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Specific and integrated roles of Lmx1a, Lmx1b and Phox2a in ventral midbrain development.

机译:Lmx1a,Lmx1b和Phox2a在腹中脑发育中的特定和综合作用。

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The severe disorders associated with a loss or dysfunction of midbrain dopamine neurons (DNs) have intensified research aimed at deciphering developmental programs controlling midbrain development. The homeodomain proteins Lmx1a and Lmx1b are important for the specification of DNs during embryogenesis, but it is unclear to what degree they may mediate redundant or specific functions. Here, we provide evidence showing that DN progenitors in the ventral midbrain can be subdivided into molecularly distinct medial and lateral domains, and these subgroups show different sensitivity to the loss of Lmx1a and Lmx1b. Lmx1a is specifically required for converting non-neuronal floor-plate cells into neuronal DN progenitors, a process that involves the establishment of Notch signaling in ventral midline cells. On the other hand, lateral DN progenitors that do not appear to originate from the floor plate are selectively ablated in Lmx1b mutants. In addition, we also reveal an unanticipated role for Lmx1b in regulating Phox2a expression and the sequential specification of ocular motor neurons (OMNs) and red nucleus neurons (RNNs) from progenitors located lateral to DNs in the midbrain. Our data therefore establish that Lmx1b influences the differentiation of multiple neuronal subtypes in the ventral midbrain, whereas Lmx1a appears to be exclusively devoted to the differentiation of the DN lineage.
机译:与中脑多巴胺神经元(DNs)丧失或功能障碍相关的严重疾病,已加强研究,旨在破译控制中脑发育的发育程序。同源域蛋白Lmx1a和Lmx1b对于胚胎形成过程中DN的规格很重要,但是目前尚不清楚它们在多大程度上可以介导冗余或特定功能。在这里,我们提供的证据表明,腹中脑中的DN祖细胞可以细分为分子上不同的内侧和外侧区域,这些亚组对Lmx1a和Lmx1b的丢失表现出不同的敏感性。 Lmx1a是将非神经元底板细胞转化为神经元DN祖细胞的特别要求,该过程涉及在腹中线细胞中建立Notch信号。另一方面,在Lmx1b突变体中选择性消融了似乎不起源于底板的侧向DN祖细胞。此外,我们还揭示了Lmx1b在调节Phox2a表达以及来自中脑DN外侧的祖细胞的眼动神经元(OMNs)和红核神经元(RNNs)的顺序规范中的意外作用。因此,我们的数据确定Lmx1b影响腹中脑中多个神经元亚型的分化,而Lmx1a似乎专门致力于DN谱系的分化。

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