A Dose‐Dependent Spatiotemporal Response of Angiogenesis Elicited by Zn Biodegradation during the Initial Stage of Bone Regeneration

Author:

Tan Junlong1ORCID,Li Shuang1,Sun Chaoyang1,Bao Guo2,Liu Meijing1,Jing Zehao3,Fu Hanwei4ORCID,Sun Yanhua5,Yang Qingmin5,Zheng Yufeng6,Wang Xiaogang1,Yang Hongtao1ORCID

Affiliation:

1. Key Laboratory of Big Data‐Based Precision Medicine School of Engineering Medicine Beihang University 37 Xueyuan Rd Beijing 100191 China

2. Department of Reproduction and Physiology National Research Institute for Family Planning Beijing 100081 China

3. Beijing Key Laboratory of Spinal Disease Research Engineering Research Center of Bone and Joint Precision Medicine Ministry of Education Department of Orthopedics Peking University Third Hospital Beijing 100191 P. R. China

4. School of Materials Science and Engineering Beihang University 37 Xueyuan Rd Beijing China

5. Shandong Provincial Key Laboratory of Microparticles Drug Delivery Technology Qilu Pharmaceutical Co. Ltd. Jinan 250100 China

6. Beijing Advanced Innovation Center for Materials Genome Engineering and School of Materials Science and Engineering Peking University Beijing 100871 China

Abstract

AbstractZinc (Zn) plays a crucial role in bone metabolism and imbues biodegradable Zn‐based materials with the ability to promote bone regeneration in bone trauma. However, the impact of Zn biodegradation on bone repair, particularly its influence on angiogenesis, remains unexplored. This study reveals that Zn biodegradation induces a consistent dose‐dependent spatiotemporal response in angiogenesis,both in vivo and in vitro. In a critical bone defect model, an increase in Zn release intensity from day 3 to 10 post‐surgery is observed. By day 10, the CD31‐positive area around the Zn implant significantly surpasses that of the Ti implant, indicating enhanced angiogenesis. Furthermore,angiogenesis exhibits a distance‐dependent pattern closely mirroring the distribution of Zn signals from the implant. In vitro experiments demonstrate that Zn extraction fosters the proliferation and migration of human umbilical vein endothelial cells and upregulates the key genes associated with tube formation, such as HIF‐1α and VEGF‐A, peaking at a concentration of 22.5 µM. Additionally, Zn concentrations within the range of 11.25−45 µM promote the polarization of M0‐type macrophages toward the M2‐type, while inhibiting polarization toward the M1‐type. These findings provide essential insights into the biological effects of Zn on bone repair, shedding light on its potential applications.

Funder

National Natural Science Foundation of China

Fundamental Research Funds for the Central Universities

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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