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首页> 外文期刊>Mechanisms of Development >Cell autonomous requirement for TGF-beta signaling during odontoblast differentiation and dentin matrix formation
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Cell autonomous requirement for TGF-beta signaling during odontoblast differentiation and dentin matrix formation

机译:成牙本质细胞分化和牙本质基质形成过程中TGF-β信号传导的细胞自主需求

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摘要

TGF-beta subtypes are expressed in tissues derived from cranial neural crest cells during early mouse craniofacial development. TGF-beta signaling is critical for mediating epithelial-mesenchymal interactions, including those vital for tooth morphogenesis. However, it remains unclear how TGF-beta signaling contributes to the terminal differentiation of odontoblast and dentin formation during tooth morphogenesis. Towards this end, we generated mice with conditional inactivation of the Tgfbr2 gene in cranial neural crest derived cells. Odontoblast differentiation was substantially delayed in the Tgfbr2(fl/fl);Wnt1-Cre mutant mice at E18.5. Following kidney capsule transplantation, Tgfbr2 mutant tooth germs expressed a reduced level of Col1a1 and Dspp and exhibited defects including decreased dentin thickness and absent dentinal tubules. In addition, the expression of the intermediate filament nestin was decreased in the Tgfbr2 mutant samples. Significantly, exogenous TGF-beta2 induced nestin and Dspp expression in dental pulp cells in the developing tooth organ. Our data suggest that TGF-beta signaling controls odontoblast maturation and dentin formation during tooth morphogenesis.
机译:在早期颅面发育过程中,TGF-β亚型在源自颅神经c细胞的组织中表达。 TGF-β信号传导对于介导上皮-间质相互作用(包括对牙齿形态发生至关重要的相互作用)至关重要。但是,尚不清楚TGF-β信号如何在牙齿形态发生过程中促进成牙本质细胞和牙本质形成的最终分化。为此,我们在颅神经rest衍生细胞中产生了Tgfbr2基因有条件失活的小鼠。在E18.5,Tgfbr2(fl / fl); Wnt1-Cre突变小鼠的成牙本质细胞分化明显延迟。肾囊移植后,Tgfbr2突变的牙胚表达的Col1a1和Dspp含量降低,并表现出缺陷,包括牙本质厚度降低和牙本质小管缺失。另外,在Tgfbr2突变体样品中,中间丝巢蛋白的表达降低了。重要的是,外源性TGF-β2诱导了牙齿器官发育中牙髓细胞中巢蛋白和Dspp的表达。我们的数据表明,TGF-β信号传导控制牙齿形态发生过程中成牙本质细胞的成熟和牙本质的形成。

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