The Bioactive Interface of Titanium Implant with Both Anti‐Oxidative Stress and Immunomodulatory Properties for Enhancing Osseointegration under Diabetic Condition

Author:

Wu Jianshuang12,Chen Maowen3,Xiao Yao2,Yang Huan2,Wang Gaoyang2,Zhang Xiaohong2,Dai Liangliang2,Yuan Zhang124ORCID

Affiliation:

1. Research & Development Institute of Northwestern Polytechnical University in Shenzhen Sanhang Science & Technology Building No. 45th, Gaoxin South 9th Road, Nanshan District Shenzhen Guangdong 518063 P. R. China

2. Xi'an Key Laboratory of Stem Cell and Regenerative Medicine Institute of Medical Research Northwestern Polytechnical University 127 West Youyi Road, Beilin District Xi'an Shaanxi 710072 P. R. China

3. School of Integrated Chinese and Western Medicine Anhui University of Chinese Medicine 81 Meishan Road Hefei Anhui 230012 P. R. China

4. Northwestern Polytechnical University Chongqing Technology Innovation Center 36 Pufu Road Chongqing 400000 P. R. China

Abstract

AbstractThe poor implant‐osseointegration under diabetic condition remains a challenge to be addressed urgently. Studies have confirmed that the diabetic pathological microenvironment is accompanied by excessive oxidative stress, imbalanced immune homeostasis, and persistent chronic inflammation, which seriously impairs the osteogenic process. Herein, a multifunctional bioactive interface with both anti‐oxidative stress and immunomodulatory properties is constructed on titanium implants. Briefly, manganese dioxide nanosheets are coated onto mesoporous polydopamine nanoparticles loaded with carbon monoxide gas precursor, namely MnO2‐CO@MPDA NPs, and then they are integrated on the titanium implant to obtain MCM‐Ti. In the simulated diabetic microenvironment, under the action of MnO2 nanoenzymes, MCM‐Ti can effectively eliminate intracellular reactive oxygen species while alleviating hypoxic state. Interestingly, the microenvironment mediates the responsive release of CO gas, which effectively drives macrophages toward M2 polarization, thereby ameliorating inflammatory response. The potential mechanism is that CO gas up‐regulates the expression of heme oxygenase‐1, further activating the Notch/Hes1/Stat3 signaling pathway. Furthermore, the conditioned medium derived from macrophages on MCM‐Ti surface significantly enhances the osteogenic differentiation of BMSCs. In a type 2 diabetic rat model, MCM‐Ti implant effectively alleviates the accompanying inflammation and enhances the osseointegration through the synergistic effects of resisting oxidative stress and remodeling immune homeostasis.

Funder

National Natural Science Foundation of China

Basic and Applied Basic Research Foundation of Guangdong Province

Natural Science Foundation of Chongqing Municipality

Key Research and Development Projects of Shaanxi Province

Publisher

Wiley

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