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ABSTRACT: Saccharide-peptide hydrogels have been developed in our laboratory as new synthetic extracellular matrices for regenerative medicine applications. In this work, we have expanded on our previously reported system and applied copolymerization of cysteine (Cys) and vinyl sulfone (VS)-functionalized saccharide-peptide polymers via Michael-type addition for encapsulation and 3D culture of cells. Specifically, our aims were to (1) develop a novel hydrogel platform, which could be applied for encapsulating and culturing mesenchymal stem cells (MSCs) in a 3D environment, (2) characterize the tunable properties of the hydrogel, specifically, degradation, mechanical, and gel network properties, and (3) determine the biocompatibility of the saccharide-peptide hydrogel material with MSCs. Hydrogel mechanical properties were tunable by varying the VS:Cys ratio (= 0.5, 1, or 2) as well as the pH (6, 7, or 8) of the cross-linking components. Stiffer gels were formed at VS:Cys = 1 and pH 6 or 7. Gels formed at pH 8 or with excess Cys (VS:Cys = 0.5) or VS (VS:Cys = 2) were significantly softer. Cross-linking pH and VS:Cys ratio also had an effect on the degradation behavior of the VS:Cys gels, with higher cross-linking pH resulting in an accelerated loss of mass. On the basis of environmental scanning electron microscopy (ESEM) analysis and fluorescence microscopy, all hydrogels appeared to exhibit porous gel networks. MSCs cultured in monolayer and exposed to soluble Cys or VS copolymers (0.1-5 mg/mL) did not exhibit measurable cytotoxicity. In addition, MSCs were cultured in 3D for up to 14 days in vitro without deleterious effects on cell viability. In summary, we have established and characterized a tunable 3D saccharide-peptide hybrid copolymer hydrogel platform for culturing MSCs. Future studies will focus on utilizing the hydrogel system for controlling the differentiation of MSCs.
Biomacromolecules 02/2011; 12(3):560-7. · 5.48 Impact Factor
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ABSTRACT: A new class of functional saccharide-peptide copolymer-based hydrogels was synthesized and investigated as synthetic extracellular matrices for regenerative medicine applications. The polymer was composed entirely of natural building blocks, namely, galactaric acid and lysine on the backbone, with tyrosine grafted onto the side chain as a handle for enzyme-catalyzed hydrogelation. The resulting hydrogels are degradable under simulated physiological conditions and exhibit minimal cytotoxicity on dermal fibroblast and PC-12 cells. As a demonstration of the versatility of the system, the mechanical properties of the gels can be independently controlled without changing the polymer chemical composition. Using an identical copolymer solution, by simply allowing different lengths of cross-linking time, a series of hydrogels was obtained with different mechanical moduli at constant chemical structure. The moduli of the resulting hydrogels varied stepwise from 1.7, 4.1, 6.9, and 12.5 kPa to allow for systematic studies on the effects of modulus on cell behavior. It was exciting to observe that a simple change in hydrogel physical properties could induce a direct phenotypic change in cell adhesion and proliferation. Depending on the substrate mechanical modulus, the cell morphology changed and proliferation rate differed by an order of magnitude for different cell lines. These data suggest our saccharide-peptide hydrogels as promising synthetic extracellular matrices for cell culture and tissue regeneration.
Journal of the American Chemical Society 11/2009; 131(48):17638-46. · 9.91 Impact Factor
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ABSTRACT: Changes in dimensional and mechanical properties of degradable sheaths in poly lactic-co glycolic acid (PLGA) have been researched extensively. Composite PLGA having variable resorption rates in multiple layers under physiological loading has not been reported. Our novel design of a PLGA sheath is composed of 3 layers with different degradation rates (i.e., the innermost layer degrades the fastest, followed by the middle, while the outer layer degrades the slowest). In the presence of physiological luminal pressure, diameter is greater, thickness is less, resorption rate is greater, pore size is greater, and incremental modulus is greater than in nonpressurized sheaths. Furthermore, the ratio of the pore size to the sheath radius affects the dimensional changes of the sheath in the radial direction. In addition to changing the pore size-to-sheath radius ratio, the dimensional changes can be manipulated by choosing different glycolic and lactic acid ratios for the different layers. The application of this novel PLGA design for gradual arterialization of vein grafts is contemplated.
Tissue Engineering 01/2008; 13(12):2855-62. · 4.02 Impact Factor
