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肾上腺素对其他激动剂诱导的猕猴血小板聚集的增强作用:对人类动脉粥样硬化研究的启示。

Potentiation with epinephrine of macaque platelet aggregation by other agonists: implications for studies on human atherosclerosis.

作者信息

Beatty C H, Howard C F, Caruso V

出版信息

Thromb Res. 1986 Feb 15;41(4):447-58. doi: 10.1016/0049-3848(86)91690-7.

Abstract

The effects of low concentrations of epinephrine on the aggregation of macaque and human platelets by arachidonic acid (AA), collagen, and thrombin were studied. When epinephrine (0.05 to 1 microM) was added to macaque or human citrated or macaque heparinized platelets, either before or after the addition of near-threshold concentrations of AA, significant increases in aggregability were always seen. Epinephrine alone did not aggregate macaque platelets from citrated blood. When near-threshold concentrations of collagen or thrombin were present in the medium, low concentrations of epinephrine (0.05 to 0.50 microM) potentiated the aggregation of macaque and human citrated platelets and macaque heparinized platelets. The P values for the addition of epinephrine were less than 0.01 in all series. The ability of low epinephrine concentrations to potentiate aggregation of macaque platelets by other agonists is of particular significance because in humans the most important effect of epinephrine on platelets in vivo is probably the potentiation, by low concentrations, of aggregation induced by other aggregatory agents normally present in the blood in low concentrations.

摘要

研究了低浓度肾上腺素对花生四烯酸(AA)、胶原蛋白和凝血酶诱导的猕猴和人血小板聚集的影响。当在加入接近阈值浓度的AA之前或之后,将肾上腺素(0.05至1微摩尔)添加到猕猴或人的枸橼酸化血小板或猕猴肝素化血小板中时,总能观察到聚集性显著增加。单独的肾上腺素不会使枸橼酸血中的猕猴血小板聚集。当培养基中存在接近阈值浓度的胶原蛋白或凝血酶时,低浓度的肾上腺素(0.05至0.50微摩尔)会增强猕猴和人枸橼酸化血小板以及猕猴肝素化血小板的聚集。在所有系列中,添加肾上腺素的P值均小于0.01。低浓度肾上腺素增强其他激动剂诱导猕猴血小板聚集的能力具有特别重要的意义,因为在人类体内,肾上腺素对血小板最重要的作用可能是低浓度时增强血液中通常以低浓度存在的其他聚集剂诱导的聚集。

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