Identification of PDZ Domain Containing Proteins Interacting with 1.2 and PMCA4b
Author(s) -
Doreen Korb,
Priscilla Tng,
Vladimir M. Milenkovic,
Nadine Reichhart,
Olaf Strauß,
Oliver Ritter,
Tobias Fischer,
Peter M. Benz,
Kai Schuh
Publication year - 2013
Publication title -
isrn cell biology
Language(s) - English
Resource type - Journals
eISSN - 2090-7389
pISSN - 2090-7370
DOI - 10.1155/2013/265182
Subject(s) - pdz domain , cask , transmembrane protein , cytoplasm , immunoprecipitation , hek 293 cells , chemistry , biophysics , protein–protein interaction , microbiology and biotechnology , biology , biochemistry , gene , genetics , receptor
PDZ (PSD-95/Disc large/Zonula occludens-1) protein interaction domains bind to cytoplasmic protein C-termini of transmembrane proteins. In order to identify new interaction partners of the voltage-gated L-type Ca 2+ channel 1.2 and the plasma membrane Ca 2+ ATPase 4b (PMCA4b), we used PDZ domain arrays probing for 124 PDZ domains. We confirmed this by GST pull-downs and immunoprecipitations. In PDZ arrays, strongest interactions with 1.2 and PMCA4b were found for the PDZ domains of SAP-102, MAST-205, MAGI-1, MAGI-2, MAGI-3, and ZO-1. We observed binding of the 1.2 C-terminus to PDZ domains of NHERF1/2, Mint-2, and CASK. PMCA4b was observed to interact with Mint-2 and its known interactions with Chapsyn-110 and CASK were confirmed. Furthermore, we validated interaction of 1.2 and PMCA4b with NHERF1/2, CASK, MAST-205 and MAGI-3 via immunoprecipitation. We also verified the interaction of 1.2 and nNOS and hypothesized that nNOS overexpression might reduce Ca 2+ influx through 1.2. To address this, we measured Ca 2+ currents in HEK 293 cells co-expressing 1.2 and nNOS and observed reduced voltage-dependent 1.2 activation. Taken together, we conclude that 1.2 and PMCA4b bind promiscuously to various PDZ domains, and that our data provides the basis for further investigation of the physiological consequences of these interactions.
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