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Drug Deliv Transl Res. 2018 Jun;8(3):853-856. doi: 10.1007/s13346-017-0471-7.
Postpartum hemorrhage is a major cause of mortality and morbidity related to childbirth in developing countries. The recommended treatment includes administration of oxytocin; however, oxytocin is a heat-labile protein, and it must be given as an intramuscular injection by skilled health care providers. To address these challenges, we developed a freeze-dried oxytocin fast-dissolving tablet (FDT) for sublingual (SL) needle-free administration. Using methods developed previously, we produced a robust FDT that maintained oxytocin stability at 40 °C, 75% relative humidity for 12 months. This formulation contains 9% sucrose, 1.5% (hydroxypropyl)methyl cellulose, 9% mannitol, 4% dextran, 1% carbomer, 1% sodium taurocholate, and 100 IU oxytocin. An in vitro study showed a > 30% reduction in tissue transepithelial electrical resistance after treatment with the oxytocin FDT, implying an increase in the permeability of the mucosal tissue to oxytocin. Anesthetized Yucatan miniature swine were administered a SL FDT, and blood was periodically collected for a pharmacokinetic study. Higher plasma concentrations were seen when larger SL doses were given. The maximum concentrations for SL and intramuscular doses in anesthetized pigs were 207 and 612 pg/mL, respectively. Whether the levels attained will be sufficient to elicit beneficial results in humans is yet to be determined. This study demonstrates the feasibility of our approach for developing a heat-stable oxytocin tablet that can be administered successfully via the SL route.
产后出血是发展中国家与分娩相关的死亡和发病的主要原因。推荐的治疗方法包括给予催产素;然而,催产素是一种热不稳定的蛋白质,必须由熟练的医疗保健提供者进行肌肉注射。为了解决这些挑战,我们开发了一种用于舌下(SL)无针给药的冻干催产素速溶片(FDT)。使用以前开发的方法,我们生产了一种坚固的 FDT,在 40°C、75%相对湿度下可将催产素的稳定性保持 12 个月。该配方含有 9%蔗糖、1.5%(羟丙基)甲基纤维素、9%甘露醇、4%右旋糖酐、1%卡波姆、1%牛磺胆酸钠和 100IU 催产素。体外研究表明,催产素 FDT 治疗后组织跨上皮电阻降低了>30%,这意味着粘膜组织对催产素的通透性增加。给麻醉的尤卡坦微型猪给予 SL FDT,并定期采集血液进行药代动力学研究。给予较大的 SL 剂量时,可观察到更高的血浆浓度。在麻醉猪中,SL 和肌肉内剂量的最大浓度分别为 207 和 612pg/mL。所达到的水平是否足以在人类中产生有益的结果还有待确定。这项研究证明了我们开发热稳定催产素片剂并通过 SL 途径成功给药的方法是可行的。