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Defining the volume dependence of multiple K flux pathways of trout red blood cells.

Authors :
Berenbrink M
Weaver YR
Cossins AR
Source :
The American journal of physiology [Am J Physiol] 1997 Apr; Vol. 272 (4 Pt 1), pp. C1099-111.
Publication Year :
1997

Abstract

The volume sensitivity of different K flux pathways has been determined in trout red blood cells subjected to volume perturbation. Gentle hyposmotic swelling induced a K influx in a Cl-containing saline but not in NO3- or methanesulfonate (MeSF)-containing salines, consistent with the activation of a Cl-dependent flux. Extreme hyposmotic swelling led to larger K fluxes in all salines but with reduced anion discrimination of the Cl-dependent flux. In contrast to these graded responses, isosmotic swelling using ammonium chloride or beta-adrenergic stimulation activated only Cl-dependent fluxes in an all-or-none fashion. The relationship between the hyposmotically and isosmotically induced pathways was studied by coactivation using either ammonium chloride or isoproterenol with anisosmotic treatment. Cells in ammonium chloride-containing hyposmotic salines showed no additive K flux over that induced by hyposmotic treatment alone, indicating that the isosmotically induced Cl-dependent flux was identical to the hyposmotically induced Cl-dependent flux. However, cells coactivated by hyposmotic and beta-adrenergic treatment showed a small Cl-dependent flux in addition to that induced by hyposmotic treatment alone. This small third component was unaffected by anisosmotic treatment. We conclude that the major Cl-dependent and Cl-independent K flux pathways are distinct and separate and that the former has an anion dependence that varies with cell volume and a volume sensitivity that varies with ionic strength.

Details

Language :
English
ISSN :
0002-9513
Volume :
272
Issue :
4 Pt 1
Database :
MEDLINE
Journal :
The American journal of physiology
Publication Type :
Academic Journal
Accession number :
9142834
Full Text :
https://doi.org/10.1152/ajpcell.1997.272.4.C1099