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首页> 外文期刊>Medicinal chemistry >Design, synthesis and biological screening of some pyridinylpyrazole and pyridinylisoxazole derivatives as potential anti-inflammatory, analgesic, antipyretic and antimicrobial agents
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Design, synthesis and biological screening of some pyridinylpyrazole and pyridinylisoxazole derivatives as potential anti-inflammatory, analgesic, antipyretic and antimicrobial agents

机译:设计,合成和生物筛选一些潜在的消炎,镇痛,解热和抗菌剂的吡啶基吡唑和吡啶基异恶唑衍生物

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摘要

A series of substituted pyridinylpyrazole (or isoxazole) derivatives was synthesized and evaluated for their antiinflammatory (AI) activity using formalin-induced paw edema bioassays. The inhibitory activities of cyclooxygenase-1 and cyclooxygenase-2 (COX-1 and COX-2) were also determined. The analgesic activity of the same compounds was evaluated using rat-tail withdrawal technique. Their antipyretic activity was also evaluated. The results revealed that compounds 4a,b, 6a, 8a, 14c and 15a exhibited significant AI and analgesic activities. Compounds 5a, 6a and 8a displayed good antipyretic activity. Compounds 14c and 15a showed good COX-2 inhibitory activity and weak inhibition of COX- 1. Additionally, the most active compounds were shown to have a large safety margin (ALD50 300-400 mg/Kg) and minimal ulcerogenic potentialities when administered orally at a dose of 300 mg/Kg. Docking studies for 14c and 15a with COX-2 showed good binding profile. Antimicrobial evaluation proved that most of the compounds exhibited distinctive activity against the gram negative bacteria, P. aeruginosa and E coli.
机译:合成了一系列取代的吡啶基吡唑(或异恶唑)衍生物,并使用福尔马林诱导的爪水肿生物测定法评估了它们的抗炎(AI)活性。还确定了环氧合酶-1和环氧合酶-2(COX-1和COX-2)的抑制活性。使用鼠尾戒断技术评估相同化合物的镇痛活性。还评估了它们的解热活性。结果表明,化合物4a,b,6a,8a,14c和15a表现出显着的AI和止痛活性。化合物5a,6a和8a显示出良好的解热活性。化合物14c和15a表现出良好的COX-2抑制活性和对COX-1的弱抑制。此外,口服给药时,活性最高的化合物显示出较大的安全裕度(ALD50> 300-400 mg / Kg)和极小的致溃疡性潜力剂量为300 mg / Kg。用COX-2对14c和15a的对接研究显示出良好的结合特性。抗菌评估证明,大多数化合物对革兰氏阴性菌,铜绿假单胞菌和大肠杆菌均表现出独特的活性。

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