Université catholique de Louvain, Institute of Neuroscience, Laboratory of Neural Differentiation, 1200 Brussels, Belgium.
Development. 2012 Sep;139(17):3109-19. doi: 10.1242/dev.078501. Epub 2012 Jul 25.
During development, spinal motoneurons (MNs) diversify into a variety of subtypes that are specifically dedicated to the motor control of particular sets of skeletal muscles or visceral organs. MN diversification depends on the coordinated action of several transcriptional regulators including the LIM-HD factor Isl1, which is crucial for MN survival and fate determination. However, how these regulators cooperate to establish each MN subtype remains poorly understood. Here, using phenotypic analyses of single or compound mutant mouse embryos combined with gain-of-function experiments in chick embryonic spinal cord, we demonstrate that the transcriptional activators of the Onecut family critically regulate MN subtype diversification during spinal cord development. We provide evidence that Onecut factors directly stimulate Isl1 expression in specific MN subtypes and are therefore required to maintain Isl1 production at the time of MN diversification. In the absence of Onecut factors, we observed major alterations in MN fate decision characterized by the conversion of somatic to visceral MNs at the thoracic levels of the spinal cord and of medial to lateral MNs in the motor columns that innervate the limbs. Furthermore, we identify Sip1 (Zeb2) as a novel developmental regulator of visceral MN differentiation. Taken together, these data elucidate a comprehensive model wherein Onecut factors control multiple aspects of MN subtype diversification. They also shed light on the late roles of Isl1 in MN fate decision.
在发育过程中,脊髓运动神经元(MNs)多样化为多种亚型,专门用于特定骨骼肌或内脏器官的运动控制。MN 多样化取决于几种转录调节因子的协调作用,包括 LIM-HD 因子 Isl1,它对 MN 的存活和命运决定至关重要。然而,这些调节因子如何合作建立每种 MN 亚型仍知之甚少。在这里,我们使用单个或复合突变体小鼠胚胎的表型分析,结合鸡胚脊髓的功能获得实验,证明了 Onecut 家族的转录激活因子在脊髓发育过程中对 MN 亚型多样化具有重要调控作用。我们提供的证据表明,Onecut 因子直接刺激特定 MN 亚型中的 Isl1 表达,因此在 MN 多样化时需要维持 Isl1 的产生。在缺乏 Onecut 因子的情况下,我们观察到 MN 命运决定的重大改变,其特征是躯体 MN 向胸段脊髓的内脏 MN 转化,以及支配四肢的运动柱中内侧 MN 向外侧 MN 的转化。此外,我们确定 Sip1(Zeb2)是内脏 MN 分化的一个新的发育调节因子。总之,这些数据阐明了 Onecut 因子控制 MN 亚型多样化的多个方面的综合模型。它们还揭示了 Isl1 在 MN 命运决定中的晚期作用。