Kim Sang Kyoon, Lee Dong Yun, Lee Eunhye, Lee Yong-kyu, Kim Choong Yong, Moon Hyun Tae, Byun Youngro
Department of Materials Science and Engineering, Gwangju Institute of Science and Technology, Gwangju, South Korea.
J Control Release. 2007 Jul 16;120(1-2):4-10. doi: 10.1016/j.jconrel.2007.03.008. Epub 2007 Mar 20.
The oral delivery of macromolecules is a topic of much interest as this would undoubtedly improve patient acceptance and compliance with chronic regimens. Heparin and insulin are perhaps among the first candidates that should be considered for oral macromolecule delivery systems. Heparin is the most potent anti-coagulant known for the prevention of deep vein thrombosis and pulmonary embolism, and an orally active heparin would undoubtedly effectively reduce chronic thrombotic events. Here, we report on the development of an orally administrable chemical conjugate of heparin and hydrophobic deoxycholic acid (DOCA), which we refer to as LHD. LHD was pre-formulated with dimethyl sulfoxide (DMSO) as solubilizer to further improve its oral bioavailability (9.1% in monkey). LHD was found to be absorbed mainly in the jejunum and ileum of the small intestine, although it is in the ileum that the absorption is most notable. From the mechanism studies of LHD absorption using Caco-2 cell monolayers for mimicking the intestine, we found that LHD highly permeated by passive diffusion through the transcellular route and its permeation was partially affected by bile acid transporters. This study demonstrates the feasibility of chemically modified heparin for long-term oral administration as an effective therapy for venous thromboembolism in clinical trials.
大分子的口服给药是一个备受关注的话题,因为这无疑会提高患者对慢性治疗方案的接受度和依从性。肝素和胰岛素可能是口服大分子递送系统首先应考虑的候选药物。肝素是预防深静脉血栓形成和肺栓塞最有效的抗凝剂,口服活性肝素无疑能有效减少慢性血栓形成事件。在此,我们报告了一种可口服的肝素与疏水性脱氧胆酸(DOCA)的化学偶联物的研发情况,我们将其称为LHD。LHD预先与二甲基亚砜(DMSO)作为增溶剂配制,以进一步提高其口服生物利用度(在猴子中为9.1%)。发现LHD主要在小肠的空肠和回肠吸收,不过在回肠吸收最为显著。通过使用Caco-2细胞单层模拟肠道对LHD吸收进行机制研究,我们发现LHD通过跨细胞途径以被动扩散方式高度渗透,其渗透部分受胆汁酸转运体影响。本研究证明了化学修饰肝素长期口服给药作为临床试验中静脉血栓栓塞有效治疗方法的可行性。
