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Quercetin-3-O-β-D-glucuronide isolated from Polygonum aviculare in hibits cellular senescence in human primary cells
( Hyo Hyun Yang ) , ( Kyoung Hwangbo ) , ( Ming Shan Zhang ) , ( Jung Hee Cho ) , ( Jong Keun Park ) , ( Hwa Young Kim ) , ( Suk Hwan Baek ) , ( Hyung Chul Choi ) , ( So Young Park ) , ( Jae Ryong Kim )
UCI I410-ECN-0102-2015-500-002240660
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Cellular senescence is known to contribute to tissue aging, a variety of age-related diseases, tissue regeneration, and cancer. Therefore, aging intervention might be useful for prevention of aging as well as age-related disease. In this study, we investigated compounds from Polygonum aviculare to determine if they inhibited cellular senescence in human primary cells, human dermal fibroblasts (HDFs) and human umbilical vein endothelial cells (HUVECs). Ten compounds from P. aviculare were purified and their inhibitory effects on adriamycin-induced cellular senescence were measured by observing senescence-associated β-galactosidase (SA-β-gal) activity and reactive oxygen species. Among them, compound 9 (quercetin-3-O-β-D-glucuronide) showed inhibitory effects against cellular senescence in HDFs and HUVECs treated with adriamycin. Additionally, compound 9 rescued replicative senescence in HDFs and HUVECs. These data imply that compound 9 represses cellular senescence in human primary cells and might be useful for the development of dietary supplements or cosmetics that ameliorate tissue aging or aging-associated diseases.

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