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El-Gizawy, S., Osman, M., Ibrahim, S. (2018). Effect of Cosolvents on the Absorptive Clearance of Ketotifen Fumarate from Rabbit Intestine, In-situ. Journal of Advanced Pharmacy Research, 2(3), 168-179. doi: 10.21608/aprh.2018.3450.1055
Sanaa El-Gizawy; Mohamed Osman; Sammar Ibrahim. "Effect of Cosolvents on the Absorptive Clearance of Ketotifen Fumarate from Rabbit Intestine, In-situ". Journal of Advanced Pharmacy Research, 2, 3, 2018, 168-179. doi: 10.21608/aprh.2018.3450.1055
El-Gizawy, S., Osman, M., Ibrahim, S. (2018). 'Effect of Cosolvents on the Absorptive Clearance of Ketotifen Fumarate from Rabbit Intestine, In-situ', Journal of Advanced Pharmacy Research, 2(3), pp. 168-179. doi: 10.21608/aprh.2018.3450.1055
El-Gizawy, S., Osman, M., Ibrahim, S. Effect of Cosolvents on the Absorptive Clearance of Ketotifen Fumarate from Rabbit Intestine, In-situ. Journal of Advanced Pharmacy Research, 2018; 2(3): 168-179. doi: 10.21608/aprh.2018.3450.1055

Effect of Cosolvents on the Absorptive Clearance of Ketotifen Fumarate from Rabbit Intestine, In-situ

Article 3, Volume 2, Issue 3, July 2018, Page 168-179  XML PDF (579.9 K)
Document Type: Research Article
DOI: 10.21608/aprh.2018.3450.1055
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Authors
Sanaa El-Gizawy; Mohamed Osman; Sammar Ibrahim email
Department of Pharmaceutical Technology, Faculty of Pharmacy, Tanta University, Tanta, Egypt.
Abstract
Objective: Investigate the effect of ethanol, polyethylene glycol 400, propylene glycol, glycerol and sorbitol on the absorptive clearance of ketotifen fumarate   in the rabbit. Methods: In-situ intestinal perfusion technique, ̎through and through ̎ was used for estimation of membrane transport parameters of ketotifen fumarate from duodenum, jejunum, ileum and ascending colon in the rabbit. These parameters include absorptive clearance per unit length PeA/L (ml/min.cm), percentage fraction absorbed per unit length (% Fa/cm) and anatomical length that required for complete absorption in specific segment (L95%). Results: The absorption was in the order ascending colon> duodenum > jejunum> ileum; where the absorptive clearance normalized to intestinal segment length PeA/L (ml/min.cm) was 0.0071 ± 0.0003, 0.0058 ± 0.0001, 0.0051 ± 0.0001, and 0.0047 ± 0.0001 in each segment respectively. The effect of cosolvents in jejunum was in the order; ethanol 15% >glycerol 30% > propylene glycol (PG40%) > polyethylene glycol400 (PEG-400 40%) >sorbitol 40%, Where the absorptive clearance normalized to intestinal segment length PeA/L (ml/min.cm), mean ± SE was: 0.0142 ±0.0011, 0.0086 ± 0.0002, 0.0075 ± 0.0003, 0.0022 ± 0.0001, and 0.0014 ± 0.0001 for each cosolvents respectively. The same order was obtained in the ascending colon. Conclusion: The enhancing action of the ethanol, propylene glycol and glycerol may be due fluidization of the cell membrane with a subsequent increase in transcellular absorption, while the inhibitory effect of polyethylene glycol and sorbitol could attributed to water secretion, H-bonding formation and reduced thermodynamic activity of drug molecules.
Keywords
Cosolvents; Intestinal absorption; Intestinal perfusion; In situ intestinal absorption; Ketotifen absorption; Ketotifen bioavailability
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