Defects of Lipid Synthesis Are Linked to the Age-Dependent Demyelination Caused by Lamin B1 Overexpression.
Harshvardhan RolyanYulia Y TyurinaMarylens HernandezAndrew A AmoscatoLouis J SparveroBruce C NmeziYue LuMarcos R H EstécioKevin LinJunda ChenRong-Rong HePin GongLora H RigattiJeffrey DupreeHülya BayırValerian E KaganPatrizia CasacciaQuasar S PadiathPublished in: The Journal of neuroscience : the official journal of the Society for Neuroscience (2015)
Autosomal dominant leukodystrophy (ADLD) is fatal neurological disorder caused by increased levels of the nuclear protein, Lamin B1. The disease is characterized by an age-dependent loss of myelin, the fatty sheath that covers nerve fibers. We have studied a mouse model where Lamin B1 level are increased in oligodendrocytes, the cell type that produces myelin in the CNS. We demonstrate that destruction of myelin in the spinal cord is responsible for the degenerative phenotype in our mouse model. We show that this degeneration is mediated by reduced expression of lipid synthesis genes and the subsequent reduction in myelin enriched lipids. These findings provide a mechanistic framework to explain the age dependence and tissue specificity of the ADLD disease phenotype.