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分子特征可识别早期小鼠肢芽中的未成熟间充质祖细胞,这些祖细胞对形态发生素信号的反应存在差异。

Molecular signatures identify immature mesenchymal progenitors in early mouse limb buds that respond differentially to morphogen signaling.

机构信息

Developmental Genetics, Department of Biomedicine, University of Basel, 4058 Basel, Switzerland.

Development and Evolution, Centro Andaluz de Biología del Desarrollo, Universidad Pablo de Olavide, 41013 Sevilla, Spain.

出版信息

Development. 2019 May 28;146(10):dev173328. doi: 10.1242/dev.173328.

Abstract

The key molecular interactions governing vertebrate limb bud development are a paradigm for studying the mechanisms controlling progenitor cell proliferation and specification during vertebrate organogenesis. However, little is known about the cellular heterogeneity of the mesenchymal progenitors in early limb buds that ultimately contribute to the chondrogenic condensations prefiguring the skeleton. We combined flow cytometric and transcriptome analyses to identify the molecular signatures of several distinct mesenchymal progenitor cell populations present in early mouse forelimb buds. In particular, jagged 1 (JAG1)-positive cells located in the posterior-distal mesenchyme were identified as the most immature limb bud mesenchymal progenitors (LMPs), which crucially depend on SHH and FGF signaling in culture. The analysis of gremlin 1 ()-deficient forelimb buds showed that JAG1-expressing LMPs are protected from apoptosis by GREM1-mediated BMP antagonism. At the same stage, the osteo-chondrogenic progenitors (OCPs) located in the core mesenchyme are already actively responding to BMP signaling. This analysis sheds light on the cellular heterogeneity of the early mouse limb bud mesenchyme and on the distinct response of LMPs and OCPs to morphogen signaling.

摘要

控制脊椎动物肢芽发育的关键分子相互作用是研究脊椎动物器官发生过程中祖细胞增殖和特化的机制的典范。然而,对于早期肢芽中最终有助于软骨形成凝聚的间充质祖细胞的细胞异质性知之甚少,这些凝聚预示着骨骼的形成。我们结合流式细胞术和转录组分析,鉴定了早期小鼠前肢芽中存在的几个不同间充质祖细胞群体的分子特征。特别是,位于后-远侧间充质中的 jagged 1(JAG1)阳性细胞被鉴定为最不成熟的肢芽间充质祖细胞(LMPs),它们在培养中严重依赖 SHH 和 FGF 信号。对 gremlin 1 () 缺陷的前肢芽的分析表明,JAG1 表达的 LMPs 通过 GREM1 介导的 BMP 拮抗作用免受凋亡。在同一阶段,位于核心间充质中的成骨-软骨祖细胞(OCPs)已经对 BMP 信号做出积极响应。这项分析揭示了早期小鼠肢芽间充质的细胞异质性,以及 LMPs 和 OCPs 对形态发生素信号的不同反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/38d0/6550019/5babaac23f87/develop-146-173328-g1.jpg

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