| Literature DB >> 30996143 |
Meredith D Hartley1,2, Tania Banerji1, Ian J Tagge3, Lisa L Kirkemo1,2, Priya Chaudhary2,4, Evan Calkins2,4, Danielle Galipeau2,4, Mitra D Shokat1, Margaret J DeBell1, Shelby Van Leuven1, Hannah Miller1, Gail Marracci2,4, Edvinas Pocius2,4, Tapasree Banerji1, Skylar J Ferrara1, J Matthew Meinig1, Ben Emery4,5, Dennis Bourdette2,4, Thomas S Scanlan1.
Abstract
Oligodendrocyte processes wrap axons to form neuroprotective myelin sheaths, and damage to myelin in disorders, such as multiple sclerosis (MS), leads to neurodegeneration and disability. There are currently no approved treatments for MS that stimulate myelin repair. During development, thyroid hormone (TH) promotes myelination through enhancing oligodendrocyte differentiation; however, TH itself is unsuitable as a remyelination therapy due to adverse systemic effects. This problem is overcome with selective TH agonists, sobetirome and a CNS-selective prodrug of sobetirome called Sob-AM2. We show here that TH and sobetirome stimulated remyelination in standard gliotoxin models of demyelination. We then utilized a genetic mouse model of demyelination and remyelination, in which we employed motor function tests, histology, and MRI to demonstrate that chronic treatment with sobetirome or Sob-AM2 leads to significant improvement in both clinical signs and remyelination. In contrast, chronic treatment with TH in this model inhibited the endogenous myelin repair and exacerbated disease. These results support the clinical investigation of selective CNS-penetrating TH agonists, but not TH, for myelin repair.Entities:
Keywords: Endocrinology; Mouse models; Multiple sclerosis; Neuroscience
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Year: 2019 PMID: 30996143 PMCID: PMC6538346 DOI: 10.1172/jci.insight.126329
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708