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   Preparation, Characterization, and Dissolution Studies of Naproxen Solid Dispersions Using Polyethylene Glycol 6000 and Labrafil M2130  
   
نویسنده Akbari Jafar ,Enayatifard Reza ,Saeedi Majid ,Morteza-Semnani Katayoun ,Rajabi Samira
منبع Pharmaceutical And Biomedical Research - 2015 - دوره : 1 - شماره : 2 - صفحه:44 -53
چکیده    Naproxen is a poor water soluble, nonsteroidal analgesic and antiinflammatory drug. the enhancement of oral bioavailability of poor water soluble drugs remains one of the most challenging aspects of drug development. although salt formation, solubilization and particle size reduction have commonly been used to increase dissolution rate and thereby oral absorption and bioavailability of low water soluble drugs, there are practical limitation of these techniques. however, the most attractive option for increasing the release rate is improvement of solubility through formulation approaches.in this study, solid dispersions (sd) of naproxen were prepared by hot melt method using various ratios of drug to polymers (peg6000) separately and characterized for physical appearance, ftir, dsc, xray crystallography, and invitro dissolution studies. the influence of several amounts of labrafil m2130 was also studied.ftir study revealed that drug was stable in sds, and great state of amorphous formed particles was proofed by dsc analyze. the in vitro dissolution studies were carried using usp type ii (paddle) dissolution apparatus at medium (ph=1.5). solubility of naproxen fromsds was increased in dissolution media. the prepared dispersion showed increase in the dissolution rate of naproxen comparing to that of physical mixtures of drug and polymers and pure drug. percent of drug released in 60 minutes was 23.92% for pure naproxen witch is increased in sds and reached to100% for best formulations of peg6000 and labrafil based sds respectively, considering ratio of drug to polymers.it is concluded that dissolution of the naproxen could be improved by the solid dispersion. although physical mixtures have increased the rate of dissolution, dissolution shows faster release from sds which would therefore be due to formation of amorphous particles through the hot melt process which was also revealed by dsc analysis and xrd.
کلیدواژه Naproxen ,Release Rate ,Hot Melt Method ,Solid Dispersion
آدرس Mazandaran University Of Medical Sciences, Faculty Of Pharmacy, Department Of Pharmaceutics, ایران, Mazandaran University Of Medical Sciences, Faculty Of Pharmacy, Department Of Pharmaceutics, ایران, Mazandaran University Of Medical Sciences, Faculty Of Pharmacy, Department Of Pharmaceutics, ایران, Mazandaran University Of Medical Sciences, Faculty Of Pharmacy, Department Of Medicinal Chemistry, ایران, Mazandaran University Of Medical Sciences, Faculty Of Pharmacy, Department Of Pharmaceutics, ایران
 
     
   
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