Selenium-Doped Mesoporous
Bioactive Glass Regulates
Macrophage Metabolism and Polarization by Scavenging ROS and Promotes
Bone Regeneration In Vivo
Posted on 2023-07-05 - 12:43
Bone regeneration is complex and involves multiple cells
and systems,
with macrophage-mediated immune regulation being critical for the
development and regulation of inflammation, angiogenesis, and osteogenesis.
Biomaterials with modified physical and chemical properties (e.g., modified wettability and morphology) effectively regulate
macrophage polarization. This study proposes a novel approach to macrophage-polarization
induction and -metabolism regulation through selenium (Se) doping.
We synthesized Se-doped mesoporous bioactive glass (Se-MBG) and demonstrated
its macrophage-polarization regulation toward M2 and its enhancement
of the macrophage oxidative phosphorylation metabolism. The underlying
mechanism is the effective scavenging of excessive intracellular reactive
oxygen species (ROS) by the Se-MBG extracts through the promotion
of peroxide-scavenging enzyme glutathione peroxidase 4 expression
in the macrophages; this, in turn, improves the mitochondrial function.
Printed Se-MBG scaffolds were implanted into rats with critical-sized
skull defects to evaluate their immunomodulatory and bone regeneration
capacity in vivo. The Se-MBG scaffolds demonstrated
excellent immunomodulatory function and robust bone regeneration capacity.
Macrophage depletion with clodronate liposomes impaired the Se-MBG-scaffold
bone regeneration effect. Se-mediated immunomodulation, which targets
ROS scavenging to regulate macrophage metabolic profiles and mitochondrial
function, is a promising concept for future effective biomaterials
for bone regeneration and immunomodulation.
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Chen, Ding; Liang, Zitian; Su, Zhikang; Huang, Jiangyong; Pi, Yixing; Ouyang, Yuanting; et al. (1753). Selenium-Doped Mesoporous
Bioactive Glass Regulates
Macrophage Metabolism and Polarization by Scavenging ROS and Promotes
Bone Regeneration In Vivo. ACS Publications. Collection. https://doi.org/10.1021/acsami.3c03446Â