Extracellular Matrix‐Mimetic Immunomodulatory Hydrogel for Accelerating Wound Healing

Author:

Wang Honglei1,Huang Runzhi2,Bai Long3,Cai Yixin1,Lei Miao1,Bao Chunyan4,Lin Shaoliang1,Ji Shizhao2,Liu Changsheng1,Qu Xue156ORCID

Affiliation:

1. Key Laboratory for Ultrafine Materials of Ministry of Education School of Material Science and Engineering Frontiers Science Center for Materiobiology and Dynamic Chemistry East China University of Science and Technology Shanghai 200237 China

2. Department of Burn Surgery Institute of Burns Changhai Hospital The Second Military Medical University Shanghai 200433 China

3. Organoid Research Center Institute of Translational Medicine Shanghai University Shanghai 200444 China

4. Key Laboratory for Advanced Materials Institute of Fine Chemical School of Chemistry and Molecular Engineering East China University of Science and Technology Shanghai 200237 China

5. Wenzhou Institute of Shanghai University Wenzhou 325000 China

6. Shanghai Frontier Science Center of Optogenetic Techniques for Cell Metabolism Shanghai 200237 China

Abstract

AbstractMacrophages play a crucial role in the complete processes of tissue repair and regeneration, and the activation of M2 polarization is an effective approach to provide a pro‐regenerative immune microenvironment. Natural extracellular matrix (ECM) has the capability to modulate macrophage activities via its molecular, physical, and mechanical properties. Inspired by this, an ECM‐mimetic hydrogel strategy to modulate macrophages via its dynamic structural characteristics and bioactive cell adhesion sites is proposed. The LZM‐SC/SS hydrogel is in situ formed through the amidation reaction between lysozyme (LZM), 4‐arm‐PEG‐SC, and 4‐arm‐PEG‐SS, where LZM provides DGR tripeptide for cell adhesion, 4‐arm‐PEG‐SS provides succinyl ester for dynamic hydrolysis, and 4‐arm‐PEG‐SC balances the stability and dynamics of the network. In vitro and subcutaneous tests indicate the dynamic structural evolution and cell adhesion capacity promotes macrophage movement and M2 polarization synergistically. Comprehensive bioinformatic analysis further confirms the immunomodulatory ability, and reveals a significant correlation between M2 polarization and cell adhesion. A full‐thickness wound model is employed to validate the induced M2 polarization, vessel development, and accelerated healing by LZM‐SC/SS. This study represents a pioneering exploration of macrophage modulation by biomaterials’ structures and components rather than drug or cytokines and provides new strategies to promote tissue repair and regeneration.

Funder

National Key Research and Development Program of China

National Natural Science Foundation of China

Higher Education Discipline Innovation Project

Science and Technology Commission of Shanghai Municipality

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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