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天然和去唾液酸α-1酸性糖蛋白对血小板聚集的抑制作用。

Inhibition of platelet aggregation by native and desialised alpha-1 acid glycoprotein.

作者信息

Costello M, Fiedel B A, Gewurz H

出版信息

Nature. 1979 Oct 25;281(5733):677-8. doi: 10.1038/281677a0.

Abstract

The alpha-1 acid glycoprotein (orosomucoid; AAG) is a normal constituent of human plasma (650+/-215 microgram ml(-1)) which increases in concentration as much as fivefold in associations with acute inflammation and cancer, and thus is recognized as an acute phase protein. AAG consists of a single polypeptide chain, has a molecular weight of 44,100, and contains approximately 45% carbohydrate including 12% sialic acid; it is the most negatively charged of the plasma proteins. Certain of the biological properties of AAG are related to its sialic acid content; thus, clearance and immunogenicity of AAG are markedly increased on desialisation. The biological functions of AAG are largely unknown. AAG has the ability to inhibit certain lymphocyte re-activities including blastogenesis in response to concanavalin A, phytohaemagglutinin and allogeneic cells, and these inhibitory effects are enhanced in association with desialisation. In view of these observations, a report that unphysiologically large (5--15 mg ml(-1)) amounts of AAG inhibit the platelet aggregation induced by ADP and adrenaline, and evidence that a sialic acid-deficient species of AAG appears elevated in several chronic disease states, we compared the effects of AAG and its desialised counterpart (AAG-D) on platelet aggregation. We report that desialisation of AAG is associated with increased expression of activity inhibitory to the platelet aggregation otherwise observed on stimulation with ADP, collagen or thrombin.

摘要

α-1酸性糖蛋白(orosomucoid;AAG)是人体血浆的正常成分(650±215微克/毫升),在急性炎症和癌症时其浓度可增加至五倍之多,因此被视为一种急性期蛋白。AAG由一条多肽链组成,分子量为44,100,含有约45%的碳水化合物,其中包括12%的唾液酸;它是血浆蛋白中带负电荷最多的。AAG的某些生物学特性与其唾液酸含量有关;因此,去唾液酸化后AAG的清除率和免疫原性显著增加。AAG的生物学功能在很大程度上尚不清楚。AAG能够抑制某些淋巴细胞的再活性,包括对伴刀豆球蛋白A、植物血凝素和异基因细胞的增殖反应,而去唾液酸化会增强这些抑制作用。鉴于这些观察结果,有报道称非生理性大量(5 - 15毫克/毫升)的AAG会抑制ADP和肾上腺素诱导的血小板聚集,并且有证据表明一种缺乏唾液酸的AAG在几种慢性疾病状态下升高,我们比较了AAG及其去唾液酸化对应物(AAG-D)对血小板聚集的影响。我们报告称,AAG去唾液酸化与对ADP、胶原或凝血酶刺激时观察到的血小板聚集抑制活性的表达增加有关。

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