Immunogold Electron Microscopic Demonstration of Distinct Submembranous Localization of the Activated {gamma}PKC Depending on the Stimulation

doi:10.1369/jhc.7A7291.2007

Journal of Histochemistry and Cytochemistry

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JHC exPRESS: First Published November 26, 2007. doi:10.1369/jhc.7A7291.2007
Copyright © Histochemical Society, Inc.

A more recent version of this article appeared on March 1, 2008.

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Immunogold Electron Microscopic Demonstration of Distinct Submembranous Localization of the Activated ${gamma}$ PKC Depending on the Stimulation

Miho Oyasu ¹, Mineko Fujimiya ¹, Kaori Kashiwagi ¹, Shiho Ohmori ¹, Hirotsugu Imaeda ¹ and Naoaki Saito ¹^*

¹ Laboratory of Molecular Pharmacology, Biosignal Research Center, Kobe University, Kobe, Japan (MO,KK,SO,NS), and Department of Anatomy, Shiga University of Medical Science, Shiga, Japan (MF,HI)

^* To whom correspondence should be addressed. E-mail: naosaito{at}kobe-u.ac.jp.

Submitted on June 11, 2007
Accepted on 5 November 2007

Abstract
We examined the precise intracellular translocation of ${gamma}$ subtypeof protein kinase C ( ${gamma}$ PKC) after various extracellular stimuliusing confocal laser scanning fluorescent microscopy (CLSM)and immunogold electron microscopy. By CLSM, the treatment with12-o-tetradecanoylphorbol 13-acetate (TPA) resulted in a slowand irreversible accumulation of GFP-tagged ${gamma}$ PKC ( ${gamma}$ PKC-GFP) onthe plasma membrane. In contrast, the treatment with Ca²⁺-ionophoreand activation of purinergic or NMDA receptors induced a rapidand transient membrane translocation of ${gamma}$ PKC-GFP. Although eachstimulus resulted in PKC localization at the plasma membrane,electron microscopy revealed that ${gamma}$ PKC showed subtly but significantlydifferent localization depending on stimulation. While TPA andUTP induced a sustained localization of ${gamma}$ PKC-GFP on the plasmamembrane, Ca²⁺-ionophore and NMDA rapidly translocated ${gamma}$ PKC-GFPto the plasma membrane and then restricted ${gamma}$ PKC-GFP in submembranousarea (<500 nm from the plasma membrane). These results suggestthat Ca²⁺ influx alone induced the association of ${gamma}$ PKC with theplasma membrane only for a moment then located this enzyme ina proper distance like touch-and-go, while diacylglycerol orTPA tightly anchored this enzyme on the plasma membrane. Thedistinct subcellular targeting of ${gamma}$ PKC in response to variousstimuli suggests a novel mechanism for PKC activation.

Key Words: protein kinase C, translocation, Ca²⁺ ionophore, phorbol ester, electron microscopy, green fluorescent protein, immunogold

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