Interactions of Sox10 and Egr2 in myelin gene regulation.

Erin A Jones, Sung-Wook Jang, Gennifer M Mager, Li-Wei Chang, Rajini Srinivasan, Nolan G Gokey, Rebecca M Ward, Rakesh Nagarajan, John Svaren
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Abstract

Myelination in the PNS is accompanied by a large induction of the myelin protein zero (Mpz) gene to produce the most abundant component in peripheral myelin. Analyses of knockout mice have shown that the EGR2/Krox20 and SOX10 transcription factors are required for Mpz expression. Our recent work has shown that the dominant EGR2 mutations associated with human peripheral neuropathies cause disruption of EGR2/SOX10 synergy at specific sites, including a conserved enhancer element in the first intron of the Mpz gene. Further investigation of Egr2/Sox10 interactions reveals that activation of the Mpz intron element by Egr2 requires both Sox10-binding sites. In addition, both Egr1 and Egr3 cooperate with Sox10 to activate this element, which indicates that this capacity is conserved among Egr family members. Finally, a conserved composite structure of Egr2/Sox10-binding sites in the genes encoding Mpz, myelin-associated glycoprotein and myelin basic protein genes was used to screen for similar modules in other myelin genes, revealing a potential regulatory element in the periaxin gene. Overall, these results elucidate a working model for developmental regulation of Mpz expression, several facets of which extend to regulation of other peripheral myelin genes.

Sox10 和 Egr2 在髓鞘基因调控中的相互作用
前神经系统的髓鞘化伴随着髓鞘蛋白零(Mpz)基因的大量诱导,以产生外周髓鞘中最丰富的成分。对基因敲除小鼠的分析表明,Mpz的表达需要EGR2/Krox20和SOX10转录因子。我们最近的研究表明,与人类周围神经病相关的显性 EGR2 突变会导致特定位点的 EGR2/SOX10 协同作用中断,包括 Mpz 基因第一个内含子中的保守增强子元件。对 Egr2/Sox10 相互作用的进一步研究表明,Egr2 对 Mpz 内含子元件的激活需要两个 Sox10 结合位点。此外,Egr1 和 Egr3 都与 Sox10 合作激活该元件,这表明这种能力在 Egr 家族成员中是保守的。最后,利用编码Mpz、髓鞘相关糖蛋白和髓鞘碱性蛋白基因的Egr2/Sox10结合位点的保守复合结构来筛选其他髓鞘基因中的类似模块,发现了periaxin基因中的潜在调控元件。总之,这些结果阐明了Mpz表达的发育调控工作模型,其中的几个方面可扩展到其他外周髓鞘基因的调控。
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来源期刊
Neuron glia biology
Neuron glia biology 医学-神经科学
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