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Am J Physiol Regul Integr Comp Physiol 281: R803-R810, 2001;
0363-6119/01 $5.00
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Vol. 281, Issue 3, R803-R810, September 2001

Volume-activated trimethylamine oxide efflux in red blood cells of spiny dogfish (Squalus acanthias)

Dana-Lynn T. Koomoa1,2, Mark W. Musch2,3, Ainsley Vaz MacLean1,2, and Leon Goldstein1,2

1 Division of Biology and Medicine, Brown University, Providence, Rhode Island 02912; 3 Department of Medicine, Inflammatory Bowel Disease Research Center, University of Chicago, Chicago, Illinois 60637; and 2 Mount Desert Island Biological Laboratory, Salisbury Cove, Maine 04672

The aims of this study were to determine the pathway of swelling-activated trimethylamine oxide (TMAO) efflux and its regulation in spiny dogfish (Squalus acanthias) red blood cells and compare the characteristics of this efflux pathway with the volume-activated osmolyte (taurine) channel present in erythrocytes of fishes. The characteristics of the TMAO efflux pathway were similar to those of the taurine efflux pathway. The swelling-activated effluxes of both TMAO and taurine were significantly inhibited by known anion transport inhibitors (DIDS and niflumic acid) and by the general channel inhibitor quinine. Volume expansion by hypotonicity, ethylene glycol, and diethyl urea activated both TMAO and taurine effluxes similarly. Volume expansion by hypotonicity, ethylene glycol, and diethyl urea also stimulated the activity of tyrosine kinases p72syk and p56lyn, although the stimulations by the latter two treatments were less than by hypotonicity. The volume activations of both TMAO and taurine effluxes were inhibited by tyrosine kinase inhibitors, suggesting that activation of tyrosine kinases may play a role in activating the osmolyte effluxes. These results indicate that the volume-activated TMAO efflux occurs via the organic osmolyte (taurine) channel and may be regulated by the volume activation of tyrosine kinases.

anion transport; taurine; protein kinases


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