfonamides chemistry

Abstract

By using phthalimido-substituted aromatic sufonamides as lead molecules, a series of new sulfonamides incorporating ortho-benzenedisulfonimide moieties have been synthesized and tested against the human (h) cytosolic carbonic anhydrase (CA, EC 4.2.1.1) isozymes hCA I and hCA II and the transmembrane, tumor-associated isozymes hCA IX and hCA XII. All these compounds showed Ki values lower than 100nM and many of them showed better Kis than the reference compound acetazolamide, a clinically used sulfonamide. The tumor-associated isozymes were better inhibited than the cytosolic ones. A molecular docking within the active site of some CA isoforms, such as hCA I, explained these findings, as the benzenedisulfonimide moiety makes favorable interactions (hydrogen bonds) with amino acid residues involved in binding of inhibitors, such as Gln92, His67, and His64., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2013

96. Synthesis and characterisation of novel Co(II) complexes of pyrazole carboxylate derivated of sulfonamide as carbonic anhydrase inhibitors.

Author

Büyükkidan N, Büyükkidan B, Bülbül M, Kasimoğullari R, Serdar M, and Mert S

Subjects

Acetazolamide chemistry, Carbonic Anhydrase I antagonists & inhibitors, Carbonic Anhydrase I metabolism, Carbonic Anhydrase II antagonists & inhibitors, Carbonic Anhydrase II metabolism, Carbonic Anhydrase Inhibitors chemical synthesis, Cations, Divalent chemistry, Coordination Complexes chemical synthesis, Erythrocytes metabolism, Humans, Isoenzymes antagonists & inhibitors, Ligands, Sulfonamides chemical synthesis, Carbonic Anhydrase Inhibitors chemistry, Cobalt chemistry, Coordination Complexes chemistry, Pyrazoles chemistry, Sulfonamides chemistry

Abstract

Objectives: Two new metal complexes, diaquabis(4-benzoyl-1,5-diphenyl-N-(5-sulfamoyl-1,3,4-thiadiazol-2-yl)-1H-pyrazole-3-carboxamide)cobalt(II) dihydrate (2) and diaquabis(ethyl-1-(3-nitrophenyl)-5-phenyl-3-(5-sulfamoyl-1,3,4-thiadiazol-2-ylcarbamoyl)-1H-pyrazole-4-carboxylate)cobalt(II) monohydrate (4), containing sulfonamide have been synthesized by the reaction of Co(II) with 4-benzoyl-1,5-diphenyl-N-(5-sulfamoyl-1,3,4-thiadiazol-2-yl)-1H-pyrazole-3-carboxamide (1) and ethyl-1-(3-nitrophenyl)-5-phenyl-3-(5-sulfamoyl-1,3,4-thiadiazol-2-ylcarbamoyl)-1H-pyrazole-4-carboxylate (3), respectively., Methods: The structures of Co(II) complexes 2 and 4 have been characterised by spectroscopic methods and elemental analyses. Human carbonic anhydrase isoenzymes (hCA-I and hCA-II) were purified from erythrocyte cells by affinity chromatography. The inhibitory effects of ligands 3 and 4, acetazolamide as a control compound and the newly synthesized complexes on the activity of hydratase and esterase of these isoenzymes have been studied in vitro., Key Findings: The concentration of compounds 2 and 4 producing a 50% inhibition of hydratase activity (IC(50) values) were 0.473 ± 0.025 and 0.065 ± 0.002 μm for hCA-I and 0.213 ± 0.015 and 0.833 ± 0.021 μm for hCA-II, respectively. The IC(50) values of synthesized compounds 2 and 4 for esterase activity were, 0.058 ± 0.006 and 0.297 ± 0.015 μm for hCA-I and 0.110 ± 0.010 and 0.052 ± 0.002 μm for hCA-II, respectively. In relation to esterase activity, the inhibition equilibrium constants (K(i) ) were determined as 0.039 ± 0.004 and 0.247 ± 0.035 μm on hCA-I and 0.078 ± 0.002 and 0.363 ± 0.015 μm on hCA-II for 2 and 4, respectively., Conclusions: The synthesized compounds 2 and 4 had effective inhibitory activity (P < 0.0001) on hCA-I and hCA-II than the corresponding free ligands, 1 and 3, and acetazolamide. Compounds 2 and 4 might be considered as potential inhibitors., (© 2012 The Authors. JPP © 2012. Royal Pharmaceutical Society.)

Published

2013

97. Preparation and evaluation of sustained release calcium alginate beads and matrix tablets of acetazolamide.

Author

Barzegar-Jalali M, Hanaee J, Omidi Y, Ghanbarzadeh S, Ziaee S, Bairami-Atashgah R, and Adibkia K

Subjects

Acetazolamide chemistry, Alginates chemistry, Delayed-Action Preparations, Glucuronic Acid administration & dosage, Glucuronic Acid chemistry, Hexuronic Acids administration & dosage, Hexuronic Acids chemistry, Solubility, Tablets, Acetazolamide administration & dosage, Alginates administration & dosage

Abstract

The aim of this study was to develop sustained release dosage forms of acetazolamide (ACZ) preparing its calcium alginate beads and matrix tablets. ACZ was incorporated into calcium alginate beads using microencapsulation method. Two methods were applied to prolong ACZ release rate. In the first method, the drug was incorporated into calcium alginate beads either alone or with various polymers in internal phase. The second method involved the preparation of matrix tablet from the beads benefiting direct compression method with or without various polymers in external phase. The release rate of these prepared formulations and an innovator's sustained-release capsule (Diamox®) were assessed. In-vitro dissolution studies revealed that the matrix tablets prepared by the second method containing NaCMC could sustain ACZ release properly and the drug released until 9 h. It was also found that several parameters such as concentration of sodium alginate, calcium chloride and ACZ; type and concentration of polymers; syringe needle size as well as distance between needle tip and surface of the calcium chloride could affect the properties of beads, matrix tablets and subsequently release profile. Preparation of polymer free beads, incorporation of polymers in internal phase of the beads and direct compression of the beads did not give sustained release property. Whereas, incorporation of NaCMC in the external phase of the beads in matrix tablets or in combination with alginate powder in directly compressed conventional tablets could produce dosage form with sustained release property similar to reference formulation., (© Georg Thieme Verlag KG Stuttgart · New York.)

Published

2013

98. Discovery of novel human aquaporin-1 blockers.

Author

Seeliger D, Zapater C, Krenc D, Haddoub R, Flitsch S, Beitz E, Cerdà J, and de Groot BL

Subjects

Acetazolamide chemistry, Acetazolamide pharmacology, Animals, Binding Sites, Humans, Models, Molecular, Xenopus, Aquaporin 1 antagonists & inhibitors, Drug Discovery, Molecular Dynamics Simulation

Abstract

Human aquaporin-1 (hAQP1) is a water channel found in many tissues and potentially involved in several human pathologies. Selective inhibitors of hAQP1 are discussed as novel treatment opportunities for glaucoma, brain edema, inflammatory pain, and certain types of cancer. However, only very few potent and chemically attractive blockers have been reported to date. In this study we present three novel hAQP1 blockers that have been identified by virtual screening and inhibit water flux through hAQP1 in Xenopus laevis oocyte swelling assays at low micromolar concentrations. The newly discovered compounds display no chemical similarity to hitherto known hAQP1 blockers and bind at the extracellular entrance of the channel, close to the ar/R selectivity filter. Furthermore, mutagenesis studies showed that Lys36, which is not conserved among the hAQP family, is crucially involved in binding and renders the discovered compounds suitable as leads for the development of selective hAQP1 inhibitors.

Published

2013

99. Intermolecular charge transfer and vibrational analysis of hydrogen bonding in acetazolamide.

Author

Chaturvedi D, Gupta V, Tandon P, Sharma A, Baraldi C, and Gamberini MC

Subjects

Hydrogen Bonding, Models, Molecular, Quantum Theory, Spectroscopy, Fourier Transform Infrared, Spectrum Analysis, Raman, Acetazolamide chemistry, Anticonvulsants chemistry, Carbonic Anhydrase Inhibitors chemistry

Abstract

In the present work the structural and spectral characteristics of acetazolamide have been studied by methods of infrared, Raman spectroscopy and quantum chemistry. Electrostatic potential surface, optimized geometry, harmonic vibrational frequencies, infrared intensities and activities of Raman scattering were calculated by density functional theory (DFT) employing B3LYP with complete relaxation in the potential energy surface using 6-311++G(d,p) basis set. Based on these results, we have discussed the correlation between the vibrational modes and the structure of the dimers of acetazolamide. The calculated vibrational spectra of three dimers of acetazolamide have been compared with observed spectra, and the assignment of observed bands was carried out using potential energy distribution. The observed spectra agree well with the values computed from the DFT. A comparison of observed and calculated vibrational spectra clearly shows the effect of hydrogen bonding. The frequency shifts observed for the different dimers are in accord with the hydrogen bonding in acetazolamide. Natural bond orbital (NBO) analyses reflect the charge transfer interaction in the individual hydrogen bond units and the stability of different dimers of acetazolamide., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

100. Structural, spectroscopic and voltammetric studies of bis(acetazolamido)bis(aquo)bis(nicotinamide)copper(II).

Author

Oztürk F, Bulut A, Paşaoğlu H, Bulut I, and Büyükgüngör O

Subjects

Acetazolamide chemistry, Crystallography, X-Ray, Electrodes, Electron Spin Resonance Spectroscopy, Hydrogen Bonding, Models, Molecular, Niacinamide chemistry, Spectrophotometry, Infrared, Stereoisomerism, Copper chemistry, Electrochemical Techniques methods, Organometallic Compounds chemistry

Abstract

Polymeric copper(II) complex, [Cu(Hacm)(2)(na)(2)(H(2)O)(2)] [H(2)acm; acetazolamide, na; nicotinamide] was synthesized and characterized by spectroscopic (IR; infrared spectroscopy, EPR; electron paramagnetic resonance), structural (XRD) and voltammetric structural (CV) methods. The copper(II) compound crystallizes in the triclinic space group P1¯, Z=1, with the unit-cell dimensions: a=7.672 (5)Å, b=8.681 (5)Å, c=11.938 (5)Å, α=90.807 (7)°, β=98.616 (5)° and γ=110.647 (5)°. The Cu(II) ion has a distorted octahedral coordination geometry. The crystal packing of the complex is stabilized by intermolecular O-H…O and N-H…O hydrogen bonds. The powder EPR spectrum of copper(II) complex have indicate that the paramagnetic center is in a tetragonal symmetry with the Cu(2+) ion having a distorted octahedral geometry. The vibrational investigation has been carried out on the basis of some characteristic IR bands of acetazolamide and nicotinamide molecules., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012