Potential Roles of the Glass Transition Temperature of PLGA Microparticles in Drug Release Kinetics
Author(s) -
Kinam Park,
Andrew Otte,
Farrokh Sharifi,
John Garner,
Sarah Skidmore,
Haesun Park,
Young Kuk Jhon,
Bin Qin,
Yan Wang
Publication year - 2020
Publication title -
molecular pharmaceutics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.13
H-Index - 127
eISSN - 1543-8392
pISSN - 1543-8384
DOI - 10.1021/acs.molpharmaceut.0c01089
Subject(s) - plga , kinetics , drug , chemistry , drug delivery , controlled release , drug carrier , chemical engineering , materials science , nanotechnology , pharmacology , organic chemistry , biochemistry , in vitro , medicine , engineering , physics , quantum mechanics
Poly(lactic- co -glycolic acid) (PLGA) has been used for long-acting injectable drug delivery systems for more than 30 years. The factors affecting the properties of PLGA formulations are still not clearly understood. The drug release kinetics of PLGA microparticles are influenced by many parameters associated with the formulation composition, manufacturing process, and post-treatments. Since the drug release kinetics have not been explainable using the measurable properties, formulating PLGA microparticles with desired drug release kinetics has been extremely difficult. Of the various properties, the glass transition temperature, T g , of PLGA formulations is able to explain various aspects of drug release kinetics. This allows examination of parameters that affect the T g of PLGA formulations, and thus, affecting the drug release kinetics. The impacts of the terminal sterilization on the T g and drug release kinetics were also examined. The analysis of drug release kinetics in relation to the T g of PLGA formulations provides a basis for further understanding of the factors controlling drug release.
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