Abstract

The overall goal of this project is to investigate the effects of polymer microsphere size and size distribution, and the shell thickness of core-shell microparticles, on macromolecule encapsulation and release. Proteins and other macromolecules form a rapidly growing class of therapeutics. Because of short in vivo half-life and poor oral bioavailability, frequently repeated injections are usually required. Alternative formulations and delivery systems for proteins present a variety of new challenges. Controlled-release drug delivery systems may provide better control of drug concentrations, reduced side effects and improved compliance. However, design of controlled-release devices, such as biodegradable polymer microspheres, is difficult because of incomplete understanding of the mechanisms that control release and that affect protein stability. We have reported a unique precision particle fabrication (PPF) technique that produces monodisperse microspheres, with precise control of particle size, and core-shell particles with control of shell thickness. Previously, we have shown that by controlling the particle size and shell thickness, we could control small-molecule release rates, and we have discovered several unexpected mechanisms by which particle size can affect release. PPF may provide a similar opportunity to control macromolecule release. Further, we hypothesize that the core-shell morphology, in particular those with aqueous cores, may provide enhanced stability of encapsulated proteins. In this project, we will test these hypotheses by investigating in vitro release of four model compounds from uniform PLGA microspheres (Aim 1) and core-shell particles of various morphologies (Aim 2). To investigate release mechanisms, experiments are also designed to follow changes in drug distribution and particle morphology during degradation. Preliminary results suggest that microspheres undergo autocatalytic degradation due to accumulation of acidic polymer degradation products to an extent depending on diameter. Thus, we will use ratiometric confocal fluorescence microscopy to measure pH microenvironment inside degrading particles with varying diameter and shell thickness (Aim 3). Finally, we will compare stability of proteins encapsulated in solid microspheres versus microcapsules, as the latter will exhibit a smaller aqueous-organic interface and may maintain more neutral intraparticle pH (Aim 4). To now, the effects of microparticle size on the factors controlling release rates have been obscured by typically broad particle size distributions. Through precision particle fabrication, this project will result in novel fundamental insights into mechanisms controlling release as well as provide a method for enhanced control of release rates. ? ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Biomedical Imaging and Bioengineering (NIBIB)
Type
Research Project (R01)
Project #
1R01EB005181-01A1
Application #
7073104
Study Section
Gene and Drug Delivery Systems Study Section (GDD)
Program Officer
Moy, Peter
Project Start
2006-04-01
Project End
2010-01-31
Budget Start
2006-04-01
Budget End
2007-01-31
Support Year
1
Fiscal Year
2006
Total Cost
$265,570
Indirect Cost

  Institution

Name
University of Illinois Urbana-Champaign
Department
Engineering (All Types)
Type
Schools of Engineering
DUNS #
041544081
City
Champaign
State
IL
Country
United States
Zip Code
61820

  Publications

Ford Versypt, Ashlee N; Arendt, Paul D; Pack, Daniel W et al. (2015) Derivation of an Analytical Solution to a Reaction-Diffusion Model for Autocatalytic Degradation and Erosion in Polymer Microspheres. PLoS One 10:e0135506
Zhu, Xiaoxiang; Braatz, Richard D (2015) A mechanistic model for drug release in PLGA biodegradable stent coatings coupled with polymer degradation and erosion. J Biomed Mater Res A 103:2269-79
Zhu, Xiaoxiang; Braatz, Richard D (2014) Modeling and analysis of drug-eluting stents with biodegradable PLGA coating: consequences on intravascular drug delivery. J Biomech Eng 136:
Xia, Yujie; Pack, Daniel W (2014) Pulsatile protein release from monodisperse liquid-core microcapsules of controllable shell thickness. Pharm Res 31:3201-10
Zhu, Xiaoxiang; Pack, Daniel W; Braatz, Richard D (2014) Modelling intravascular delivery from drug-eluting stents with biodurable coating: investigation of anisotropic vascular drug diffusivity and arterial drug distribution. Comput Methods Biomech Biomed Engin 17:187-98
Versypt, Ashlee N Ford; Braatz, Richard D (2014) Analysis of Finite Difference Discretization Schemes for Diffusion in Spheres with Variable Diffusivity. Comput Chem Eng 71:241-252
Ford Versypt, Ashlee N; Pack, Daniel W; Braatz, Richard D (2013) Mathematical modeling of drug delivery from autocatalytically degradable PLGA microspheres--a review. J Control Release 165:29-37
Kishida, Masako; Ford Versypt, Ashlee N; Pack, Daniel W et al. (2013) Optimal Control of One-dimensional Cellular Uptake in Tissue Engineering. Optim Control Appl Methods 34:680-695
Xia, Yujie; Ribeiro, Pedro F; Pack, Daniel W (2013) Controlled protein release from monodisperse biodegradable double-wall microspheres of controllable shell thickness. J Control Release 172:707-14
Xu, Qingxing; Leong, Jiayu; Chua, Qi Yi et al. (2013) Combined modality doxorubicin-based chemotherapy and chitosan-mediated p53 gene therapy using double-walled microspheres for treatment of human hepatocellular carcinoma. Biomaterials 34:5149-62

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