Abstract
Collagen hydrogels are among the most well-studied platforms for drug delivery and in situ tissue engineering, thanks to their low cost, low immunogenicity, versatility, biocompatibility, and similarity to the natural extracellular matrix (ECM). Despite collagen being largely responsible for the tensile properties of native connective tissues, collagen hydrogels have relatively low mechanical properties in the absence of covalent cross-linking. This is particularly problematic when attempting to regenerate stiffer and stronger native tissues such as bone. Furthermore, in contrast to hydrogels based on ECM proteins such as fibronectin, collagen hydrogels do not have any growth factor (GF)-specific binding sites and often cannot sequester physiological (small) amounts of the protein. GF binding and in situ presentation are properties that can aid significantly in the tissue regeneration process by dictating cell fate without causing adverse effects such as malignant tumorigenic tissue growth. To alleviate these issues, researchers have developed several strategies to increase the mechanical properties of collagen hydrogels using physical or chemical modifications. This can expand the applicability of collagen hydrogels to tissues subject to a continuous load. GF delivery has also been explored, mathematically and experimentally, through the development of direct loading, chemical cross-linking, electrostatic interaction, and other carrier systems. This comprehensive article explores the ways in which these parameters, mechanical properties and GF delivery, have been optimized in collagen hydrogel systems and examines their in vitro or in vivo biological effect. This article can, therefore, be a useful tool to streamline future studies in the field, by pointing researchers into the appropriate direction according to their collagen hydrogel design requirements.
Highlights
Collagen is the most abundant protein in the animal kingdom and is a key component of the extracellular matrix (ECM)
Physical cross-linking Collagen I monomers self-assemble into fibrillar structures that may cross-link and/or entangle to form viscoelastic gels with varied network structures and mechanical properties in a process known as fibrillogenesis, that is generally accompanied by an increase in turbidity [51, 52]
This promoted an increase in viability, invasion, and assembly of endothelial cells into the collagen hydrogel compared with the no vascular endothelial growth factor (VEGF) and soluble VEGF groups
Summary
Collagen is the most abundant protein in the animal kingdom and is a key component of the extracellular matrix (ECM). Collagen is and cheaply isolated from tissues such as skin, tendon, pericardium, and other and is widely used as a biomaterial, such as hydrogels (materials with a water content >90%), for tissue regeneration. It is extracted from bovine, porcine, or rat specimens and from marine or recombinant sources [3]. We will overview the various techniques used to produce collagen hydrogels with varying mechanical and degradation properties for different tissue engineering applications. Given that collagen is an important biomaterial used extensively in tissue engineering, this article is important in guiding future research in the field
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