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Publication : Conditional knockout of TOG results in CNS hypomyelination.

First Author  Maggipinto MJ Year  2017
Journal  Glia Volume  65
Issue  3 Pages  489-501
PubMed ID  28063167 Mgi Jnum  J:238707
Mgi Id  MGI:5823498 Doi  10.1002/glia.23106
Citation  Maggipinto MJ, et al. (2017) Conditional knockout of TOG results in CNS hypomyelination. Glia 65(3):489-501
abstractText  The tumor overexpressed gene (TOG) protein is present in RNA granules that transport myelin basic protein (MBP) mRNA in oligodendrocyte processes to the myelin compartment. Its role was investigated by conditionally knocking it out (KO) in myelinating glia in vivo. TOG KO mice have severe motor deficits that are already apparent at the time of weaning. This phenotype correlates with a paucity of myelin in several CNS regions, the most severe being in the spinal cord. In the TOG KO optic nerve <30% of axons are myelinated. The number of oligodendrocytes in the corpus callosum, cerebellum, and cervical spinal cord is normal. In the absence of TOG, the most patent biochemical change is a large reduction in MBP content, yet normal amounts of MBP transcripts are found in the brain of affected animals. MBP transcripts are largely confined to the cell body of the oligodendrocytes in the TOG KO in contrast to the situation in wild type mice where they are found in the processes of the oligodendrocytes and in the myelin compartment. These findings indicate that MBP gene expression involves a post-transcriptional TOG-dependent step. TOG may be necessary for MBP mRNA assembly into translation permissive granules, and/or for transport to preferred sites of translation. GLIA 2017;65:489-501.
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