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Two Origins of Blastemal Progenitors Define Blastemal Regeneration of Zebrafish Lower Jaw

机译:胚基前体细胞起源的两个斑马鱼的定义下颌的胚基再生

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摘要

Zebrafish possess a remarkable ability to regenerate complicated structures by formation of a mass of undifferentiated mesenchymal cells called blastema. To understand how the blastema retains the original structural form, we investigate cellular transitions and transcriptional characteristics of cell identity genes during all stages of regeneration of an amputated lower jaw. We find that mesenchymal blastema originates from multiple sources including nucleated blood cells, fibroblasts, damaged muscle cells and pigment cells. These cells are transformed into two populations of blastemal progenitors: foxi1-expression and isl1-expression, before giving rise to cartilage, bone, and muscle. Time point- based transcriptomal analysis of 45 annotated Hox genes reveal that five 3′-end Hox genes and an equal number of 5′-end Hox genes are activated largely at the stage of blastema reformation. RNA in situ hybridization shows that foxi1 and pax3a are respectively expressed in the presumptive mandible skeletal region and regenerating muscle at 5 dpa. In contrast, hoxa2b and hoxa11b are widely expressed with different domain in chondrogenic blastema and blastema mesenchyme. Knockdown foxi1 changes the expression patterns of sox9a and hoxa2b in chondrogenic blastema. From these results we propose that two origins of blastemal progenitors define blastema skeleton and muscle respecifications through distinct signaling pathways. Meanwhile, the positional identity of blastema reformation is implicated in mesenchymal segmentation and characteristic expression pattern of Hox genes.
机译:斑马鱼具有通过形成大量未分化的间充质细胞(胚细胞)来再生复杂结构的显着能力。为了了解胚细胞如何保留原始结构形式,我们研究了截肢下颌再生的所有阶段的细胞迁移和细胞同一性基因的转录特征。我们发现间充质细胞起源于多种来源,包括有核血细胞,成纤维细胞,受损的肌肉细胞和色素细胞。在产生软骨,骨骼和肌肉之前,这些细胞被转化为两个胚祖细胞群:foxi1表达和isl1表达。对45个带注释的Hox基因进行基于时间点的转录组分析,发现五个3'-端Hox基因和相等数量的5'-端Hox基因在胚泡重构阶段被大量激活。 RNA原位杂交表明,foxi1和pax3a分别在推测的下颌骨骨骼区域和5 dpa的再生肌肉中表达。相比之下,hoxa2b和hoxa11b在软骨母细胞和母细胞间质中以不同的域广泛表达。敲低foxi1改变软骨形成性母细胞中sox9a和hoxa2b的表达模式。根据这些结果,我们提出胚细胞祖细胞的两个起源通过不同的信号传导途径定义了胚细胞的骨骼和肌肉的重新指定。同时,胚泡再形成的位置同一性与Hox基因的间质分割和特征性表达模式有关。

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