Harnessing Thrombospondin‐1‐Enabled Decellularized Nucleus Pulposus Matrices and Elastin‐Like Recombinamers to Rebuild an Avascular Analogue of the Intervertebral Disc

去细胞化 血管生成 材料科学 生物材料 自愈水凝胶 弹性蛋白 生物医学工程 椎间盘 生物物理学 体内 细胞外基质 新生血管 生物相容性 脚手架 化学 解剖 纳米技术 生物化学 病理 生物 高分子化学 医学 生物技术 癌症研究 冶金
作者
C.M. Botelho,José Carlos Rodríguez‐Cabello,Mário A. Barbosa
出处
期刊:Journal of Biomedical Materials Research Part A [Wiley]
卷期号:113 (5)
标识
DOI:10.1002/jbm.a.37911
摘要

ABSTRACT With the degeneration of the intervertebral disc (IVD), the ingrowth of vascular and neural structures occurs. Both nerves and blood vessels engage in the development of inflammation and the onset of discogenic pain. The present study aimed to produce a hierarchical biomaterial capable of inhibiting angiogenesis by emulating the microenvironment of non‐degenerated IVDs. To this end, we have incorporated an angiogenesis modulator—thrombospondin‐1 (TSP‐1) into a three‐dimensional (3D) hydrogel network containing decellularized nucleus pulposus (dNPs) and azide‐cyclooctyne modified elastin‐like recombinamers (ELRs). Following the decellularization of nucleus pulposus (NPs) isolated from bovine tissues, pre‐gels (pGs) were assembled based on the acid‐pepsin extraction of soluble collagens found in the dNPs. Given the inherent affinity of these macromolecules to TSP‐1, which was corroborated by immunohistochemical analysis and FT‐IR spectroscopy, the pGs were supplemented with two concentrations of TSP‐1. Angiogenesis was evaluated using the chick chorioallantoic membrane (CAM) in vivo model. Conjugation of TSP‐1 with the pGs resulted in a synergistic suppression of blood vessel formation. Complexation with the ELRs improved the viscoelastic moduli and the structural stability of the hydrogels, which maintained their hydration and osmolarity properties due to the presence of the dNPs. When placed in direct contact with human primary fibroblasts, the materials displayed high cytocompatibility and tunable degradation rates. Our findings indicate that TSP‐1‐enabled dNP‐derived pGs inhibit angiogenesis in vivo, while the presence of the ELRs aids in improving the mechanical properties of the hydrogels, thus providing a platform for rebuilding an avascular analogue of the healthy IVD.
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