Endothelial stress induces the release of vitamin D-binding protein, a novel growth factor |
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Authors: | Raymond Marc-André Désormeaux Anik Labelle Andrée Soulez Mathilde Soulez Gilles Langelier Yves Pshezhetsky Alexey V Hébert Marie-Josée |
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Affiliation: | Research Centre CHUM, University of Montreal, 1560 Sherbrooke East, Montreal, Que., Canada H2L 4M1. |
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Abstract: | Endothelial cells (EC) under stress release paracrine mediators that facilitate accumulation of vascular smooth muscle cells (VSCM) at sites of vascular injury. We found that medium conditioned by serum-starved EC increase proliferation and migration of VSCM in vitro. Fractionation of the conditioned medium followed by mass spectral analysis identified one bioactive component as vitamin D-binding protein (DBP). DBP induced both proliferation and migration of VSMC in vitro in association with increased phosphorylation of ERK 1/2. PD 98059, a biochemical inhibitor of ERK 1/2, abrogated these proliferative and migratory responses in VSMC. DBP is an important carrier for the vitamin-D sterols, 25-hydroxyvitamin-D, and 1alpha,25-dihydroxyvitamin-D. Both sterols inhibited the activity of DBP on VSMC, suggesting that vitamin D binding sites are important for initiating the activities of DBP on VSMC. Release of DBP at sites of endothelial injury represents a novel pathway favoring accumulation of VSMC at sites of vascular injury. |
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Keywords: | Endothelial cell Vascular smooth muscle cells Vitamin-D binding protein Proliferation Migration ERK 1/2 Vitamin-D sterols |
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