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Wnt11 通过作用于皮肌节细胞来指导轴旁肌体节的形态发生。

Wnt11 acts on dermomyotome cells to guide epaxial myotome morphogenesis.

机构信息

Department of Biological Sciences, Graduate School of Science, University of Tokyo, Tokyo, Japan.

Centre for Organismal Studies, Heidelberg University, Heidelberg, Germany.

出版信息

Elife. 2022 May 6;11:e71845. doi: 10.7554/eLife.71845.

Abstract

The dorsal axial muscles, or epaxial muscles, are a fundamental structure covering the spinal cord and vertebrae, as well as mobilizing the vertebrate trunk. To date, mechanisms underlying the morphogenetic process shaping the epaxial myotome are largely unknown. To address this, we used the medaka -enhancer mutant (), which exhibits ventralized dorsal trunk structures resulting in impaired epaxial myotome morphology and incomplete coverage over the neural tube. In wild type, dorsal dermomyotome (DM) cells reduce their proliferative activity after somitogenesis. Subsequently, a subset of DM cells, which does not differentiate into the myotome population, begins to form unique large protrusions extending dorsally to guide the epaxial myotome dorsally. In , by contrast, DM cells maintain the high proliferative activity and mainly form small protrusions. By combining RNA- and ChIP-sequencing analyses, we revealed direct targets of Zic1, which are specifically expressed in dorsal somites and involved in various aspects of development, such as cell migration, extracellular matrix organization, and cell-cell communication. Among these, we identified as a crucial factor regulating both cell proliferation and protrusive activity of DM cells. We propose that dorsal extension of the epaxial myotome is guided by a non-myogenic subpopulation of DM cells and that empowers the DM cells to drive the coverage of the neural tube by the epaxial myotome.

摘要

背轴肌肉,或轴上肌肉,是覆盖脊髓和脊椎的基本结构,也是运动脊椎动物躯干的结构。迄今为止,形成轴上肌体形态发生过程的机制在很大程度上尚不清楚。为了解决这个问题,我们使用了 medaka -enhancer 突变体 (),它表现出腹侧化的背侧躯干结构,导致轴上肌体形态受损和神经管覆盖不完全。在野生型中,背侧真皮肌节 (DM) 细胞在体节形成后会降低其增殖活性。随后,一部分 DM 细胞不会分化为肌体群体,开始形成独特的大突起,向背部延伸,引导轴上肌体向背部延伸。相比之下,DM 细胞保持高增殖活性,主要形成小突起。通过结合 RNA 和 ChIP-seq 分析,我们揭示了 Zic1 的直接靶标,这些靶标特异性表达在背侧体节中,参与各种发育方面,如细胞迁移、细胞外基质组织和细胞间通讯。在这些靶标中,我们确定了 作为调节 DM 细胞增殖和突起活性的关键因素。我们提出,轴上肌体的背侧延伸是由 DM 细胞的非肌肉亚群引导的,而 赋予 DM 细胞动力,以覆盖神经管的轴上肌体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/51f6/9075960/18cc5f8f5dd0/elife-71845-fig1.jpg

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