Abstract

The large majority of chromaffin vesicles are excluded from the plasma membrane by a cortical F-actin network. Treatment of chromaffin cells with phorbol 12-myristate 13-acetate produces disassembly of cortical F-actin, increasing the number of vesicles at release sites (Vitale, M. L., Seward, E. P., and Trifaró, J. M. (1995) Neuron 14, 353-363). Here, we provide evidence for involvement of myristoylated alanine-rich protein kinase C substrate (MARCKS), a protein kinase C substrate, in chromaffin cell secretion. MARCKS binds and cross-links F-actin, the latter is inhibited by protein kinase C-induced MARCKS phosphorylation. MARCKS was found in chromaffin cells by immunoblotting. MARCKS was also detected by immunoprecipitation. In intact or permeabilized cells MARCKS phosphorylation increased upon stimulation with 10(-7) m phorbol 12-myristate 13-acetate. This was accompanied by cortical F-actin disassembly and potentiation of secretion. MARCKS phosphorylation, cortical F-actin disassembly, and potentiation of Ca(2+)-evoked secretion were inhibited by a peptide (MARCKS phosphorylation site domain sequence (MPSD)) with amino acid sequence corresponding to MARCKS phosphorylation site. MPSD was phosphorylated in the process. A similar peptide (alanine-substituted phosphorylated site domain) with four serine residues of MPSD substituted by alanines was ineffective. These results provide the first evidence for MARCKS involvement in chromaffin cell secretion and suggest that regulation of cortical F-actin cross-linking might be involved in this process.

Highlights

  • Chromaffin cells store their secretory products in membranebound organelles and chromaffin vesicles that release their contents to the extracellular medium by exocytosis

  • myristoylated alanine-rich protein kinase C substrate (MARCKS) phosphorylation, cortical F-actin disassembly, and potentiation of Ca2؉-evoked secretion were inhibited by a peptide (MARCKS phosphorylation site domain sequence (MPSD)) with amino acid sequence corresponding to MARCKS phosphorylation site

  • MARCKS is a member of a family of PKC substrates that potentially can interact with F-actin and calmodulin, proteins that are widely distributed in the nervous system [20, 21, 26, 45, 46]

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Summary

Introduction

Chromaffin cells store their secretory products in membranebound organelles and chromaffin vesicles that release their contents to the extracellular medium by exocytosis. Resting permeabilized chromaffin cells have an unexpected relatively high basal level of MARCKS phosphorylation that, after treatment with PMA, increased only by 1.5 times (Fig. 3, A and C).

Results
Conclusion

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