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Notch 表现出配体偏向,并在胚胎干细胞中操纵阶段特异性的神经分化转向。

Notch exhibits ligand bias and maneuvers stage-specific steering of neural differentiation in embryonic stem cells.

机构信息

National Centre for Cell Science, Ganeshkhind, Pune 411007, Maharashtra, India.

出版信息

Mol Cell Biol. 2010 Apr;30(8):1946-57. doi: 10.1128/MCB.01419-09. Epub 2010 Feb 12.

Abstract

Notch dictates multiple developmental events, including stem cell maintenance and differentiation, through intercellular communication. However, its temporal influence during early development and, of particular interest, its regulation of binary fate decision at different stages during neurogenesis are among the least explored. Here, using an embryonic stem cell (ESC) model, we have deciphered Notch ligand preference during ESC commitment to different germ layers and determined the stage-specific temporal effect of Notch during neural differentiation. ESCs during maintenance remain impervious to Notch inhibition. However, Notch activation promotes differentiation even in the presence of leukemia inhibitory factor (LIF), displaying ligand preference-associated lineage discrimination, where Jagged-1 favors neural commitment and Delta-like-4 favors the mesoderm. This differential ligand action involves a combination of Notch receptors influencing specific downstream target gene expression. Though Notch activation during early neural differentiation specifically promotes neural stem cells or early neural progenitors and delays their maturation, its inhibition promotes late neural progenitors and expedites neurogenesis, with a preference for neurons over glia. However, gliogenesis is promoted upon Notch activation only when executed in combination with ciliary neurotrophic factor. Thus, our investigation underscores a multifaceted role of Notch, demonstrating the interdependency of ligand usage and lineage specification and Notch acting as a master switch, displaying stage-specific influence on neurogenesis.

摘要

Notch 通过细胞间通讯决定多种发育事件,包括干细胞的维持和分化。然而,它在早期发育过程中的时间影响,特别是在神经发生过程中不同阶段对二元命运决定的调节,是研究最少的方面之一。在这里,我们使用胚胎干细胞(ESC)模型,解析了 ESC 向不同胚层分化过程中 Notch 配体的偏好,并确定了 Notch 在神经分化过程中的特定阶段的时间效应。维持中的 ESC 仍然对 Notch 抑制不敏感。然而,即使在白血病抑制因子(LIF)存在的情况下,Notch 的激活也能促进分化,表现出与配体偏好相关的谱系区分,Jagged-1 有利于神经分化,Delta-like-4 有利于中胚层。这种差异配体作用涉及影响特定下游靶基因表达的 Notch 受体的组合。尽管 Notch 在早期神经分化过程中的激活特异性地促进神经干细胞或早期神经祖细胞,并延迟其成熟,但它的抑制促进晚期神经祖细胞并加速神经发生,对神经元的偏好超过对神经胶质的偏好。然而,只有当与睫状神经营养因子联合使用时,Notch 的激活才会促进神经胶质发生。因此,我们的研究强调了 Notch 的多方面作用,表明了配体使用和谱系特异性之间的相互依赖性,以及 Notch 作为主开关的作用,对神经发生具有特定阶段的影响。

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