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Development of hot-melt extrusion as a novel technique for the ...

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1.8 Aims and objectivesThe purpose <strong>of</strong> this research study is to develop HME <strong>as</strong> an efficient <strong>technique</strong> <strong>for</strong> <strong>the</strong><strong>for</strong>mulation <strong>of</strong> various oral solid dosage <strong>for</strong>ms with <strong>the</strong> aim <strong>of</strong> incre<strong>as</strong>ing <strong>the</strong> dissolution rate <strong>of</strong>some poorly soluble model APIs (i.e ibupr<strong>of</strong>en, indomethacin, famotidine) via <strong>the</strong> <strong>for</strong>mation <strong>of</strong>solid dispersions. Also <strong>the</strong> evaluation <strong>of</strong> t<strong>as</strong>te m<strong>as</strong>king efficiency (in vivo and in vitro) <strong>of</strong>different polymeric matrices (via intermolecular hydrogen bonding) <strong>as</strong> well <strong>as</strong> characterizing allpossible intermolecular interactions in <strong>the</strong> solid dispersions h<strong>as</strong> been prioritised <strong>as</strong> second aim <strong>of</strong>this research.1.9 References1. Kalivoda A, Fischbach M, Kleinebudde P. Application <strong>of</strong> mixtures <strong>of</strong> polymeric carriers<strong>for</strong> dissolution enhancement <strong>of</strong> oxeglitazar using <strong>hot</strong>-<strong>melt</strong> <strong>extrusion</strong>. Int J Pharm. 2012;439(1-2):145-56.2. Repka MA, Shah S, Lu J, Maddineni S, Morott J, Patwardhan K, Mohammed NN. Melt<strong>extrusion</strong>: process to product. Exp Opin Drug Deliv 2012; 9(1):105-25.3. Repka MA, Majumdar S, Kumar Battu S, Srirangam R, Upadhye SB. Applications <strong>of</strong> <strong>hot</strong><strong>melt</strong><strong>extrusion</strong> <strong>for</strong> drug delivery. Exp Opin Drug Deliv 2008; 5(12):1357-76.4. Repka MA, Battu SK, Upadhye SB, Thumma S, Crowley MM, Zhang F, Martin C,McGinity JW. Pharmaceutical applications <strong>of</strong> <strong>hot</strong>-<strong>melt</strong> <strong>extrusion</strong>: Part II. Drug Dev IndPharm 2007; (10):1043-57.5. Kolter K, Karl M, Gryczke A. Hot-<strong>melt</strong> <strong>extrusion</strong> with BASF Pharma polymers,Extrusion Compendium (2 nd edition), BASF Germany. 2012.6. Crowley MM, Thumma S, Updhye SB. Pharmaceutical applications <strong>of</strong> <strong>hot</strong> <strong>melt</strong> <strong>extrusion</strong>:part- I. Drug Dev Ind Pharm 2007; 33(9):909-26.7. James S. Encyclopedia <strong>of</strong> Pharmaceutical Technology. 2004; 3rd Ed (3); P-20.8. Andrews GP and Jones DS. Formulation and Characterization <strong>of</strong> Hot Melt ExtrudedDosage Forms: Challenges and Opportunities. Chemin<strong>for</strong>m 2010; 41(43).9. Breitenbach J. Melt <strong>extrusion</strong>: from process to drug delivery technology. Eur J PharmBiopharm 2002; 54:107–117.10. Andrews GP, David S, Osama AM, Daniel NM, Mark.S. Hot Melt Extrusion: AnEmerging Drug Delivery Technology. Pharm Tech Europe 2009; 21 (1):24-27.11. Follonier N, Doelker E, Cole ET. Evaluation <strong>of</strong> <strong>hot</strong>-<strong>melt</strong> <strong>extrusion</strong> <strong>as</strong> a new <strong>technique</strong> <strong>for</strong><strong>the</strong> production <strong>of</strong> polymerb<strong>as</strong>ed pellets <strong>for</strong> sustained rele<strong>as</strong>e capsules containing highloadings <strong>of</strong> freely soluble drugs. Drug Dev Ind Pharm 1994; 20(8):1323-133.13 | P a g e

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