Abstract
We have previously demonstrated that in Ehrlich cells a bumetanide-sensitive Na +,K +,2Cl − cotransporter is activated during regulatory volume decrease after cell shrinkage (hypertonic conditions) as well as during the late phase of regulatory volume decrease (hypotonic conditions). It is, however, quiescent under isotonic conditions. Using a protein kinase C assay system (Amersham, UK) it is here demonstrated that hypertonic cell shrinkage results in an increase in protein kinase C activity to 174% within the first minute, concomitant with the activation of the Na +,K +,2Cl − cotransporter. Hypotonic cell swelling results in a late activation of protein kinase C concomitant with a late activation of the Na +,K +,2Cl − cotransporter. The activation of protein kinase C during hypertonic as well as hypotonic conditions is inhibited by H-7. The more specific protein kinase C inhibitor chelerythrine inhibited protein kinase C as well as the Na +,K +,2Cl − cotransporter to the same extent as did H-7. These results indicate the involvement of protein kinase C in the regulation of the Na +,K +,2Cl − cotransporter in Ehrlich ascites tumor cells during cell volume regulation.
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Schedule a callMore From: Biochimica et Biophysica Acta (BBA) - Molecular Cell Research
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