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去氨加压素可增强血小板对人动脉内皮下层的黏附及血小板聚集体的生长。

DDAVP enhances platelet adherence and platelet aggregate growth on human artery subendothelium.

作者信息

Sakariassen K S, Cattaneo M, vd Berg A, Ruggeri Z M, Mannucci P M, Sixma J J

出版信息

Blood. 1984 Jul;64(1):229-36.

PMID:6428488
Abstract

The effect of intravenous 1-deamino (8-D-arginine)vasopressin (DDAVP) administration on platelet interaction with human artery subendothelium was investigated with flowing blood from five normal individuals and 12 patients with von Willebrand's disease (vWD). Three of the patients were diagnosed as vWD subtype I, four as subtype IIa, and five as subtype IIb. DDAVP administration to normals enhanced platelet adherence, in parallel with increasing plasma levels of factor VIII-related antigen ( FVIIIR :Ag) and ristocetin cofactor activity ( FVIIIR :RCF). Platelet aggregate formation was transiently increased within 90 minutes. Platelet adherence in patient blood before DDAVP infusion was subnormal. In patients with subtype I, administration of DDAVP normalized the bleeding time, enhanced the platelet adherence, and transiently improved the platelet aggregate formation. The platelet adherence was more corrected than would have been expected on the basis of the FVIIIR :Ag and FVIIIR :RCF levels. In patients with subtype IIa, infusion of DDAVP increased the FVIIIR :Ag levels approximately threefold, without affecting the FVIIIR :RCF levels, and in only two of four patients was a transiently enhanced platelet adherence with a corresponding shortening of the bleeding time observed. In patients with subtype IIb, administration of DDAVP increased the FVIIIR :Ag levels about threefold and the FVIIIR :RCF levels five to tenfold, but decreased the platelet adherence significantly. The bleeding time values were not normalized. A close association between the bleeding time values and corresponding platelet adherence values before and after DDAVP infusion was observed. Normalization of the bleeding time was paralleled with normalization of platelet adherence. We conclude that DDAVP improves the primary hemostasis by causing enhanced FVIII-vWF-mediated platelet adherence. DDAVP has little or no effect on the bleeding time in patients with subtype IIa and subtype IIb, because the platelet adherence is not normalized.

摘要

研究了静脉注射1-去氨基(8-D-精氨酸)血管加压素(DDAVP)对5名正常人和12名血管性血友病(vWD)患者血小板与人动脉内皮下相互作用的影响。其中3例患者被诊断为vWD I型,4例为IIa型,5例为IIb型。给正常人注射DDAVP可增强血小板黏附,同时血浆中VIII因子相关抗原(FVIIIR:Ag)水平和瑞斯托霉素辅因子活性(FVIIIR:RCF)升高。血小板聚集在90分钟内短暂增加。DDAVP输注前患者血液中的血小板黏附低于正常水平。I型患者注射DDAVP可使出血时间正常化,增强血小板黏附,并短暂改善血小板聚集。血小板黏附的改善程度超过了根据FVIIIR:Ag和FVIIIR:RCF水平预期的程度。IIa型患者输注DDAVP可使FVIIIR:Ag水平升高约三倍,而不影响FVIIIR:RCF水平,且在4例患者中只有2例观察到血小板黏附短暂增强,出血时间相应缩短。IIb型患者注射DDAVP可使FVIIIR:Ag水平升高约三倍,FVIIIR:RCF水平升高五至十倍,但显著降低血小板黏附。出血时间值未恢复正常。观察到DDAVP输注前后出血时间值与相应血小板黏附值之间密切相关。出血时间正常化与血小板黏附正常化平行。我们得出结论,DDAVP通过增强FVIII-vWF介导的血小板黏附来改善初级止血。DDAVP对IIa型和IIb型患者的出血时间几乎没有影响,因为血小板黏附未恢复正常。

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