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首页> 外文期刊>Cell stem cell >Wnt1-lmx1a forms a novel autoregulatory loop and controls midbrain dopaminergic differentiation synergistically with the SHH-FoxA2 pathway.
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Wnt1-lmx1a forms a novel autoregulatory loop and controls midbrain dopaminergic differentiation synergistically with the SHH-FoxA2 pathway.

机译:Wnt1-lmx1a形成一个新的自动调节环,并与SHH-FoxA2途径协同控制中脑多巴胺能分化。

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摘要

Selective degeneration of midbrain dopaminergic (mDA) neurons is associated with Parkinson's disease (PD), and thus an in-depth understanding of molecular pathways underlying mDA development will be crucial for optimal bioassays and cell replacement therapy for PD. In this study, we identified a novel Wnt1-Lmx1a autoregulatory loop during mDA differentiation of ESCs and confirmed its in vivo presence during embryonic development. We found that the Wnt1-Lmx1a autoregulatory loop directly regulates Otx2 through the beta-catenin complex and Nurr1 and Pitx3 through Lmx1a. We also found that Lmx1a and Lmx1b cooperatively regulate mDA differentiation with overlapping and cross-regulatory functions. Furthermore, coactivation of both Wnt1 and SHH pathways by exogenous expression of Lmx1a, Otx2, and FoxA2 synergistically enhanced the differentiation of ESCs to mDA neurons. Together with previous works, this study shows that two regulatory loops (Wnt1-Lmx1a and SHH-FoxA2) critically link extrinsic signals to cell-intrinsic factors and cooperatively regulate mDA neuron development.
机译:中脑多巴胺能(mDA)神经元的选择性变性与帕金森氏病(PD)相关,因此深入了解mDA发育的分子途径对于PD的最佳生物测定和细胞替代治疗至关重要。在这项研究中,我们确定了ESC的mDA分化过程中的新型Wnt1-Lmx1a自调节环,并证实了其在胚胎发育过程中的体内存在。我们发现Wnt1-Lmx1a自动调节回路通过β-catenin复合物直接调节Otx2,通过Lmx1a直接调节Nurr1和Pitx3。我们还发现,Lmx1a和Lmx1b通过重叠和交叉调节功能协同调节mDA分化。此外,通过Lmx1a,Otx2和FoxA2的外源表达对Wnt1和SHH途径的共激活可以协同增强ESC向mDA神经元的分化。与以前的工作一起,这项研究表明,两个调节环(Wnt1-Lmx1a和SHH-FoxA2)将外部信号关键性地连接到细胞内在因子上,并共同调节mDA神经元的发育。

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