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首页> 外文期刊>Development >LIM homeodomain transcription factor-dependent specification of bipotential MGE progenitors into cholinergic and GABAergic striatal interneurons.
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LIM homeodomain transcription factor-dependent specification of bipotential MGE progenitors into cholinergic and GABAergic striatal interneurons.

机译:LIM同源域转录因子依赖的双潜MGE祖细胞到胆碱能和GABA能的纹状体中间神经元的规范。

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Coordination of voluntary motor activity depends on the generation of the appropriate neuronal subtypes in the basal ganglia and their integration into functional neuronal circuits. The largest nucleus of the basal ganglia, the striatum, contains two classes of neurons: the principal population of medium-sized dense spiny neurons (MSNs; 97-98% of all striatal neurons in rodents), which project to the globus pallidus and the substantia nigra, and the locally projecting striatal interneurons (SINs; 2-3% in rodents). SINs are further subdivided into two non-overlapping groups: those producing acetylcholine (cholinergic) and those producing gamma-amino butyric acid (GABAergic). Despite the pivotal role of SINs in integrating the output of striatal circuits and the function of neuronal networks in the ventral forebrain, the lineage relationship of SIN subtypes and the molecular mechanisms that control their differentiation are currently unclear. Using genetic fate mapping, we demonstrate here that the majority of cholinergic and GABAergic SINs are derived from common precursors generated in the medial ganglionic eminence during embryogenesis. These precursors express the LIM homeodomain protein Lhx6 and have characteristics of proto-GABAergic neurons. By combining gene expression analysis with loss-of-function and misexpression experiments, we provide evidence that the differentiation of the common precursor into mature SIN subtypes is regulated by the combinatorial activity of the LIM homeodomain proteins Lhx6, Lhx7 (Lhx8) and Isl1. These studies suggest that a LIM homeodomain transcriptional code confers cell-fate specification and neurotransmitter identity in neuronal subpopulations of the ventral forebrain.
机译:自愿运动活动的协调取决于基底神经节中合适的神经元亚型的产生及其与功能性神经元回路的整合。基底神经节的最大核(纹状体)包含两类神经元:中型致密多刺神经元(MSN;啮齿动物中所有纹状体神经元的97-98%)的主要种群,它们投射到苍白球和黑质,以及局部突出的纹状体中间神经元(SIN;啮齿动物中占2-3%)。 SIN进一步分为两个不重叠的组:产生乙酰胆碱的(胆碱能的)和产生γ-氨基丁酸的那些(GABA能的)。尽管SIN在整合纹状体回路的输出和腹侧前脑神经网络的功能方面起着关键作用,但目前尚不清楚SIN亚型的谱系关系和控制它们分化的分子机制。使用遗传命运图谱,我们在这里证明了大多数胆碱能和GABA能SIN都来自胚胎发生过程中在内侧神经节突起中产生的常见前体。这些前体表达LIM同源域蛋白Lhx6,并具有原GABA能神经元的特征。通过将基因表达分析与功能丧失和错误表达实验相结合,我们提供了证据,即LIM同源结构域蛋白Lhx6,Lhx7(Lhx8)和Isl1的组合活性可调节常见前体分化为成熟的SIN亚型。这些研究表明LIM同源域转录代码赋予腹侧前脑神经元亚群中的细胞命运规范和神经递质同一性。

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