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通过体内输注抗血小板糖蛋白IIb/IIIa受体单克隆抗体的F(ab')2片段抑制犬血小板功能。

Inhibition of dog platelet function by in vivo infusion of F(ab')2 fragments of a monoclonal antibody to the platelet glycoprotein IIb/IIIa receptor.

作者信息

Coller B S, Scudder L E

出版信息

Blood. 1985 Dec;66(6):1456-9.

PMID:2998514
Abstract

To assess the potential of monoclonal antibodies that inhibit platelet function in vitro as in vivo therapeutic agents, F(ab')2 fragments (0.17 to 0.81 mg/kg) of a murine monoclonal antibody (7E3) that binds to platelet glycoproteins IIb and/or IIIa and blocks platelet aggregation induced by ADP were infused into three dogs. Soon after infusion, platelets recovered from the dogs showed a decreased aggregation response to adenosine diphosphate, with the highest dose producing nearly total inhibition. These platelets also showed decreased ability to bind 125I-7E3, which was assumed to reflect occupancy of the sites by the unlabeled F(ab')2 fragments. At the highest dose, the binding decreased by 85%, reflecting the binding of approximately 44,000 molecules of 7E3 F(ab')2 per platelet. Platelet counts decreased after antibody infusion by less than 20%, and none of the dogs showed spontaneous bleeding. Both the aggregation and binding results reverted toward normal within one day. We conclude that it is possible to profoundly inhibit platelet function by in vivo infusion of F(ab')2 fragments of a monoclonal antiplatelet antibody without producing spontaneous hemorrhage or significant thrombocytopenia.

摘要

为了评估在体外抑制血小板功能的单克隆抗体作为体内治疗剂的潜力,将一种与血小板糖蛋白IIb和/或IIIa结合并阻断ADP诱导的血小板聚集的鼠单克隆抗体(7E3)的F(ab')2片段(0.17至0.81mg/kg)注入三只狗体内。注入后不久,从狗身上回收的血小板对二磷酸腺苷的聚集反应降低,最高剂量几乎产生完全抑制。这些血小板与125I-7E3结合的能力也降低,这被认为反映了未标记的F(ab')2片段占据了这些位点。在最高剂量下,结合减少了85%,这反映了每个血小板约有44,000个7E3 F(ab')2分子的结合。注入抗体后血小板计数下降不到20%,且没有一只狗出现自发性出血。聚集和结合结果在一天内都恢复到正常。我们得出结论,通过体内注入单克隆抗血小板抗体的F(ab')2片段可以深刻抑制血小板功能,而不会产生自发性出血或显著的血小板减少症。

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