Defective myelination in an RNA polymerase III mutant leukodystrophic mouse
Emilio Merheb, Min-Hui Cui, Juwen C. DuBois, Craig A. Branch, Maria Gulinello, Bridget Shafit‐Zagardo, Robyn D. Moir, Ian M. Willis
Abstract
, specifically in Olig2-expressing cells, have impaired growth and developmental delay, deficits in cognitive, sensory, and fine sensorimotor function, and hypomyelination in multiple regions of the cerebrum and spinal cord. These phenotypes reflect a subset of clinical features seen in patients. In contrast, the gross motor defects and cerebellar hypomyelination that are common features of severely affected patients are absent in the mice, suggesting a relatively mild form of the disease in this conditional model. Our results show that disease pathogenesis in the mice involves defects that reduce both the number of mature myelinating oligodendrocytes and the ability of these cells to produce a myelin sheath of normal thickness. The findings suggest unique sensitivities of oligodendrogenesis and myelination to perturbations of Pol III transcription.