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Cyclooxygenase isozymes: the biology of prostaglandin synthesis and inhibition.

机译:环氧合酶同工酶:前列腺素的合成和抑制生物学。

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Nonsteroidal anti-inflammatory drugs (NSAIDs) represent one of the most highly utilized classes of pharmaceutical agents in medicine. All NSAIDs act through inhibiting prostaglandin synthesis, a catalytic activity possessed by two distinct cyclooxygenase (COX) isozymes encoded by separate genes. The discovery of COX-2 launched a new era in NSAID pharmacology, resulting in the synthesis, marketing, and widespread use of COX-2 selective drugs. These pharmaceutical agents have quickly become established as important therapeutic medications with potentially fewer side effects than traditional NSAIDs. Additionally, characterization of the two COX isozymes is allowing the discrimination of the roles each play in physiological processes such as homeostatic maintenance of the gastrointestinal tract, renal function, blood clotting, embryonic implantation, parturition, pain, and fever. Of particular importance has been the investigation of COX-1 and -2 isozymic functions in cancer, dysregulation of inflammation,and Alzheimer's disease. More recently, additional heterogeneity in COX-related proteins has been described, with the finding of variants of COX-1 and COX-2 enzymes. These variants may function in tissue-specific physiological and pathophysiological processes and may represent important new targets for drug therapy.
机译:非甾体抗炎药(NSAIDs)代表了医学上使用最广泛的药物类别之一。所有的NSAID都通过抑制前列腺素的合成而发挥作用,前列腺素的合成是由分别的基因编码的两种不同的环氧合酶(COX)同工酶所具有的催化活性。 COX-2的发现开启了NSAID药理学的新纪元,从而导致了COX-2选择性药物的合成,销售和广泛使用。这些药物已迅速确立为重要的治疗药物,其副作用可能比传统的NSAID少。此外,两种COX同工酶的特征允许区分各自在生理过程中所扮演的角色,例如胃肠道的稳态维持,肾功能,凝血,胚胎着床,分娩,疼痛和发烧。特别重要的是研究COX-1和-2同工酶在癌症,炎症失调和阿尔茨海默氏病中的功能。最近,随着发现COX-1和COX-2酶的变异,已经描述了COX相关蛋白中的其他异质性。这些变体可以在组织特异性的生理和病理生理过程中起作用,并且可以代表药物治疗的重要新靶标。

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