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Spatial and temporal regulation of ventral spinal cord precursor specification by Hedgehog signaling.

机译:Hedgehog信号传导对脊髓前体规格的时空调节。

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摘要

Graded Hedgehog (Hh) signaling patterns the spinal cord dorsoventral axis by inducing and positioning distinct precursor domains, each of which gives rise to a different type of neuron. These domains also generate glial cells, but the full range of cell types that any one precursor population produces and the mechanisms that diversify cell fate are unknown. By fate mapping and clonal analysis in zebrafish, we show that individual ventral precursor cells that express olig2 can form motoneurons, interneurons and oligodendrocytes. However, olig2(+) precursors are not developmentally equivalent, but instead produce subsets of progeny cells in a spatially and temporally biased manner. Using genetic and pharmacological manipulations, we provide evidence that these biases emerge from Hh acting over time to set, maintain, subdivide and enlarge the olig2(+) precursor domain and subsequently specify oligodendrocyte development. Our studies show that spatial and temporal differences in Hh signaling within a common population of neural precursors can contribute to cell fate diversification.
机译:分级的刺猬(Hh)信号通过诱导和定位不同的前体结构域来图案化脊髓背腹轴,每个前体结构域都会引起不同类型的神经元。这些结构域还产生神经胶质细胞,但是任何一种前体种群产生的全部细胞类型以及使细胞命运多样化的机制尚不清楚。通过命运映射和斑马鱼的克隆分析,我们表明表达olig2的单个腹侧前体细胞可以形成运动神经元,中间神经元和少突胶质细胞。但是,olig2(+)前体在发育上不是等效的,而是以时空偏向的方式产生子代细胞的子集。使用遗传和药理学操作,我们提供的证据表明,随着时间的流逝,这些偏倚会随着Hh的出现而发生,以设置,维持,细分和扩大olig2(+)前体域,并随后指定少突胶质细胞的发育。我们的研究表明,在常见的神经前体群体中,Hh信号的时空差异可以促进细胞命运的多样化。

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