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使用聚合物递送系统的低分子量肝素的口服生物利用度。

Oral bioavailability of a low molecular weight heparin using a polymeric delivery system.

作者信息

Hoffart Valérie, Lamprecht Alf, Maincent Philippe, Lecompte Thomas, Vigneron Claude, Ubrich Nathalie

机构信息

Inserm U734-EA 3452, Laboratory of Pharmaceutical Technology, School of Pharmacy, 5 rue Albert Lebrun, 54001 Nancy Cedex, France.

出版信息

J Control Release. 2006 Jun 12;113(1):38-42. doi: 10.1016/j.jconrel.2006.03.020. Epub 2006 Apr 7.

Abstract

Low molecular weight heparins (LMWHs) are the standards of anticoagulant for the prevention of deep vein thrombosis (DVT) in patients undergoing arthroplasty and abdominal surgery. However, LMWHs are so far only administered by parenteral route. Thus, they are usually replaced by oral warfarin for outpatient therapy. Since warfarin has a slow onset and high incidence of drug-drug interaction, there is a great need for the development of an oral LMWH formulation. LMWH (tinzaparin)-loaded nanoparticles prepared with a blend of a polyester and a polycationic polymethacrylate by the double emulsion method were administered orally in fasted rabbits. The plasma tinzaparin concentration was measured by a chromogenic anti-factor Xa assay. After oral administration of two doses of tinzaparin-loaded nanoparticles (200 and 600 anti-Xa U/kg), the oral absorption was observed between 4 and 10 or 12 h, with a delayed onset of action ranging from 3 to 4 h. Mean absolute bioavailabilities were 51% and 59% for the two tested doses. We now report that the encapsulation of tinzaparin into nanoparticles is likely to contribute to its oral efficacy with an anticoagulant effect prolonged up to 8 h.

摘要

低分子量肝素(LMWHs)是关节置换术和腹部手术患者预防深静脉血栓形成(DVT)的抗凝标准药物。然而,迄今为止,LMWHs仅通过胃肠外途径给药。因此,门诊治疗时它们通常会被口服华法林取代。由于华法林起效缓慢且药物相互作用发生率高,因此迫切需要开发口服LMWH制剂。采用双乳液法,用聚酯和聚阳离子聚甲基丙烯酸酯的混合物制备了载有LMWH(替扎肝素)的纳米颗粒,并将其口服给予禁食的兔子。通过显色抗Xa因子测定法测量血浆替扎肝素浓度。口服两剂载有替扎肝素的纳米颗粒(200和600抗Xa U/kg)后,在4至10或12小时观察到口服吸收,起效延迟3至4小时。两种测试剂量的平均绝对生物利用度分别为51%和59%。我们现在报告,将替扎肝素包封到纳米颗粒中可能有助于其口服疗效,抗凝作用延长至8小时。

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