Matrix stiffness regulates neovascular homeostasis through autophagy in nude mice

Author:

Wang Bingqing12ORCID,Yang Yuqing12,Wang Yichen2,Yang Yanxin2,Li Yi2,Hu Chenxi2,Xue Changyue123

Affiliation:

1. Department of Oral Implantology The Affiliated Stomatological Hospital of Nanjing Medical University Nanjing China

2. Jiangsu Key Laboratory of Oral Diseases Nanjing Medical University Nanjing China

3. Jiangsu Province Engineering Research Center of Stomatological Translational Medicine Nanjing Medical University Nanjing China

Abstract

AbstractOne of the major obstacles to the effective application of vascularized fruit is an insufficient understanding of the relationship between the microenvironment and neovascular homeostasis. The role of extracellular matrix stiffness in regulating the structural and functional stability of neovascularization has not yet been elucidated. This study explored the effects of matrix stiffness on neovascular homeostasis in nude mice. Dextran hydrogels with three different stiffnesses were separately combined with mouse bone marrow‐derived endothelial progenitor cells (EPCs) and subcutaneously implanted into the backs of nude mice. After 14 days, neovascular homeostasis indicators in the different groups were measured. Cell autophagy levels were evaluated, and inhibitor assays were performed to explore the underlying mechanism. New blood vessels were generated in the three stiffnesses of the EPC‐loaded dextran hydrogels 14 days after implantation. The newly formed vessels tended to have better structural stability in softer hydrogels. Endothelial function markers, such as endothelial nitric oxide synthase and E‐selectin, were downregulated as the matrix stiffness increased. Furthermore, we found that cell autophagy levels decreased in stiffer matrices, and autophagy inhibition attenuated neovascular homeostasis. A soft matrix is conducive to maintaining neovascular homeostasis through autophagy in nude mice.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

Cell Biology,Clinical Biochemistry,Physiology

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