Developing an Oral-Insulin-Delivery System using GET-peptide-mediated transcytosisTools Rehmani, Sahrish (2021) Developing an Oral-Insulin-Delivery System using GET-peptide-mediated transcytosis. PhD thesis, University of Nottingham.
AbstractInsulin a peptide hormone regulates blood glucose levels and is considered a mainstay of treatment for diabetic patients. Oral insulin delivery still represents an overwhelming challenge due to its physio-chemical instability in gastro-intestinal tract (GIT) and poor intestinal permeability. A novel multidomain fusion-peptide system was employed to overcome these barriers termed Glycosaminoglycan (GAG)-binding enhanced transduction (GET) system, where GAG-binding motif promotes cell targeting and surface binding, whereas cell-penetrating-peptides (CPPs) region allows efficient cell entry. Here, potential of GET system in enhancing intestinal insulin permeation (transcytosis and translocation efficiency) was assessed across an in-vitro gut model system (Caco-2 cell monolayers). Insulin recycling was studied using different secretion regulators, moreover functional activity (by employing insulin-reporter cells) and stability of insulin-GET nanocomplexes (NCs) was also determined. In-house synthesised NHS-Fluorescein labelled insulin (Ins-F, non-quenchable) was used for studying internalisation, and transcytosis. Different stability assays were developed for GET system and insulin-GET NCs using quenchable proprietary FITC-insulin (Ins-F*). The difference in fluorescent behaviour of both insulins was studied using quenching and dequenching assays. pH-sensitive micro-particulates (MPs) based on Eudragit-L100 served as an enteric carrier system for insulin-GET NCs. These Eudragit-L100-MPs were characterised for their size, charge, morphology, drug release as a function of pH, and cellular uptake efficiency of released NCs across Caco-2 monolayers. Furthermore, enteric coated minicapsules were developed as an alternative to MPs for oral insulin delivery.
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