Progesterone solutions for increased bioavailability
作者: Saujanya L. Gosangari , Zhi Liu , Aqeel Fatmi , Dana S. Toops
DOI:
关键词: Dissolution 、 Bioavailability 、 Capsule 、 Chromatography 、 Hydrophobic drug 、 Long chain 、 Organic chemistry 、 In vivo 、 Micronized progesterone 、 Materials science 、 Organic acid
摘要: Fill materials for hydrophobic drugs, such as progesterone, and methods of making using thereof are described herein. The fill material contains the drug dissolved in one or more fatty acids. concentration is typically from about 7% to 50% by weight material. acids 60% 95% carrier. formulation also an organic acid both pharmaceutically acceptable alcohols mono-, di-, triesters medium long chain can be encapsulated a hard soft capsule. formulations herein have higher dissolution rate faster onset compared micronized progesterone suspended oil thus should increased bioavailability vivo.
google.ch 参考文章(13)
Vibeke Friis Nielsen, Stability of progestogen formulations ,(2006)
Nirmal Mulye, Microemulsion concentrate composition of cyclosporin ,(1999)
Karl F. Popp, Dermatologic soft gel compositions ,(2005)
Adedotun Tony Adesunloye, Paul Edward Stach, Filled gelatin capsules ,(1997)
Wayne S. Maxson, Joel T. Hargrove, Philip G. Meyers, Method for treatment of premenstrual syndrome ,(1988)
Aqeel A. Fatmi, Nachiappan Chidambaram, Emadeldin M. Hassan, Enteric composition for the manufacture of soft capsule wall ,(2003)
Tomas Andrysek, Ales Vrana, Crystallization inhibitor and its use in gelatin capsules ,(2006)
Susan Gerrard Chandler, Elizabeth Anne Perry, Josephine Joan Christine Ferdinando, Oral pharmaceutical compositions containing sex hormones ,(1997)
Jonathan Ernest Lacy, Jonathan Kenneth Embleton, Delivery systems for hydrophobic drugs ,(1995)
Hiroshi Ninomiya, Yoshiyasu Henmi, Masaru Suzuki, Takashi Terada, Etoposide soft capsules ,(1985)