Formulation buoyancy of nanoencapsulated gliclazide using primary, conjugated and deconjugated bile acids

Mathavan S.; Ionescu C.; Božica Kovačević; Momir Mikov; Svetlana Goločorbin-Kon; Mooranian A.; Dass C.; Al-Salami H.

Молимо вас користите овај идентификатор за цитирање или овај линк до ове ставке: https://open.uns.ac.rs/handle/123456789/15910

Назив:	Formulation buoyancy of nanoencapsulated gliclazide using primary, conjugated and deconjugated bile acids
Аутори:	Mathavan S. Ionescu C. Božica Kovačević Momir Mikov Svetlana Goločorbin-Kon Mooranian A. Dass C. Al-Salami H.
Кључне речи:	buoyancy;cell viability;drug tissue permeation;excipient stabilizing;gliclazide;muscle cells
Датум издавања:	1-јан-2019
Часопис:	Therapeutic Delivery
Сажетак:	© 2019 Newlands Press. Aim: Recent studies suggest potential applications of endogenously produced human bile acids as formulation-excipient and drug tissue permeation enhancers in Type 1 diabetes. We aimed to examine the stability, tissue permeation and ex vivo muscle-cell effects of microencapsulated gliclazide (G) incorporated with a primary (chenodeoxycholic acid [CDCA]), a secondary (ursodeoxycholic acid [UDCA]) or a tertiary (taurocholic acid [TCA]) bile acid. Materials & methods: Four formulations made of sodium alginate, CDCA, UDCA and TCA were examined for buoyancy, tissue-enhancing effects (in vivo) and local (ex vivo) viability effects. Results & conclusion: CDCA, UDCA and TCA improved buoyancy and cell viability but not tissue-specific uptake. G-TCA-sodium alginate microcapsules exerted hypoglycemic effects, suggesting significant improvement of G gut-uptake by TCA, possibly via improving buoyancy.
URI:	https://open.uns.ac.rs/handle/123456789/15910
ISSN:	20415990
DOI:	10.4155/tde-2019-0058
Налази се у колекцијама:	MDF Publikacije/Publications