Myelination depends on the synthesis of large amounts of myelin transcripts and proteins and is controlled by Nrg1/ErbB/Shp2 signaling. We developed a novel pulse labeling strategy based on stable isotope labeling with amino acids in cell culture (SILAC) to measure the dynamics of myelin protein production in mice. We found that protein synthesis is dampened in the maturing postnatal peripheral nervous system, and myelination then slows down. Remarkably, sustained activation of MAPK signaling by expression of the Mek1DD allele in mice overcomes the signals that end myelination, resulting in continuous myelin growth. MAPK activation leads to minor changes in transcript levels but massively up-regulates protein production. Pharmacological interference in vivo demonstrates that the effects of activated MAPK signaling on translation are mediated by mTOR-independent mechanisms but in part also by mTOR-dependent mechanisms. Previous work demonstrated that loss of ErbB3/Shp2 signaling impairs Schwann cell development and disrupts the myelination program. We found that activated MAPK signaling strikingly compensates for the absence of ErbB3 or Shp2 during Schwann cell development and myelination.
Activation of MAPK overrides the termination of myelin growth and replaces Nrg1/ErbB3 signals during Schwann cell development and myelination.
MAPK 的激活会抑制髓鞘生长,并在雪旺细胞发育和髓鞘形成过程中取代 Nrg1/ErbB3 信号
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作者:Sheean Maria E, McShane Erik, Cheret Cyril, Walcher Jan, Müller Thomas, Wulf-Goldenberg Annika, Hoelper Soraya, Garratt Alistair N, Krüger Markus, Rajewsky Klaus, Meijer Dies, Birchmeier Walter, Lewin Gary R, Selbach Matthias, Birchmeier Carmen
| 期刊: | Genes & Development | 影响因子: | 7.700 |
| 时间: | 2014 | 起止号: | 2014 Feb 1; 28(3):290-303 |
| doi: | 10.1101/gad.230045.113 | 研究方向: | 细胞生物学 |
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