Biphasic biomimetic scaffolds based on a regionally decalcified bone framework and pre-chondrogenic microspheres for osteochondral defect repair

IF 10.2 1区 医学 Q1 ENGINEERING, BIOMEDICAL Materials Today Bio Pub Date : 2025-04-01 Epub Date: 2025-01-13 DOI:10.1016/j.mtbio.2025.101494
Zhuo Liang , Qingqing Pan , Fei Xue , Jingdi Zhang , Zhenlin Fan , Weiyun Wang , Xueqiang Guo , Zhuang Qian , Yaping Shen , Wenjuan Song , Lei Wang , Guangdong Zhou , Yong He , Wenjie Ren
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Abstract

Osteochondral defects are still facing a significant challenge in clinical surgery, making post-trauma repair difficult. Tissue engineering has provided a promising approach to solving these defects. However, existing scaffolds cannot replicate the complex biphasic cartilage-bone microenvironment with accuracy. We aimed to develop a biphasic biomimetic scaffold with regionally regulated vascularization that promoted chondrogenesis and osteogenesis through bidirectional regulation of endochondral ossification. This scaffold consisted of pre-chondrogenic microspheres (PCMs) and a decalcified bone frame prepared by decalcifying the cartilage layer and bone layer of the scaffold to varying degrees. Incorporation of PCMs into the cartilage layer created a microenvironment that promoted cartilage regeneration while axitinib was modified to inhibit vascularization and enhance cartilage regeneration. The bone layer provided a microenvironment that promoted endochondral ossification and facilitated bone repair. In vitro studies have shown that axitinib-modified cartilage layers significantly inhibit the VEGF expression of pre-chondrogenic cells, while decalcified bone powder from the bone layer significantly promotes the ossification of PCMs. In vivo experiments indicated that this decalcified bone frame controls the endochondral ossification of PCMs through regionalized angiogenesis, promoting the integrated regeneration and reconstruction of osteochondral defects in rabbit knee joints. These results suggest that our designed demineralized bone frame can precisely engineer the osteochondral regeneration microenvironment, providing theoretical guidance for the integrated regeneration and repair of anisotropic tissue injuries.

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基于局部脱钙骨框架和软骨前微球的双相仿生支架用于骨软骨缺损修复。
骨软骨缺损在临床手术中仍面临重大挑战,给创伤后修复带来困难。组织工程为解决这些缺陷提供了一种很有前途的方法。然而,现有的支架不能准确地复制复杂的双相软骨-骨微环境。我们的目标是开发一种具有区域调节血管形成的双相仿生支架,通过双向调节软骨内成骨来促进软骨形成和成骨。该支架由成软骨前微球(PCMs)和脱钙骨框架组成,通过对支架的软骨层和骨层进行不同程度的脱钙制备。将PCMs掺入软骨层创造了促进软骨再生的微环境,而阿西替尼则被修饰为抑制血管形成并增强软骨再生。骨层提供了促进软骨内成骨和促进骨修复的微环境。体外研究表明,阿西替尼修饰的软骨层可显著抑制软骨前细胞VEGF的表达,而骨层脱钙骨粉可显著促进pcm的骨化。体内实验表明,该脱钙骨框架通过区域化血管生成控制pcm软骨内成骨,促进兔膝关节骨软骨缺损的整体再生重建。这些结果表明,我们设计的脱矿骨框架可以精确地工程化骨软骨再生微环境,为各向异性组织损伤的综合再生和修复提供理论指导。
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来源期刊
CiteScore
8.30
自引率
4.90%
发文量
303
审稿时长
30 days
期刊介绍: Materials Today Bio is a multidisciplinary journal that specializes in the intersection between biology and materials science, chemistry, physics, engineering, and medicine. It covers various aspects such as the design and assembly of new structures, their interaction with biological systems, functionalization, bioimaging, therapies, and diagnostics in healthcare. The journal aims to showcase the most significant advancements and discoveries in this field. As part of the Materials Today family, Materials Today Bio provides rigorous peer review, quick decision-making, and high visibility for authors. It is indexed in Scopus, PubMed Central, Emerging Sources, Citation Index (ESCI), and Directory of Open Access Journals (DOAJ).
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