Colon-specific drug delivery systems based on cyclodextrin prod rugs: In vivo evaluation of 5-aminos

来源 :World Journal of Gastroenterology | 被引量 : 0次 | 上传用户:jf8410
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AIM: To investigate the release of cyclodextrin-5-amino-salicylic acid (CyD-5-ASA) in cecum and colon. METHODS: An anti-inflammatory drug 5-ASA was conjugated onto the hydroxyl groups of α-,β- and γ-cyclodextrins (CyDs) through an ester linkage, and the in vivo drug release behavior of these prodrugs in rat’ s gastrointestinal tract after the oral administration was investigated. RESULTS: The 5-ASA concentration in the rat’s stomach and small intestine after the oral administration of CyD-5-ASA conjugate was much lower than that after the oral administration of 5-ASA alone. The lower concentration was attributable to the passage of the conjugate through the stomach and small intestine without significant degradation or absorption, followed by the degradation of the conjugate site-specific in the cecum and colon. The oral administration of CyD-5-ASA resulted in lower plasma and urine concentration of 5-ASA than that of 5-ASA alone. CONCLUSION: CyD-5-ASA conjugates may be used as prodrugs for colon-specific drug delivery system. AIM: To investigate the release of cyclodextrin-5-amino-salicylic acid (CyD-5-ASA) in cecum and colon. METHODS: An anti-inflammatory drug 5-ASA was conjugated onto the hydroxyl groups of α-, β- and γ-cyclodextrins (CyDs) through an ester linkage, and the in vivo drug release behavior of these prodrugs in rat ’s gastrointestinal tract after the oral administration was investigated. RESULTS: The 5-ASA concentration in the rat’s stomach and small intestine after the oral administration of CyD-5-ASA conjugate was much lower than that after oral administration of 5-ASA alone. The lower concentration was attributable to the passage of the conjugate through the stomach and small intestine without significant degradation or absorption, followed by the degradation of the conjugate site-specific in the cecum and colon. The oral administration of CyD-5-ASA resulted in lower plasma and urine concentration of 5-ASA than that of 5-ASA alone. CONCLUSION: CyD-5-ASA conjugates may be used as prod rugs for colon-specific drug delivery system.
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