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动脉壁从前列腺素内过氧化物生成一种物质(前列腺素X),该物质可使肠系膜动脉和腹腔动脉条松弛,并抑制血小板聚集。

Arterial walls generate from prostaglandin endoperoxides a substance (prostaglandin X) which relaxes strips of mesenteric and coeliac ateries and inhibits platelet aggregation.

作者信息

Bunting S, Gryglewski R, Moncada S, Vane J R

出版信息

Prostaglandins. 1976 Dec;12(6):897-913. doi: 10.1016/0090-6980(76)90125-8.

Abstract

Fresh arterial tissue generates an unstable substance (prostablandin X) which relaxes vascular smooth muscle and potently inhibits platelet aggregation. The release of prostaglandin (PG) X can be stimulated by incubation with arachidonic acid or prostaglandin endoperoxides PGG2 or PGH2. The basal release of PGX or the release stimulated with arachidonic acid can be inhibited by previous treatment with indomethacin or by washing the tissue with a solution containing indomethacin. The formation of PGX from prostaglandin endoperoxides PGG2 or PGH2 is not inhibited by indomethacin. 15-hydroperoxy arachidonic acid (15-HPAA) inhibits the basal release of PGX as well as the release stimulated by arachidonic acid or prostaglandin endoperoxides (PGG2 or PGH2). Fresh arterial tissue obtained from control or indomethacin treated rabbits, when incubated with platelet rich plasma (PRP) generates PGX. This generation is inhibited by treating the tissue with 15-HPAA. A biochemical interaction between platelets and vessel wall is postulated by which platelets feed the vessel wall with prostaglandin endoperoxides which are utilized to form PGX. Formation of PGX could be the underlying mechanism which actively prevents, under normal conditions, the accumulation of platelets on the vessel wall.

摘要

新鲜动脉组织会产生一种不稳定物质(前列腺素X),它能使血管平滑肌松弛,并有效抑制血小板聚集。通过与花生四烯酸或前列腺素内过氧化物PGG2或PGH2孵育可刺激前列腺素(PG)X的释放。PGX的基础释放或由花生四烯酸刺激引起的释放可被吲哚美辛预处理或用含吲哚美辛的溶液冲洗组织所抑制。吲哚美辛不会抑制由前列腺素内过氧化物PGG2或PGH2形成PGX。15 - 氢过氧花生四烯酸(15 - HPAA)会抑制PGX的基础释放以及由花生四烯酸或前列腺素内过氧化物(PGG2或PGH2)刺激引起的释放。从对照兔或经吲哚美辛处理的兔获得的新鲜动脉组织,与富含血小板血浆(PRP)一起孵育时会产生PGX。用15 - HPAA处理组织会抑制这种产生。推测血小板与血管壁之间存在生化相互作用,通过这种相互作用血小板为血管壁提供前列腺素内过氧化物,这些内过氧化物被用于形成PGX。PGX的形成可能是在正常情况下积极防止血小板在血管壁上积聚的潜在机制。

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