[No authors listed]
Secreted frizzled-related protein 5 (SFRP5) is one of the anti-inflammatory adipokines secreted from white adipose tissue. However, little is known about the effect of SFRP5 on the cardiovascular system. The aim of the present study was to determine the effect of SFRP5 on smooth muscle cell (SMC) proliferation, migration and inflammation. The plasma levels of SFRP5 were evaluated in a cohortâbased elderly population using ELISA, and the expression of SFRP5 in SpragueâDawley rat aortas was detected using immunohistochemistry. SMC proliferation and migration were evaluated in vitro using 5âethynylâ2'âdeoxyuridine cell proliferation and woundâhealing assays, respectively, while reactive oxygen species production and cell signaling were assessed using a 2',7'âdichlorodihydrofluorescein diacetate assay and immunoblotting, respectively. The results revealed that plasma levels of SFRP5 were positively correlated with age in the elderly Chinese cohort. Similarly, aorta SFRP5 expression was significantly higher in 15âmonthâold rats compared with 6âmonthâold rats. In vitro, SFRP5 significantly inhibited rat aortic SMC proliferation and migration that were induced by plateletâderived growth factor (PDGF)âBB, as well as inhibiting generation. Compared with the effect of PDGFâBB on SMCs, SFRP5 at 100 and 200 ng/ml significantly decreased SMC proliferation by 31.5 and 34.8%, respectively (P<0.05). SFRP5 at 100 and 200 ng/ml also inhibited the migration of SMCs by 24.9 and 28.4%, respectively, when compared with the effects of PDGFâBB. SFRP5 attenuated the PDGFâBBâinduced expression of βâcatenin and proliferating cell nuclear antigen, while p38 phosphorylation was significantly attenuated. Together, the present results suggested that SFRP5 may inhibit SMC proliferation, migration and inflammation by suppressing the Wnt/βâcatenin and p38/mitogenâactivated protein kinase signaling pathways.
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