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Poly-D,L-Lactic Acid Filler Increases Extracellular Matrix by Modulating Macrophages and Adipose-Derived Stem Cells in Aged Animal Skinopen access

Authors
Oh, SeyeonSeo, Suk BaeKim, GunpoongBatsukh, SosorburamPark, Chul-HyunSon, Kuk HuiByun, Kyunghee
Issue Date
Jun-2023
Publisher
MDPI
Keywords
aged skin; NRF2; macrophage; collagen; elastic fiber
Citation
ANTIOXIDANTS, v.12, no.6
Journal Title
ANTIOXIDANTS
Volume
12
Number
6
URI
https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/88544
DOI
10.3390/antiox12061204
ISSN
2076-3921
Abstract
Poly-D,L-lactic acid (PDLLA) filler corrects soft tissue volume loss by increasing collagen synthesis in the dermis; however, the mechanism is not fully understood. Adipose-derived stem cells (ASCs) are known to attenuate the decrease in fibroblast collagen synthesis that occurs during aging, and nuclear factor (erythroid-derived 2)-like-2 factor (NRF2) increases ASCs survival by inducing M2 macrophage polarization and IL-10 expression. We evaluated the ability of PDLLA to induce collagen synthesis in fibroblasts by modulating macrophages and ASCs in a H2O2-induced cellular senescence model and aged animal skin. PDLLA increased M2 polarization and NRF2 and IL-10 expression in senescence-induced macrophages. Conditioned media from senescent macrophages treated with PDLLA (PDLLA-CMM & phi;) reduced senescence and increased proliferation and expression of transforming growth factor-& beta; (TGF-& beta;) and fibroblast growth factor (FGF) 2 in senescence-induced ASCs. Conditioned media from senescent ASCs treated with PDLLA-CMM & phi; (PDLLA-CMASCs) increased the expression of collagen 1a1 and collagen 3a1 and reduced the expression of NF-& kappa;B and MMP2/3/9 in senescence-induced fibroblasts. Injection of PDLLA in aged animal skin resulted in increased expression of NRF2, IL-10, collagen 1a1, and collagen 3a1 and increased ASCs proliferation in aged animal skin. These results suggest that PDLLA increases collagen synthesis by modulating macrophages to increase NRF2 expression, which stimulates ASCs proliferation and secretion of TGF-& beta; and FGF2. This leads to increased collagen synthesis, which can attenuate aging-induced soft tissue volume loss.
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