Protein kinase C activity modulates myelin gene expression in enriched oligodendrocytes
- 1 April 1993
- journal article
- Published by Wiley in Journal of Neuroscience Research
- Vol. 34 (5) , 571-588
- https://doi.org/10.1002/jnr.490340509
Abstract
Protein kinase C (PKC) and its potential role in myelin gene expression were investigated in primary cultured rat oligodendrocytes. The major myelin genes were expressed in a developmentally coordinated manner in cultured oligodendrocytes. PKC activity in these cells was similarly regulated with differential expression of PKC isozyme mRNAs. PKC-gamma mRNA was expressed transiently and was most abundant in 9-day cells in vitro. PKC-alpha and PKC-beta mRNAs were present at low levels throughout development in these cells, and their expression increased in 18-25 day cells. Immunocytochemical colocalization of PKC with oligodendrocyte-specific markers--O4, galactosyl cerebroside, MBP, and PLP--in enriched oligodendrocyte cultures suggested that the PKC enzyme activities assayed in these cultures were predominantly contributed by oligodendrocytes. PKC inhibition resulting from long-term exposure to 4 beta-phorbol-12,13-dibutyrate (4 beta-PDB) reduced steady-state levels of MBP, PLP, MAG, CNP, and PKC-alpha mRNAs, as detected by slot blots or in situ hybridization, and downregulated the oligodendrocyte-specific markers O4, galactosyl cerebroside, and the major constituent proteins MBP and PLP, as detected by immunocytochemistry. PKC-mediated downmodulation of myelin gene expression was most profound in normally differentiating oligodendrocytes at or before the onset of myelin protein synthesis. Six-day oligodendrocytes were most susceptible to such modulation. To elucidate the mechanism of reduction in various myelin gene messages upon modulation of PKC, we analyzed mRNA levels in oligodendrocytes, which were pretreated with either the transcriptional inhibitor actinomycin D or the protein synthesis blocker cycloheximide before exposure to 4 beta-PDB. Our results demonstrate that the PKC inhibition-mediated loss in myelin mRNA levels did not require the transcription of any genes, but appeared to be at least partially dependent on continuous protein synthesis.Keywords
This publication has 87 references indexed in Scilit:
- Transient reversion of O4+ Galc− oligodendrocyte progenitor development in response to the phorbol ester TPAJournal of Neuroscience Research, 1993
- Protein kinase C stimulation enhances the process formation of adult oligodendrocytes and induces proliferationJournal of Neuroscience Research, 1991
- Recent Advances in Studies on Genes for Myelin ProteinsDevelopment, Growth & Differentiation, 1991
- Age‐dependent decrease of process formation by cultured oligodendrocytes is augmented by protein kinase C stimulationJournal of Neuroscience Research, 1991
- Differential expression of galactocerebroside, myelin basic protein, and 2′,3′‐cyclic nucleotide 3′‐phosphohydrolase during development of oligodendrocytes in vitroJournal of Neuroscience Research, 1988
- Phorbol ester enhances morphological differentiation of oligodendrocytes in cultureJournal of Neuroscience Research, 1988
- Disappearance of Ca2+-sensitive, phospholipid-dependent protein kinase activity in phorbol ester-treated 3T3 cellsBiochemical and Biophysical Research Communications, 1984
- Cell that are O4 antigen-positive and O1 antigen-negative differentiate into O1 antigen-positive oligodendrocytesNeuroscience Letters, 1982
- Preparation and Properties of an Immunosorbent Column Specific for the Myelin Basic ProteinJournal of Neurochemistry, 1981
- Preparation of separate astroglial and oligodendroglial cell cultures from rat cerebral tissue.The Journal of cell biology, 1980