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Design Synthesis and Study of Nitrogen Monoxide Donors as Potent Hypolipidaemic and Anti-Inflammatory Agents

机译:一氧化氮供体作为高效降血脂和抗炎药的设计合成和研究

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摘要

Inflammation and oxidative stress are involved in cardiovascular diseases. Nitrogen monoxide participates in the regulation of endothelial processes. Thus, derivatives of classic nonsteroidal anti-inflammatory drugs (NSAIDs), trolox or cinnamic acids esterified with 2-(nitrooxy)ethanol were designed and studied. It was found that the nitrogen monoxide (NO) releasing activity was comparable to that of -nitroso- -acetylpenicillamine. The nitrooxy derivatives decreased potently lipid indices in the plasma of hyperlipidaemic rats (30–85%). All compounds presented increased anti-inflammatory activity in vivo, inhibiting carrageenan-induced rat paw oedema as high as 76%, up to six times higher than that of the parent acids. Lipoxygenase inhibitory activity was significant for most of them, although the parent molecules exerted a minor effect (IC > 0.2 mM). Those compounds incorporating an antioxidant structure inhibited rat microsomal membrane lipid peroxidation strongly and possessed radical scavenging activity. These results indicated that the described compounds could act at different targets in multifactorial diseases, further limiting the possible adverse effects of drug combinations.
机译:炎症和氧化应激与心血管疾病有关。一氧化氮参与内皮过程的调节。因此,设计并研究了经典的非甾体类抗炎药(NSAID),trolox或肉桂酸被2-(硝基氧基)乙醇酯化的衍生物。发现一氧化氮(NO)的释放活性与-亚硝基-乙酰青霉胺的释放活性相当。硝基氧衍生物可有效降低高脂血症大鼠血浆中的脂质指数(30-85%)。所有化合物在体内均具有增强的抗炎活性,抑制角叉菜胶诱导的大鼠爪水肿高达76%,是母体酸的六倍。尽管母体分子发挥的作用较小(IC> 0.2 mM),但大多数脂氧合酶的抑制活性都很显着。那些具有抗氧化剂结构的化合物强烈抑制大鼠微粒体膜脂质过氧化并具有自由基清除活性。这些结果表明,所描述的化合物可以在多因素疾病中作用于不同的靶标,进一步限制了药物组合的可能的不良作用。

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