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一种新开发的用于治疗深静脉血栓的口服肝素衍生物:非人灵长类动物研究。

A newly developed oral heparin derivative for deep vein thrombosis: non-human primate study.

作者信息

Kim Sang Kyoon, Lee Dong Yun, Kim Choong Yong, Nam Jong Hee, Moon Hyun Tae, Byun Youngro

机构信息

Department of Materials Science and Engineering, Gwangju Institute of Science and Technology, Gwangju 500-712, Republic of Korea.

出版信息

J Control Release. 2007 Nov 6;123(2):155-63. doi: 10.1016/j.jconrel.2007.08.007. Epub 2007 Aug 16.

Abstract

The development of orally active heparin will have tremendous clinical importance since it can be used to effectively prevent deep vein thrombosis (DVT) in a long-term chronic treatment. We developed in this study a new orally active heparin derivative (Db-LHD), which has heparin chemically conjugated with deoxycholic acid and DMSO molecules by secondary interactions. Db-LHD was prepared in the powder form in soft capsules. When we administered Db-LHD capsules to monkeys, its oral physiological availability was increased up to 16.6%. The maximum anti-FXa activity at 5 mg/kg of Db-LHD was more than twice the minimum effective anti-FXa activity (MEC, 0.1 IU/mL) for preventing DVT, and the anti-FXa activity in plasma was maintained for 10 h above the MEC in monkeys. Also, we evaluated anti-thrombogenic effect of Db-LHD in a rat thrombosis model. A subcutaneous administration of enoxaparin (100 IU/kg), which was the highest recommended dose for the prevention of venous thromboembolism, reduced thrombus formation by 38.9+/-14.2%. On the other hand, 5 mg/kg (425 IU/kg) of orally administered Db-LHD reduced thrombus formation by 51.0+/-2.0. We propose a new orally active heparin, Db-LHD, in a solid dosage form to effectively prevent DVT and PE.

摘要

口服活性肝素的研发具有重大临床意义,因为它可用于长期慢性治疗中有效预防深静脉血栓形成(DVT)。在本研究中,我们开发了一种新型口服活性肝素衍生物(Db-LHD),它通过次级相互作用使肝素与脱氧胆酸和二甲基亚砜分子化学偶联。Db-LHD制成软胶囊中的粉末形式。当我们给猴子服用Db-LHD胶囊时,其口服生理利用率提高到了16.6%。5mg/kg的Db-LHD的最大抗FXa活性是预防DVT的最小有效抗FXa活性(MEC,0.1IU/mL)的两倍多,并且在猴子体内血浆中的抗FXa活性在MEC以上维持了10小时。此外,我们在大鼠血栓形成模型中评估了Db-LHD的抗血栓形成作用。皮下注射依诺肝素(100IU/kg),这是预防静脉血栓栓塞的最高推荐剂量,可使血栓形成减少38.9±14.2%。另一方面,口服5mg/kg(425IU/kg)的Db-LHD可使血栓形成减少51.0±2.0。我们提出了一种新型口服活性肝素Db-LHD,制成固体剂型以有效预防DVT和PE。

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