材料科学
多孔性
纳米技术
生物物理学
复合材料
生物
作者
Shuang Li,Hongtao Yang,Xinhua Qu,Yu Qin,Aobo Liu,Guo Bao,He Huang,Chaoyang Sun,Jiabao Dai,Junlong Tan,Jiahui Shi,Yan Guan,Wei Pan,Xuenan Gu,Bo Jia,Peng Wen,Xiaogang Wang,Yufeng Zheng
标识
DOI:10.1038/s41467-024-47189-5
摘要
Abstract Reconciling the dilemma between rapid degradation and overdose toxicity is challenging in biodegradable materials when shifting from bulk to porous materials. Here, we achieve significant bone ingrowth into Zn-based porous scaffolds with 90% porosity via osteoinmunomodulation. At microscale, an alloy incorporating 0.8 wt% Li is employed to create a eutectoid lamellar structure featuring the LiZn 4 and Zn phases. This microstructure optimally balances high strength with immunomodulation effects. At mesoscale, surface pattern with nanoscale roughness facilitates filopodia formation and macrophage spreading. At macroscale, the isotropic minimal surface G unit exhibits a proper degradation rate with more uniform feature compared to the anisotropic BCC unit. In vivo, the G scaffold demonstrates a heightened efficiency in promoting macrophage polarization toward an anti-inflammatory phenotype, subsequently leading to significantly elevated osteogenic markers, increased collagen deposition, and enhanced new bone formation. In vitro, transcriptomic analysis reveals the activation of JAK/STAT pathways in macrophages via up regulating the expression of Il-4 , Il-10 , subsequently promoting osteogenesis.
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