A glycosidic spinasterol from Koreana stewartia promotes procollagen production and inhibits matrix metalloproteinase-1 expression in UVB-irradiated human dermal fibroblasts.

Tae Hoon Lee, Sang Min Lee, Dae-Young Lee, Youngsook Son, Dae Kyun Chung, Nam-In Baek, Jiyoung Kim

Graduate School of Biotechnology and College of Life Science, Kyung Hee University, Korea.

Journal Article: Biological & Pharmaceutical Bulletin (impact factor: 1.81). 01/2011; 34(5):768-73.

Abstract

Methanol extract of Koreana stewartia leaves (SKE) stimulated collagen production in ultraviolet-B (UVB)-irradiated human fibroblast cells. An active compound was isolated from SKE by successive partitioning and chromatography, and the chemical structure was determined to be 3-O-β-D-glucopyranosylspinasterol (spinasterol-Glc) by spectroscopic characterization. Spinasterol-Glc increased collagen production in the supernatant of UVB-irradiated dermal fibroblast cell cultures in a dose-dependent manner. The effects of spinasteol-Glc on expression of procollagen and matrix metalloproteinase-1 (MMP-1) were further evaluated. We found that the compound stimulated collagen production in UVB-treated fibroblasts than in vehicle-treated control cells by about 3-fold. In addition, we also demonstrate that the compound increased the mRNA and protein levels of procollagen in UVB-treated fibroblast cells, while it inhibited expression of MMP-1. These results indicate that spinasterol-Glc protects fibroblast cells from the adverse effects of UV radiation via stimulation of procollagen synthesis as well as inhibition of MMP-1 expression. Spinasterol-Glc may be useful in the future development of therapeutic and cosmetic applications.

Source: PubMed

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Keywords

active compound
 
adverse effects
 
chromatography
 
collagen production
 
cosmetic applications
 
dose-dependent manner
 
fibroblast cells
 
future development
 
Koreana stewartia
 
matrix metalloproteinase-1
 
MMP-1 expression
 
procollagen
 
procollagen synthesis
 
spectroscopic characterization
 
UV radiation
 
UVB)-irradiated human fibroblast cells
 
UVB-irradiated dermal fibroblast cell cultures
 
UVB-treated fibroblast cells
 
UVB-treated fibroblasts
 
vehicle-treated control cells