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      Cell-Matrix Interactions in the Genesis of Arteriosclerosis and Atheroma. : Effect of Aging

      , ,
      Annals of the New York Academy of Sciences
      Wiley

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          The elastin receptor: a galactoside-binding protein.

          The elastin receptor complex contains a component of 67 kilodaltons that binds to a glycoconjugate affinity column containing beta-galactoside residues and is eluted from this column with lactose. This protein component is also released from the surface of cultured chondroblasts by incubation with lactose, and its association with immobilized elastin is inhibited by lactose. Since lactose also blocks elastic fiber formation by cultured chondroblasts, the galactoside-binding property of the elastin receptor is implicated in this process.
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            Effect of elastin peptides on ion fluxes in mononuclear cells, fibroblasts, and smooth muscle cells.

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              Effect of elastin peptides on human monocytes: Ca2+ mobilization, stimulation of respiratory burst and enzyme secretion.

              The effect of elastin peptides (Kappa-elastin) was investigated on human monocytes. The data presented here indicate that elastin peptides increase the intracellular Ca2+ level measured by Quin 2 fluorescence and mediate the release of beta glucuronidase and elastase. The O2 consumption and H2O2 release were stimulated in a dose-dependent manner. The early rise of cAMP was followed by a return to the original level at 30 min and by a concomitant increase of cGMP level. The action of elastin peptides on intracellular calcium level and cGMP levels may well be related to its previously demonstrated chemotactic activity. These activities may well play a role in the modifications of the extracellular matrix following elastin degradation as observed in atherosclerosis, emphysema and aging.
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                Author and article information

                Journal
                Annals of the New York Academy of Sciences
                Ann NY Acad Sci
                Wiley
                0077-8923
                1749-6632
                December 1992
                December 1992
                : 673
                : 1 Physiopatholo
                : 331-341
                Article
                10.1111/j.1749-6632.1992.tb27468.x
                2ff1427e-4496-4f13-8d61-a99e7a76ccee
                © 1992

                http://doi.wiley.com/10.1002/tdm_license_1.1

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