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Hox 基因在第二心脏场域内定义了不同的祖细胞亚区。

Hox genes define distinct progenitor sub-domains within the second heart field.

机构信息

Laboratoire de Génétique Médicale et Génomique Fonctionnelle, Inserm UMR_S910, Université d'Aix-Marseille, 27 Bd Jean Moulin, 13005 Marseille, France.

出版信息

Dev Biol. 2011 May 15;353(2):266-74. doi: 10.1016/j.ydbio.2011.02.029. Epub 2011 Mar 6.

DOI:10.1016/j.ydbio.2011.02.029
PMID:21385575
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3115524/
Abstract

Much of the heart, including the atria, right ventricle and outflow tract (OFT) is derived from a progenitor cell population termed the second heart field (SHF) that contributes progressively to the embryonic heart during cardiac looping. Several studies have revealed anterior-posterior patterning of the SHF, since the anterior region (anterior heart field) contributes to right ventricular and OFT myocardium whereas the posterior region gives rise to the atria. We have previously shown that Retinoic Acid (RA) signal participates to this patterning. We now show that Hoxb1, Hoxa1, and Hoxa3, as downstream RA targets, are expressed in distinct sub-domains within the SHF. Our genetic lineage tracing analysis revealed that Hoxb1, Hoxa1 and Hoxa3-expressing cardiac progenitor cells contribute to both atria and the inferior wall of the OFT, which subsequently gives rise to myocardium at the base of pulmonary trunk. By contrast to Hoxb1(Cre), the contribution of Hoxa1-enhIII-Cre and Hoxa3(Cre)-labeled cells is restricted to the distal regions of the OFT suggesting that proximo-distal patterning of the OFT is related to SHF sub-domains characterized by combinatorial Hox genes expression. Manipulation of RA signaling pathways showed that RA is required for the correct deployment of Hox-expressing SHF cells. This report provides new insights into the regulatory gene network in SHF cells contributing to the atria and sub-pulmonary myocardium.

摘要

心脏的大部分组织,包括心房、右心室和流出道(OFT),均来源于被称为第二心脏场(SHF)的祖细胞群,该细胞群在心脏环化过程中逐渐为胚胎心脏做出贡献。几项研究揭示了 SHF 的前后模式,因为前区域(前心脏场)有助于右心室和 OFT 心肌,而后区域则产生心房。我们之前已经表明,视黄酸(RA)信号参与了这种模式形成。我们现在表明,作为 RA 的下游靶标,Hoxb1、Hoxa1 和 Hoxa3 在 SHF 内的不同亚区表达。我们的遗传谱系追踪分析表明,表达 Hoxb1、Hoxa1 和 Hoxa3 的心脏祖细胞有助于心房和 OFT 的下壁,随后在肺动脉干基部产生心肌。与 Hoxb1(Cre)不同,Hoxa1-enhIII-Cre 和 Hoxa3(Cre)标记的细胞的贡献仅限于 OFT 的远端区域,这表明 OFT 的近-远模式与以组合 Hox 基因表达为特征的 SHF 亚区有关。RA 信号通路的操纵表明,RA 是 SHF 细胞中正确表达 Hox 所需的。本报告为参与心房和亚肺心肌的 SHF 细胞的调控基因网络提供了新的见解。

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Endogenous retinoic acid regulates cardiac progenitor differentiation.内源性视黄酸调节心脏祖细胞的分化。
小鼠颅神经板中时空基因表达的单细胞图谱。
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A single-cell atlas of spatial and temporal gene expression in the mouse cranial neural plate.小鼠颅神经板中空间和时间基因表达的单细胞图谱。
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