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Variants of cyclooxygenase-1 and their roles in medicine.

机译:环氧合酶-1的变体及其在医学中的作用。

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摘要

Acetaminophen (paracetamol) and other analgesic/antipyretic drugs such as dipyrone have been postulated to act centrally through inhibition of cyclooxygenases (COXs). COX activity in lipopolysaccharide-stimulated mammalian leukocytes, microglial cells, and platelets is inhibited by these drugs at physiological concentrations. Yet purified COX enzymes are poorly inhibited by acetaminophen, particularly under conditions of high oxidant tone and elevated substrate levels. This suggests the presence of cell-specific differences that govern COX inhibition by these drugs. COX-3, a variant of COX-1, has been found in canine brain and is inhibited by acetaminophen and dipyrone at physiological concentrations. Additionally, other new COX-1-derived proteins called PCOX have been identified that do not make prostaglandins but apparently bind heme and may have other enzymatic properties. Antibodies specific for these variants detect analogous proteins in human tissues. Expression of COX variants is postulated to be an integral part of the mechanism of action of analgesic/antipyretic drugs.
机译:对乙酰氨基酚(扑热息痛)和其他止痛/解热药(如双嘧达隆)已被假定通过抑制环氧合酶(COXs)起到集中作用。这些药物在生理浓度下会抑制脂多糖刺激的哺乳动物白细胞,小胶质细胞和血小板中的COX活性。然而,对乙酰氨基酚对纯化的COX酶的抑制作用较弱,特别是在高氧化剂色调和底物水平升高的条件下。这表明存在控制这些药物抑制COX的细胞特异性差异。 COX-3是COX-1的变体,已在犬脑中发现,并在生理浓度下被对乙酰氨基酚和双嘧啶抑制。此外,还发现了其他新的源自COX-1的蛋白,称为PCOX,它们不制造前列腺素,但显然与血红素结合,并可能具有其他酶促特性。这些变体特异的抗体可检测人体组织中的类似蛋白。假定COX变体的表达是止痛/解热药作用机制的组成部分。

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