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Engineering cryoelectrospun elastin-alginate scaffolds to serve as stromal extracellular matrices

弹性蛋白 细胞外基质 脚手架 组织工程 去细胞化 自愈水凝胶 材料科学 生物医学工程 粘弹性 纳米技术 化学 复合材料 高分子化学 生物化学 医学 病理
作者
Pujhitha Ramesh,Nicholas Moskwa,Zachary Hanchon,Adam Koplas,Deirdre A. Nelson,Kristen L. Mills,James Castracane,Melinda Larsen,Susan T. Sharfstein,Yubing Xie
出处
期刊:Biofabrication [IOP Publishing]
卷期号:14 (3): 035010-035010 被引量:5
标识
DOI:10.1088/1758-5090/ac6b34
摘要

Abstract Scaffold-based regenerative strategies that emulate physical, biochemical, and mechanical properties of the native extracellular matrix (ECM) of the region of interest can influence cell growth and function. Existing ECM-mimicking scaffolds, including nanofiber (NF) mats, sponges, hydrogels, and NF-hydrogel composites are unable to simultaneously mimic typical composition, topography, pore size, porosity, and viscoelastic properties of healthy soft-tissue ECM. In this work, we used cryoelectrospinning to fabricate 3D porous scaffolds with minimal fibrous backbone, pore size and mechanical properties similar to soft-tissue connective tissue ECM. We used salivary glands as our soft tissue model and found the decellularized adult salivary gland (DSG) matrix to have a fibrous backbone, 10–30 μ m pores, 120 Pa indentation modulus, and ∼200 s relaxation half time. We used elastin and alginate as natural, compliant biomaterials and water as the solvent for cryoelectrospinning scaffolds to mimic the structure and viscoelasticity of the connective tissue ECM of the DSG. Process parameters were optimized to produce scaffolds with desirable topography and compliance similar to DSG, with a high yield of >100 scaffolds/run. Using water as solvent, rather than organic solvents, was critical to generate biocompatible scaffolds with desirable topography; further, it permitted a green chemistry fabrication process. Here, we demonstrate that cryoelectrospun scaffolds (CESs) support penetration of NIH 3T3 fibroblasts 250–450 µ m into the scaffold, cell survival, and maintenance of a stromal cell phenotype. Thus, we demonstrate that elastin-alginate CESs mimic many structural and functional properties of ECM and have potential for future use in regenerative medicine applications.

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