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一种与成骨诱导性氧化甾醇脂质体集成的生物材料支架的开发,以增强 Hedgehog 信号和骨修复。

Development of a Biomaterial Scaffold Integrated with Osteoinductive Oxysterol Liposomes to Enhance Hedgehog Signaling and Bone Repair.

机构信息

Division of Advanced Prosthodontics, University of California, Los Angeles, California 90095, United States.

Department of Pathology, School of Medicine, Johns Hopkins University, Baltimore, Maryland 21205, United States.

出版信息

Mol Pharm. 2021 Apr 5;18(4):1677-1689. doi: 10.1021/acs.molpharmaceut.0c01136. Epub 2021 Mar 24.

DOI:10.1021/acs.molpharmaceut.0c01136
PMID:33760625
Abstract

Bone repair requires the tightly regulated control of multiple intrinsic and extrinsic cell types and signaling pathways. One of the positive regulatory signaling pathways in membranous and endochondral bone healing is the Hedgehog (Hh) signaling family. Here, a novel therapeutic liposomal delivery vector was developed by self-assembly of an Hh-activating cholesterol analog with an emulsifier, along with the addition of Smoothened agonist (SAG) as a drug cargo, for the enhancement of Hh signaling in bone regeneration. The drug-loaded nanoparticulate agonists of Hh signaling were immobilized onto trabecular bone-mimetic apatite-coated 3D scaffolds using bioinspired polydopamine adhesives to ensure favorable microenvironments for cell growth and local therapeutic delivery. Results showed that SAG-loaded liposomes induced a significant and dose-dependent increase in Hh-mediated osteogenic differentiation, as evidenced by analysis of bone marrow stromal cells, and calvarial bone healing, as evidenced using all radiographic parameters and histomorphometric analyses. Moreover, favorable outcomes were achieved in comparison to standards of care, including collagen sponge-delivered rBMP2 or allograft bone. In summary, this study demonstrates using a nanoparticle packaged Hh small molecule as a widely applicable bone graft substitute for robust bone repair.

摘要

骨修复需要多种内在和外在细胞类型和信号通路的严格调控。膜内和软骨内骨愈合中的一个正向调节信号通路是 Hedgehog(Hh)信号家族。在这里,通过将 Hh 激活胆固醇类似物与乳化剂自组装,同时添加作为药物有效成分的 Smoothened 激动剂(SAG),开发了一种新型治疗性脂质体递药载体,用于增强骨再生中的 Hh 信号。使用仿生聚多巴胺粘合剂将 Hh 信号的载药纳米颗粒激动剂固定在拟骨小梁状磷灰石涂层的 3D 支架上,以确保有利于细胞生长和局部治疗性递药的微环境。结果表明,SAG 负载的脂质体诱导了 Hh 介导的成骨分化的显著且剂量依赖性增加,这一点通过骨髓基质细胞分析得到了证实,并且使用所有放射影像学参数和组织形态计量学分析证实了颅顶骨愈合。此外,与包括胶原海绵递送的 rBMP2 或同种异体骨在内的对照治疗相比,取得了有利的结果。总之,本研究表明,使用纳米颗粒包裹的 Hh 小分子作为一种广泛适用的骨移植物替代物,可实现强大的骨修复。

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