3D-Printed Scaffolds for Ear Reconstruction Using Decellularized Human Cartilage-Derived Bioink and Polycaprolactone

去细胞化 聚己内酯 材料科学 3d打印 软骨 脚手架 生物医学工程 复合材料 解剖 工程类 医学 聚合物
作者
Jung Hwan Um,Ji Hwan Park,Tae Ho Kim,So Hyun Park,Je‐Ho Mun,Eun Hye Kang,Min Ji Kim,Kyung Hyun Min,Young Seok Kim,Tai Suk Roh,Kee-Won Lee,In Sik Yun
出处
期刊:ACS Biomaterials Science & Engineering [American Chemical Society]
标识
DOI:10.1021/acsbiomaterials.4c01990
摘要

Reconstructing auricular tissue is challenging because ear cartilage has few blood vessels and limited regenerative capacity. Traditional methods that utilize autologous costal cartilage or synthetic polymers often lead to donor site morbidity and suboptimal biocompatibility. In this study, we introduce 3D-printed scaffolds composed of decellularized human cartilage-derived bioink combined with polycaprolactone (PCL), designed to enhance both tissue regeneration and mechanical stability. The decellularization process effectively removed cellular components while preserving glycosaminoglycan and total collagen, comparable to those in native cartilage. We formulated the bioink by incorporating decellularized human cartilage particles into hyaluronic acid and carboxymethyl cellulose gels, optimizing the rheological properties for 3D printing. In vitro tests demonstrated that the decellularized human cartilage-derived bioink exhibited no cytotoxicity and facilitated the migration and chondrogenic differentiation of human adipose-derived stem cells. We fabricated 3D-printed scaffolds using this bioink combined with PCL and evaluated their performance in rabbits over a one-year implantation period. Our results indicated that the scaffolds maintained structural integrity throughout the year and exhibited significant neovascularization and chondrogenesis. Histological analysis revealed increased blood vessel formation in scaffolds with higher ratios and greater decellularized cartilage content with notable differences observed across varying porosities. These findings suggest that 3D-printed scaffolds with decellularized human cartilage-derived bioink and PCL offer a promising approach for auricular reconstruction, potentially improving outcomes for patients with microtia.
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