Abstract
Towards optimizing the growth of extracellular matrix to produce repair cartilage for healing articular cartilage (AC) defects in joints, scaffold-based tissue engineering approaches have recently become a focus of clinical research. Scaffold-based approaches by electrospinning aim to support the differentiation of chondrocytes by providing an ultrastructure similar to the fibrillar meshwork in native cartilage. In a first step, we demonstrate how the blending of chitosan with poly(ethylene oxide) (PEO) allows concentrated chitosan solution to become electrospinnable. The chitosan-based scaffolds share the chemical structure and characteristics of glycosaminoglycans, which are important structural components of the cartilage extracellular matrix. Electrospinning produced nanofibrils of ∼100 nm thickness that are closely mimicking the size of collagen fibrils in human AC. The polymer scaffolds were stabilized in physiological conditions and their stiffness was tuned by introducing the biocompatible natural crosslinker genipin. We produced scaffolds that were crosslinked with 1.0% genipin to obtain values of stiffness that were in between the stiffness of the superficial zone human AC of 600 ± 150 kPa and deep zone AC of 1854 ± 483 kPa, whereas the stiffness of 1.5% genipin crosslinked scaffold was similar to the stiffness of deep zone AC. The scaffolds were degradable, which was indicated by changes in the fibril structure and a decrease in the scaffold stiffness after seven months. Histological and immunohistochemical analysis after three weeks of culture with human articular chondrocytes (HACs) showed a cell viability of over 90% on the scaffolds and new extracellular matrix deposited on the scaffolds.
Highlights
Tissue engineering and regenerative medicine are concerned with the replacement or regeneration of cells, tissues, or organs to restore the normal biological function in the human body
Chitosan/poly(ethylene oxide) (PEO) blended at a ratio of 1:0.33 was electrospun into randomly oriented fibrils that are similar to the collagen fibril meshwork in native articular cartilage (AC)
The as-spun chitosan-PEO fibrils were stable in dry state, but they rapidly dissolved when transferred to an aqueous solution
Summary
Tissue engineering and regenerative medicine are concerned with the replacement or regeneration of cells, tissues, or organs to restore the normal biological function in the human body. The growth and remodeling of tissues are based on an ongoing, bidirectional interaction between cells and the extracellular matrix (ECM), in which the ECM exerts mechanical force directly on the cell membrane or indirectly putting force on the integrins. Both pathways are initiating cell-signaling cascades that produce changes in gene expressions, whereas cellular changes, in turn, affect the composition and structural arrangement of the ECM.[2,3] To regrow functional AC, it is, important to provide the cells with their appropriate microenvironment, including the ultrastructure, stiffness and growth factors to control the cell fate and direct tissue development. It is vital to provide the cells with a microenvironment that mimics the native AC and favours neo-cartilage growth.[5]
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