Polymer1 Poly (L-lacitde)/Poly (1,5- dioxepan-2-one) Blends in Drug Release Device Maggie Wang October 27, 2000 The main article came from Journal of Polymer Science V38,786,2000
Polymer2CONTENT n Introduction Gene Therapy Drug Delivery Gene Therapy Drug Delivery Immunoisolation Device Biodegradable Polyester Immunoisolation Device Biodegradable Polyester n Materials PLLA, PDXO, Copolymer, Homopolymer Blends PLLA, PDXO, Copolymer, Homopolymer Blends n Result Analysis Microshpere Morphology, In vitro degradation, Drug Release, Storage Stability Microshpere Morphology, In vitro degradation, Drug Release, Storage Stability n Conclusion
Polymer3INTRODUCTION Gene Therapy Gene Therapy Human gene therapy is defined as a medical intervention based on the alteration of genetic material of living cells in humans. Human gene therapy is defined as a medical intervention based on the alteration of genetic material of living cells in humans. Drug Delivery What’s the big challenge? What’s the big challenge? two approaches two approaches Cell Encapsulation--- T.M.S. Chang 1964 What kind of requirement for the device? What kind of requirement for the device?, Biodegradable Polyester
Polymer4 MATERIALS CHARACTERISTIC Biodegradable Polyester biocompatibility nontoxicity processability resorption of degradation product
Polymer5 Biodegradable Polyester The family Lactide, glycolide, -caprolcatone, trimethylene carbonate, etc Why did they need morphology engineering? n Hydrophobicity and semicrystalline n hard to control degradation rate n attachment to drug or protein
Polymer6 PLLA- Poly (L-lactide) n Semicrystalline n Tg 55 C n In Homopolymer, the crystalline domain show high resistance to degradation Bu 2 SnO 15h 120°C
Polymer7 PDXO-Poly (1,5-dioxepan-2-one) n Completely amorphous n high viscous, Tg -39 C n no tendency to crystallize, excellent choice for the amorphous block in a copolymer Bu 2 SnO 14h 40°C
Polymer8 Copolymer P(L-LA-co-DXO) n Copolymer is semicrystalline n more flexible, moldable n consisting soft and hard segments: soft phase(DXO) elasticity and the degradation hard phase(LLA) mechanical strength
Polymer9 Homopolymerization Blends PLLA-PDXO n Blends exhibit advantageous physical and mechanical properties n phase-separated can obtain double - layered particles n the degradation and release performance can be controlled by means of component ratio.
Polymer10 RESULT ANALYSIS n Morphology of Microspheres n In vitro Degradation n Drug Release n Storage Stability
Polymer11 Morphology of Microspheres Copolymer 50 m More dense less porous Blends 20 m Very porous interconnecting channels
Polymer12Crystallinity n crystallinity increase as the PLLA ratio increased n PDXO in the PLLA domains disturb the crystal
Polymer13 DSC thermograms
Polymer14 In vitro degradation n In theory,DXO are slower degrading than the L-LA n a high content of L-LA degrade faster n Copolymer trendency n Blends trendency---L-LA matrices resistant to water penetration
Polymer15 Drug Release in buffer solution
Polymer16 Storage Stability n Weight change ---moisture adsorption cause chain cleavage n higher humidity, more decrease of MW n storage induce crystallization n copolymer appear more sensitive to storage degradation
Polymer17 CONLUSION
Polymer18 Blends of PLLA-PDXO easily control get what you want