药物输送
前药
医学
溃疡性结肠炎
药品
靶向给药
炎症性肠病
炎症
囊性纤维化
药理学
疾病
免疫学
内科学
纳米技术
材料科学
作者
Niranjan G. Kotla,Shubhasmin Rana,Gandhi Sivaraman,Omprakash Sunnapu,Praveen Kumar Vemula,Abhay Pandit,Yury Rochev
标识
DOI:10.1016/j.addr.2018.06.021
摘要
Oral colon-specific delivery systems emerged as the main therapeutic cargos by making a significant impact in the field of modern medicine for local drug delivery in intestinal inflammation. The site-specific delivery of therapeutics (aminosalicylates, glucocorticoids, biologics) to the ulcerative mucus tissue can provide prominent advantages in mucosal healing (MH). Attaining gut mucosal healing and anti-fibrosis are main treatment outcomes in inflammatory bowel disease (IBD). The pharmaceutical strategies that are commonly used to achieve a colon-specific drug delivery system include time, pH-dependent polymer coating, prodrug, colonic microbiota-activated delivery systems and a combination of these approaches. Amongst the different approaches reported, the use of biodegradable polysaccharide coated systems holds great promise in delivering drugs to the ulcerative regions. The present review focuses on major physiological gastro-intestinal tract challenges involved in altering the pharmacokinetics of delivery systems, pathophysiology of MH and fibrosis, reported drug-polysaccharide cargos and focusing on conventional to advanced disease responsive delivery strategies, highlighting their limitations and future perspectives in intestinal inflammation therapy.
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