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KMID : 1377020170140030297
Tissue Engineering and Regenerative Medicine
2017 Volume.14 No. 3 p.297 ~ p.306
Oligomeric Procyanidins (OPCs) Inhibit Procollagen Type I Secretion of Fibroblasts
Kim Byung-Jun

Park Jung-Keun
Kim Byeong-Kyu
Park Soo-Jin
Kim Min-Kyung
Lee Chang-Won
Choi La-Mee
Hur Ji-An
Kim Sang-Hyon
Beom Jae-Won
Kim Jung-Yoon
Oh Byung-Mo
Choi Tae-Hyun
Kim Suk-Wha
Abstract
Wound healing is composed of a complex process that requires harmonies of various cell populations where fibroblasts play the main role. Oligomeric procyanidins (OPC) are main components of grape (Vitis vinifera) seed extracts, and recent studies showed OPC¡¯s effects on inflammation, cell migration, and proliferation. We investigated the effect of OPC on fibroblasts to regulate wound healing process. Human dermal fibroblast known as Hs27 cells were treated with various concentrations of OPC (0, 2.5, 5, 10, and 20 ¥ìg/¥ìl). Cell cytotoxicity was evaluated by the Cell Counting Kit assay, and the expression levels of secreted procollagen were analyzed. Procollagen levels in OPC treated cells exposed to transforming growth factor beta 1 (TGF-¥â1) or ascorbic acid were evaluated using Western blot and immunocytochemistry. Relative mRNA expressions of procollagen, molecular chaperone such as HSP47, P4H were determined by real-time PCR in OPC treated cells. OPC showed no cytotoxicity on Hs27 cells at every concentration but inhibited procollagen secretion in a dose-dependent manner. The inhibitory effect also appeared under TGF-¥â1 induced collagen overproduction. Immunocytochemistry showed that higher levels of intracytoplasmic procollagen were accumulated in TGF-¥â1 treatment group, whereas ascorbic acid induced a release of accumulated procollagen under OPC treatment. The mRNA expressions of procollagen, molecular chaperone were not affected by OPC, but procollagen level was increased when exposed to TGF-¥â1. OPC inhibits procollagen secretion from fibroblasts with no effects on cell proliferations even under the environment of TGF-¥â1-induced collagen overproduction. OPC could regulate the diseases and symptoms of abnormal overabundant collagen production.
KEYWORD
Oligomeric procyanidins, Fibroblasts, Procollagen, Ascorbic acid, Vitis vinifera
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