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The Journal of Neuroscience, January 15, 2003, 23(2):403-415
Modulation of Type 1 Inositol (1,4,5)-Trisphosphate Receptor
Function by Protein Kinase A and Protein Phosphatase 1
Tie-Shan
Tang*,
Huiping
Tu*,
Zhengnan
Wang, and
Ilya
Bezprozvanny
Department of Physiology, University of Texas Southwestern Medical
Center, Dallas, Texas 75390
Type 1 inositol (1,4,5)-trisphosphate receptors
(InsP3R1s) play a major role in neuronal calcium
(Ca2+) signaling. The InsP3R1s are
phosphorylated by protein kinase A (PKA), but the functional
consequences of InsP3R1 phosphorylation and the mechanisms
that control the phosphorylated state of neuronal InsP3R1s
are poorly understood. In a yeast two-hybrid screen of rat brain cDNA
library with the InsP3R1-specific bait, we isolated the
protein phosphatase 1 (PP1 ). In biochemical experiments, we
confirmed the specificity of the InsP3R1-PP1
association and immunoprecipitated the InsP3R1-PP1 complex
from rat brain synaptosomes and from the neostriatal lysate. We also
established that the association with PP1 facilitates dephosphorylation
of PKA-phosphorylated InsP3R1 by the endogenous neostriatal
PP1 and by the recombinant PP1 . We demonstrated that exposure of
neostriatal slices to 8-bromo-cAMP, dopamine, calyculin A, or
cyclosporine A, but not to 10 nM okadaic acid, promotes the
phosphorylation of neostriatal InsP3R1 by PKA in
vivo. We discovered that PKA activates and PP1 inhibits the activity of recombinant InsP3R1 reconstituted into planar
lipid bilayers. We found that phosphorylation of InsP3R1 by
PKA induces at least a fourfold increase in the sensitivity of
InsP3R1 to activation by InsP3 without shifting
the peak of InsP3R1 bell-shaped Ca2+
dependence. Based on these data, we suggest that InsP3R1
may participate in cross talk between cAMP and Ca2+
signaling in the neostriatum and possibly in other regions of the brain.
Key words:
inositol trisphosphate receptor; calcium signaling; dopamine; protein phosphorylation; yeast two-hybrid; planar lipid
bilayers
*
T.-S.T. and H.T. contributed equally to this work
Copyright © 2003 Society for Neuroscience 0270-6474/03/232403-13$05.00/0
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