| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 10871793 | FEBS Letters | 2011 | 8 Pages |
Abstract
Multiple sclerosis is a common demyelinating disease that worsens over the course of disease, a significant problem in clinical management. Disability in MS is significantly promoted by poor repair and remyelination of lesions. Both oligodendrocyte recruitment and maturation defects are seen as major causes of poor remyelination in MS. The mechanisms behind impaired remyelination in animal models include involvement of the Notch1, wnt, and hyaluronan/TLR2 pathways. RXR/PPAR signaling has also more recently been identified as an important regulator of remyelination. The local inflammatory milieu also appears to play critical and conflicting roles in promotion and inhibition of remyelination in MS. Understanding the forces regulating remyelination in MS represents an exciting and important initial step towards developing therapeutics targeting chronic disability in MS.
Keywords
Retinoid X receptorHMWOPCEAETLRCNPcKONgR1WntLPSNICDPLPSmall inhibitory RNARXRDPLNotch1LINGO1Notch1 intracellular domainPPARkDakiloDaltonMBPHDACMAGDRGLMWdorsal root ganglion15-deoxy-Δ12,14-Prostaglandin J22′,3′-cyclic nucleotide 3′-phosphodiesteraseProteolipid proteinRemyelinationsiRNAexperimental allergic encephalomyelitisToll-like receptorCNSOligodendrocyte progenitor cellcentral nervous systemconditional knockoutlipopolysaccharideMultiple sclerosisNeurofascinHyaluronanhistone deacetylasehigh molecular weightlow molecular weightMyelin basic proteingalactocerebrosideGalCMyelin associated glycoproteinPeroxisome proliferator activated receptoroligodendrocytes
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Authors
Khalid A. Hanafy, Jacob A. Sloane,