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DESIGN OF A SOFT, SELF-UNCOILING STENT FOR EXTENDED RETENTION OF DRUG DELIVERY IN THE SMALL INTESTINE

机译:柔软,自损伤支架的设计,用于延长小肠中药物递送的延长保留

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Despite being the preferred route of drug administration, the oral formulation of biological drugs is limited due to its intrinsic instability, low permeability, and physical, chemical and immunological barriers. Various innovative swallowable technologies such as drug-loaded, dissolvable microneedles, mucoadhesive patches, and various microdevices present unique drug-carrying capabilities. The current work presents a novel soft stent platform that can facilitate contact between the small intestine tissue and drug carriers to enhance drug absorption and increase residence time. This study aims to prove the concept of this novel platform and determine if the soft stent will retain orally to the ileocecal valve longer than a capsule-shaped bolus. Benchtop studies on an intestinal simulator showed successful retention of the soft stent compared to a control capsule. In vivo studies in pig models also showed that the soft stent was retained longer than the control capsule. Overall, this study shows promise that this novel platform could be used for oral drug delivery of biologics.
机译:尽管是药物施用的优选途径,但由于其内在的不稳定性,低渗透性和物理,化学和免疫屏障,对生物药物的口腔制剂受到限制。各种创新的吞咽技术,如药物负载,可溶解的微针,粘膜粘附贴片和各种微生物,具有独特的药物承载能力。目前的工作提出了一种新型软支架平台,可以促进小肠组织和药物载体之间的接触,以提高药物吸收和增加停留时间。本研究旨在证明该新颖平台的概念,并确定软支架是否会使口腔阀门更长,而不是胶囊形的推注。与对照胶囊相比,对肠道模拟器的Benchtop研究表明,软支架的成功保留了软支架。在猪模型的体内研究中也表明软支架保持比对照胶囊更长。总体而言,本研究表明,这一新颖性平台可用于对生物制剂的口服药物传递。

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