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血管细胞的跨细胞硫肽白三烯生物合成能力。

Transcellular sulfidopeptide leukotriene biosynthetic capacity of vascular cells.

作者信息

Maclouf J, Murphy R C, Henson P M

机构信息

Department of Pharmacology, University of Colorado Health Sciences Center, Denver 80262.

出版信息

Blood. 1989 Aug 1;74(2):703-7.

PMID:2546629
Abstract

Cells in the vasculature, including polymorphonuclear leukocytes, platelets, and endothelial cells, have been shown to be jointly involved in the biosynthesis of active lipid mediators derived from arachidonic acid. Stimulation of neutrophils with the calcium ionophore A23187 as a model for cell activation results in production of leukotriene (LT)A4 with subsequent intracellular conversion into LTB4. When platelets or endothelial cells were present in the incubation system, LTC4 was produced from the neutrophil-derived LTA4. Whereas production and release of LTA4 under resting conditions in vivo might be expected to be quite low, under pathologic conditions, LTA4 production could be markedly increased. Therefore, the metabolism of exogenous LTA4 by platelets and endothelial cells was studied at a wide range of LTA4 concentrations. The production of LTC4 during coincubation of neutrophils with platelets was found to be dependent on neutrophil number ranging from 2 x 10(5) to 2 x 10(7) cells/mL. When a fixed number of neutrophils were stimulated with platelets alone or with mixtures of platelets and endothelial cells, LTC4 production was observed to be dependent on both acceptor cell types. These results suggest that mixed cell populations, which are likely to occur in vivo, may be critical determinants of the profile of eicosanoids produced in pathophysiologic circumstances. We suggest that both endothelial cells and platelets, in the presence of neutrophils, contribute large quantities of sulfidopeptide leukotrienes to inflammatory and thrombotic situations. Furthermore, platelets, because of their quantity and reactivity, may play a pivotal role in transcellular biosynthesis of eicosanoids.

摘要

脉管系统中的细胞,包括多形核白细胞、血小板和内皮细胞,已被证明共同参与源自花生四烯酸的活性脂质介质的生物合成。用钙离子载体A23187刺激中性粒细胞作为细胞活化模型,会导致白三烯(LT)A4的产生,随后在细胞内转化为LTB4。当血小板或内皮细胞存在于孵育系统中时,中性粒细胞衍生的LTA4会生成LTC4。虽然在体内静息条件下LTA4的产生和释放可能相当低,但在病理条件下,LTA4的产生可能会显著增加。因此,研究了血小板和内皮细胞在广泛的LTA4浓度下对外源性LTA4的代谢。发现中性粒细胞与血小板共孵育期间LTC4的产生取决于中性粒细胞数量,范围为2×10⁵至2×10⁷个细胞/毫升。当用单独的血小板或血小板与内皮细胞的混合物刺激固定数量的中性粒细胞时,观察到LTC4的产生取决于两种受体细胞类型。这些结果表明,体内可能出现的混合细胞群体可能是病理生理情况下类花生酸产生情况的关键决定因素。我们认为,在内皮细胞和血小板存在的情况下,中性粒细胞会在炎症和血栓形成情况下产生大量的硫肽白三烯。此外,由于血小板的数量和反应性,它们可能在类花生酸的跨细胞生物合成中起关键作用。

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