Rofecoxib definition of rofecoxib by the free dictionary. A quantitative structureactivity relationship study of. Quantitative structure activity relationships studies of. The 3d structure of cyclooxygenase enzyme cox2 was downloaded from protein data bank. We have performed the quantitative structure activity relationship qsar study for n1. The daily telegraph reported that powerful painkillers used by thousands of arthritis sufferers almost double the chance of a patient suffering a heart attack and stroke. Rofecoxib is a potent, specific and orally active cox2 inhibitor, with ic 50 s of 26 and 18 nm for human cox2 in human osteosarcoma cells and chinese hamster ovary cells, with a fold selectivity for cox2 over human cox1 ic 50 50.
Qsars are mathematical models used to predict measures of toxicity from the physical characteristics of the structure of chemicals known as molecular. Apoptolidin a is a macrolide known to be cytotoxic to specific cancerous cell lines and therefore is of interest as a therapeutic lead. It is known that the so2nhcoch3 moiety is a 10 5106 more reactive. Structureactivity relationship of celecoxib and rofecoxib for. The toxicity estimation software tool test was developed to allow users to easily estimate the toxicity of chemicals using quantitative structure activity relationships qsars methodologies. Rofecoxib is also an effective analgesic in patients with primary dysmenorrhoea or postoperative dental pain and demonstrates similar analgesic efficacy to that of naproxen sodium and ibuprofen. Structurefunctional relationship of prodigiosin and cycloprodigiosin was evaluated to know their biological activity against the cox2 using the 3d structure of the receptor retrieved from protein data bank site of cox2 enzyme pdb code. One group at eli lilly used a traditional hts to identify a lead compound that was subsequently improved by examination of structureactivity relationship using in vitro assays sawyer et al. To understand the membrane permeabilizing activity of coxibs in terms of their structure activity relationship, we separated the structures of celecoxib and rofecoxib into three parts, synthesized hybrid compounds by substitution of each of the parts, and examined the membrane permeabilizing activities of these hybrids. In the present investigation, molecular docking studies were performed for both prodigiosin and cycloprodigiosins to evaluate the in silico antiinflammatory activity against cycloxigenase2 cox2 protein as model compound and the data compared with rofecoxib. The results of the assessment were summarized in the following table as extracted from the study report.
Quantitative structure activity relationships studies of nonsteroidal antiinflammatory drugs. Quantitative structure activity relationships qsar is a useful mean which maximizes the. Prostaglandins are chemicals that are important in promoting inflammation and its signspain, fever, swelling and tenderness. Twodimensionalquantitative structureactivity relationship studies. Rofecoxib has greater selectivity for cox2 than celecoxib, meloxicam, diclofenac and indomethacin. In silico molecular docking analysis of prodigiosin and. Merck announced a voluntary worldwide withdrawal of vioxx rofecoxib 2.
The 3d structure was generated in mol2 with open babel software, minimized, and optimized with cresset flare software. The relationship of the cardiovascular findings to the use of rofecoxib is not known. The molecular modeling studies were performed using cs chem. Structure activity relationship sar analysis software programs, such as oncologic and multicase mcase, work by analyzing the chemical structure of a compound of unknown toxicity and predicting its likelihood to be a carcinogen based on comparisons to the structures of compounds with known toxicity and programmed chemical and.
Rofecoxib is a nonsteroidal antiinflammatory drug that is used to treat pain, particularly the pain of osteoarthritis and menstrual cramps. The high expression of the multiresistance protein 4 in patients with transitory aspirin resistance, points to the importance of finding new molecules, including those that are not affected by these proteins. Structureactivity relationship studies suggested that nphenyl ring substituted with pcf 3 substituent 3b, 3k and 3q leads to more selective inhibition of cox2. Research open access silico molecular docking analysis of.
Rofecoxib binds to and inhibits the enzyme cyclooxygenase2 cox2, resulting in an inhibition of the conversion of arachidonic acid to prostaglandins. Structure activity relationship sar is an approach to find qualitative relationships between chemical structure and their biological activity quantitative structure activity relationship qsar models are theoretical models that relate a. To understand the membrane permeabilizing activity of coxibs in terms of their structureactivity relationship, we separated the structures of. The activity of many natural products is elucidated by structure activity relationship studies where portions of the molecule are modified and the resulting changes in bioactivity are noted. Previously marketed drugs such as celecoxib, rofecoxib, and etodolac act. Users can perform simple and advanced searches based on annotations relating to sequence, structure and function. A quantitative structure activity relationship qsar study of 3, 4diaryloxazolones has been performed to evaluate the descriptors responsible for the cox2 inhibitory activity of the molecules. Structureactivity relationship of celecoxib and rofecoxib. Extensive structureactivity relationship sar studies for the diarylheterocyclic class of compounds have shown that a so2nh2, or a so2me, substituent at the paraposition of one of the aryl rings is a requirement for optimum cox2 selectivity and potency 8. While rofecoxib contains a methyl sulfone constituent, celecoxib and valdecoxib possess an unsubstituted arylsulfonamide moiety. Quantitative structureactivity relationship qsar searches information. Structureactivity relationship qsar analysis was performed on the cox2.
Discovery and development of cyclooxygenase 2 inhibitors. Classification of scaffoldhopping approaches bhsai. Synthesis, antiinflammatory activity, and in silico study. The content on this site is presented in a summary fashion, and is intended to be used for educational and entertainment purposes only. Over the last 60 years there have been a multitude of ways to capture structureactivity relationships. Toxicity estimation software tool test safer chemicals. Design, synthesis and structureactivity relationship studies of novel. Rofecoxib should be used with caution in patients with fluid retention, hypertension or heart failure as fluid retention and edema has been observed in some patients. The chemical name is 44methylsulfonylphenyl3phenyl25hfuranone. The newspaper reports that the cox2 inhibitor vioxx was withdrawn in 2004 after a study showed that it doubled the risk of heart attacks.
Some epithelial tumor cell types overexpress proangiogenic cox2. If the target structure is known, computational chemistry and molecular modelling software packages can be useful in identifying binding site interactions. Covalent binding of rofecoxib, but not other cyclooxygenase2. To understand the membrane permeabilizing activity of coxibs in terms of their structureactivity relationship, we separated the structures of celecoxib and rofecoxib into three parts, synthesized hybrid compounds by substitution of each of the parts, and examined the. Rofecoxib is a selective cyclooxygenase cox2 inhibitor which has little or no effect on the cox1 isoenzyme at doses up to mgday. The rcsb pdb also provides a variety of tools and resources. The regions with carbonyl carbons that have the structure activity relationship are marked with red circles. Deletion of the so2ch3 group of rofecoxib switches the compound from a cox2 to a cox1selective inhibitor, providing a 3,4diarylfuran25hone scaffold for structureactivity relationship. Structure activity relationships sar can be used to predict biological activity from molecular structure. Quantitative data and detailed annnotation of the targets of licensed and experimental drugs. Rofecoxib was approved as safe and effective by the food and drug administration fda on may 20, 1999 and was subsequently marketed under the brand name vioxx, ceoxx and ceeoxx. A series of novel cox2seh dual inhibitors were rationally designed and synthesized to provide the basis for a structureactivity relationship sar study. In silico and in vitro proteasome inhibition by curcumin. Structure activity relationship sar studies for diaryl.
Computational methods in drug discovery pubmed central pmc. Rofecoxib is a nonsteroidal antiinflammatory drug nsaid that selectively inhibits cyclooxgenase2 cox2, which was used in the therapy of chronic arthritis and mildtomoderate musculoskeletal pain. Quantitative structure activity relationships studies of nonsteroidal. We can broadly divide them into two groups those based on statistical or data mining methods e. Patients being treated for rheumatoid arthritis with rofecoxib at a dose of 25 mg a day have been reported to have a higher incidence of hypertension compared to patients treated with naproxen at a dose of mg a day. Cox2 inhibitors within the last two decades, the volume of literature on the structural types introduced as selective cox2 inhibitors is enormous. Synthesis and structureactivity relationship studies of. Rofecoxib was withdrawn in 2004 because of an association with an increase in cardiovascular events with its long term use. Rofecoxib was approved in the us by the us food and drug administration fda in may 1999, and was marketed under the brand names vioxx, ceoxx, and ceeoxx. It is not intended to be and should not be interpreted as medical advice or a diagnosis of any health or fitness problem, condition or disease. Quantitative structureactivity relationship based modeling of.
The empirical formula for rofecoxib is c 17 h 14 o 4 s, and it has the following chemical structure. Evaluation of three stateoftheart metabolite prediction software packages meteor, metasite, and stardrop through independent and synergistic use. Rofecoxib is a cox2 selective nonsteroidal antiinflammatory drug. As a member of the wwpdb, the rcsb pdb curates and annotates pdb data according to agreed upon standards. Kellog 1996, the use of less expensive software which is available in our group. This powerful technology is used in drug discovery to guide the acquisition or synthesis of desirable new compounds, as well as to further. Prodigiosin and cycloprodigiosin are tripyrrole red pigmented compounds with medical importance for their anticancer property. New carboxamide derivatives bearing benzenesulphonamide as.
E software measurement of light emission from the 1483. These molecules are visualized, downloaded, and analyzed by users who range from students to specialized scientists. Structure of selective cox2 inhibitor celecoxib 1 and rofecoxib 2, target compounds 712, 1625, 28, 29, 32, and 33 and illustration of in situ click chemistry reaction principle inside. Synthesis, biological activity, and molecular modeling. The rcaresearch cooperative agreement with fdamethod expert analysis is a protocol currently used to perform. Structureactivity relationship sar data were supported with predicted binding data, retrieved by molecular docking studies with human cox1 pdb code 3kk6 and human cox2 pdb code 5kir. Rofecoxib blocks the enzyme that makes prostaglandins cyclooxygenase 2 and thereby reduces the amounts of prostaglandins.
Rofecoxib should not be given to patients who have experienced asthma, urticaria, or allergictype reactions after taking aspirin or other nonsteroidal antiinflammatories. In this work, we describe the synthesis and biological. One compound 7c showed more potent antiinflammatory activity than celecoxib at 3 h in carrageenaninduced rat paw edema bioassay. Structurebased discovery of mpges1 inhibitors suitable for preclinical testing in wildtype mice as a new generation of antiinflammatory drugs. Deletion of the so2ch3 group of rofecoxib switches the compound from a cox2 to a cox1selective inhibitor, providing a 3,4diarylfuran25hone scaffold for structure activity relationship. Structurebased discovery of mpges1 inhibitors suitable. New analogues of hydroxyocatdecadienoic acid and 12. Structure activity relationships sar explore the relationship between a molecules biological activity and the three dimensional structure of the molecule. A quantitative structureactivity relationship study of novel inhibitors of cyclooxygenase2. Quantitative structureactivity relationship qsar study of. Unexpected nanomolar inhibition of carbonic anhydrase by. In this study, design, synthesis and structureactivity relationship. Design and synthesis of new rofecoxib analogs as selective. Coxrelated metabolic pathways may represent key regulators of cell proliferation and neoangiogenesis.
For this the docked binding mode was established to link the docking scoring func. Finally, the invention also provides methods of developing and identifying enhanced pin1targeted atrarelated compounds based on the newly defined unique binding pockets in the pin1 active site revealed from the cocrystal structure, structureactivity relationship, and structural modeling. Sixteen new carboxamide derivatives bearing substituted benzenesulphonamide moiety 7ap were synthesized by boric acid mediated amidation of appropriate benzenesulphonamide with 2amino4picoline and tested for antiinflammatory activity. In situ click chemistry generation of cyclooxygenase2. We synthesized 10 compounds based on the structures of analogues of 12hydroxyeicosatetraenoic acid and hydroxyocatdecadienoic acid and evaluated their effect on platelet aggregation triggered by arachidonic acid. Design, synthesis, and structureactivity relationship studies of. The incidence of hematological disorders has increased steadily in western countries despite the advances in drug development. Quantitative structureactivity relationship based modeling of substituted indole schiff bases.
The findings obtained by molecular modeling study support the sar data and binding similarities and differences on both isozymes. The compounds synthesized as dmls demonstrate significant inhibition to both cox2 selectively and seh. The chemical structure of compounds was drawn via marven sketch software version 18. Curcumin inhibits the proteasome activity in human colon. The 5aryl2,2dialkyl4phenyl32 hfuranone derivatives, p singh, manju shekhawat. An assisting software in structure based drug design using fingerprint of proteinligand interaction profiles. Synthesis and antiplatelet activity of antithrombotic. Structure activity relationship sar dup697 was a buildingblock for synthesis of cox2 inhibitors and served as the basic chemical model for the coxibs that are the only selective cox2 inhibitors on the market today. To corroborate obtained experimental biological data, molecular docking study was carried out which revealed that compound 3b showed stronger binding interaction with cox2 as. Rofecoxib is a nonsteroidal antiinflammatory drug that was used in the treatment of osteoarthritis, acute pain conditions, and dysmenorrhoea. B, molecular orbital energy analysis is shown by drawing and electron density isosurface and coloring by nucleophilic susceptibility.
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