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Axoskeletal proteins prevent oligodendrocyte from toxic injury by upregulating survival,proliferation, and differentiation in vitro
Authors:Catherine Fressinaud,Joë  l Eyer
Affiliation:1. Neurology Department, University Hospital, ANGERS, France;2. Transgenesis and Neurobiology Laboratory, UPRES EA 3143, University Hospital, ANGERS, France
Abstract:Neurofilaments (NF) are detected in the cerebrospinal fluid of multiple sclerosis (MS) patients, and their concentration correlates with disease severity. We recently demonstrated that NF and co-isolated proteins increase the proliferation and differentiation of oligodendrocytes (OL) in vitro. If these proteins are released in the extracellular environment in MS, they might then regulate remyelination by OL. To test this hypothesis we took advantage of a paradigm of OL toxic injury using lysophosphatidyl choline (LPC), which decreases proliferation and differentiation of surviving cells, and destroys myelin-like membranes. In OL cultures that have been treated with LPC, NF fractions as well as tubulin (TUB) significantly improved recovery: the number of OL progenitors (OLP, A2B5+ cells) increased by 100% and their proliferation by 200%, whereas differentiated (CNP+) and mature (MBP+) cells increased by 150% compared to cultures treated with LPC alone. When added at the time of LPC treatment, NF and TUB protected OL from LPC toxicity; they increased OLP by 90%, as well as the number of CNP+ and MBP+ OL by 65–110%, respectively, compared to cultures treated only with LPC. These effects were specific since irrelevant proteins (actin, skin proteins) were ineffective. This demonstrates that NF and TUB protect OL and increase OLP proliferation, as well as their survival, when challenged with LPC, without delaying differentiation and maturation in vitro. Thus, NF and TUB delivered following axonal damage in MS could participate in the regulation of remyelination through this process.
Keywords:BrdU, bromodeoxyuridine   CDM, chemically-defined medium   CNP, 2&prime  ,3&prime  -cyclic nucleotide 3&prime  -phosphodiesterase   CNS, central nervous system   CSF, cerebrospinal fluid   MAP, microtubule associated protein   MBP, myelin basic protein   MS, multiple sclerosis   NF, neurofilaments   OL, oligodendrocyte   OLP, oligodendrocyte progenitor   TUB, tubulin
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