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头部到尾部的体轴形成过程中的神经中胚层特化。

Neuromesodermal specification during head-to-tail body axis formation.

机构信息

Institute of Molecular Biotechnology of the Austrian Academy of Sciences, Vienna BioCenter, Vienna, Austria.

Centre for Regenerative Medicine, Institute for Stem Cell Research, School of Biological Sciences, University of Edinburgh, Edinburgh, United Kingdom.

出版信息

Curr Top Dev Biol. 2024;159:232-271. doi: 10.1016/bs.ctdb.2024.02.012. Epub 2024 Mar 19.

DOI:10.1016/bs.ctdb.2024.02.012
PMID:38729677
Abstract

The anterior-to-posterior (head-to-tail) body axis is extraordinarily diverse among vertebrates but conserved within species. Body axis development requires a population of axial progenitors that resides at the posterior of the embryo to sustain elongation and is then eliminated once axis extension is complete. These progenitors occupy distinct domains in the posterior (tail-end) of the embryo and contribute to various lineages along the body axis. The subset of axial progenitors with neuromesodermal competency will generate both the neural tube (the precursor of the spinal cord), and the trunk and tail somites (producing the musculoskeleton) during embryo development. These axial progenitors are called Neuromesodermal Competent cells (NMCs) and Neuromesodermal Progenitors (NMPs). NMCs/NMPs have recently attracted interest beyond the field of developmental biology due to their clinical potential. In the mouse, the maintenance of neuromesodermal competency relies on a fine balance between a trio of known signals: Wnt/β-catenin, FGF signalling activity and suppression of retinoic acid signalling. These signals regulate the relative expression levels of the mesodermal transcription factor Brachyury and the neural transcription factor Sox2, permitting the maintenance of progenitor identity when co-expressed, and either mesoderm or neural lineage commitment when the balance is tilted towards either Brachyury or Sox2, respectively. Despite important advances in understanding key genes and cellular behaviours involved in these fate decisions, how the balance between mesodermal and neural fates is achieved remains largely unknown. In this chapter, we provide an overview of signalling and gene regulatory networks in NMCs/NMPs. We discuss mutant phenotypes associated with axial defects, hinting at the potential significant role of lesser studied proteins in the maintenance and differentiation of the progenitors that fuel axial elongation.

摘要

脊椎动物的体轴从前到后(头到尾)具有非常多样的形式,但在物种内是保守的。体轴的发育需要一群位于胚胎后端的轴向祖细胞来维持伸长,一旦轴延伸完成,这些祖细胞就会被消除。这些祖细胞在胚胎的后端(尾部)占据不同的区域,并沿着体轴为各种谱系做出贡献。具有神经中胚层能力的轴向祖细胞亚群将在胚胎发育过程中产生神经管(脊髓的前体)以及躯干和尾部体节(产生骨骼肌肉)。这些轴向祖细胞被称为神经中胚层祖细胞(NMC)和神经中胚层前体细胞(NMP)。由于其临床潜力,NMC/NMP 最近除了在发育生物学领域之外,也引起了其他领域的关注。在小鼠中,神经中胚层能力的维持依赖于三种已知信号之间的精细平衡:Wnt/β-catenin、FGF 信号活性和视黄酸信号抑制。这些信号调节中胚层转录因子 Brachyury 和神经转录因子 Sox2 的相对表达水平,允许当它们共同表达时维持祖细胞身份,并且当平衡分别向 Brachyury 或 Sox2 倾斜时分别进行中胚层或神经谱系的承诺。尽管在理解这些命运决定中涉及的关键基因和细胞行为方面取得了重要进展,但如何实现中胚层和神经命运之间的平衡在很大程度上仍然未知。在本章中,我们提供了 NMC/NMP 中信号和基因调控网络的概述。我们讨论了与轴向缺陷相关的突变表型,这些表型暗示了在维持和分化为轴向伸长提供动力的祖细胞中,较少研究的蛋白质可能具有重要作用。

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