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Cdx 对轴伸长的调节

Regulation of axial elongation by Cdx.

机构信息

Department of Cellular and Molecular Medicine, Faculty of Medicine, University of Ottawa, 451 Smyth Road, Ottawa, Ontario, K1H 8M5, Canada.

Department of Cellular and Molecular Medicine, Faculty of Medicine, University of Ottawa, 451 Smyth Road, Ottawa, Ontario, K1H 8M5, Canada.

出版信息

Dev Biol. 2022 Mar;483:118-127. doi: 10.1016/j.ydbio.2021.12.011. Epub 2021 Dec 25.

Abstract

The primordia of the post-otic mouse embryo forms largely from a bipotential cell population containing neuromesodermal progenitors (NMP) which reside in the tail bud and contribute to the elaboration of the major body axis after gastrulation. The mechanisms by which the NMP population is both maintained and subsequently directed down mesodermal and neural lineages is incompletely understood. The vertebrate transcription factor Cdx2, is essential for axial elongation and has been implicated in maintaining the NMP niche and in specification of NMP derivatives. To better understand the role of the Cdx family in axial elongation, we employed a conditional mutant allele which evokes total loss of Cdx function, and enriched for tail bud progenitors through the use of a Pax2-GFP transgenic reporter. Using this approach, we identified 349 Cdx-dependent genes by RNA sequencing (RNA-seq). From these, Gene Ontology and chromatin immunoprecipitation analysis further revealed a number of putative direct Cdx candidate target genes implicated in axial elongation, including Sp8, Isl1, Evx1, Zic3 and Nr2f1. Additional analysis of available single-cell RNA-seq data from mouse tail buds revealed the co-expression of Sp8, Isl1, Evx1 and Zic3 with Cdx2 in putative NMP cells, while Nr2f1 was excluded from this population. These findings identify a number of novel Cdx targets and provide further insight into the critical roles for Cdx in elaborating the post-otic embryo.

摘要

后耳鼠胚的原基主要由具有神经中胚层祖细胞(NMP)的双潜能细胞群体形成,这些细胞位于尾芽中,并在原肠胚后为主要体轴的形成做出贡献。NMP 群体既被维持又被定向到中胚层和神经谱系的机制尚未完全理解。脊椎动物转录因子 Cdx2 对于轴的伸长是必不可少的,并且与 NMP 生态位的维持以及 NMP 衍生物的特化有关。为了更好地理解 Cdx 家族在轴向伸长中的作用,我们使用了一种条件性突变等位基因,该基因可引发 Cdx 功能的完全丧失,并通过使用 Pax2-GFP 转基因报告基因来富集尾芽祖细胞。使用这种方法,我们通过 RNA 测序(RNA-seq)鉴定了 349 个 Cdx 依赖性基因。从中,基因本体论和染色质免疫沉淀分析进一步揭示了一些假定的直接 Cdx 候选靶基因,这些基因与轴向伸长有关,包括 Sp8、Isl1、Evx1、Zic3 和 Nr2f1。对来自小鼠尾芽的现有单细胞 RNA-seq 数据的进一步分析表明,Sp8、Isl1、Evx1 和 Zic3 与 Cdx2 在假定的 NMP 细胞中共同表达,而 Nr2f1 则被排除在该群体之外。这些发现确定了一些新的 Cdx 靶标,并进一步深入了解了 Cdx 在阐述后耳胚胎中的关键作用。

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