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[3H]taurine and D-[3H]aspartate release from astrocyte cultures are differently regulated by tyrosine kinases.

作者信息

Mongin A A, Reddi J M, Charniga C, Kimelberg H K

机构信息

Division of Neurosurgery, Albany Medical College, Albany, New York 12208, USA.

出版信息

Am J Physiol. 1999 May;276(5):C1226-30. doi: 10.1152/ajpcell.1999.276.5.C1226.

Abstract

Volume-dependent anion channels permeable for Cl- and amino acids are thought to play an important role in the homeostasis of cell volume. Astrocytes are the main cell type in the mammalian brain showing volume perturbations under physiological and pathophysiological conditions. We investigated the involvement of tyrosine phosphorylation in hyposmotic medium-induced [3H]taurine and D-[3H]aspartate release from primary astrocyte cultures. The tyrosine kinase inhibitors tyrphostin 23 and tyrphostin A51 partially suppressed the volume-dependent release of [3H]taurine in a dose-dependent manner with half-maximal effects at approximately 40 and 1 microM, respectively. In contrast, the release of D-[3H]aspartate was not significantly affected by these agents in the same concentration range. The inactive analog tyrphostin 1 had no significant effect on the release of both amino acids. The data obtained suggest the existence of at least two volume-dependent anion channels permeable to amino acids in astrocyte cultures. One of these channels is permeable to taurine and is under the control of tyrosine kinase(s). The other is permeable to both taurine and aspartate, but its volume-dependent regulation does not require tyrosine phosphorylation.

摘要

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