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首页> 外文期刊>Journal of molecular histology >FAM20A is essential for amelogenesis, but is dispensable for dentinogenesis
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FAM20A is essential for amelogenesis, but is dispensable for dentinogenesis

机译:FAM20A对蛋白发生至关重要,但对于牙本质发生是必不可少的

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摘要

Mutations in the gene encoding family with sequence similarity 20, member A (FAM20A) caused amelogenesis imperfecta (AI), in humans. However, the roles of FAM20A in amelogenesis and dentinogenesis are poorly understood. In this study, we generated a Fam20a knockout (Sox2-Cre;Fam20a(fl/fl)) mouse model by crossing Fam20a(fl/fl) mice with Sox2-Cre transgenic mice, in which Fam20a was ablated in both dental epithelium and dental mesenchyme. We found that these mice developed an enamel phenotype that resembles human AI associated with FAM20A mutations, but did not have apparent dentin defects. The secretory stage ameloblasts in the mandibular incisors from the Sox2-Cre;Fam20a(fl/fl) mice were shorter and detached from the enamel matrix, and subsequently lost their polarity, became disorganized and formed numerous spherical extracellular matrices in place of normal enamel. At the molecular level, the Sox2-Cre;Fam20a(fl/fl) mice displayed dramatically reduced expression levels of the genes encoding the enamel matrix proteins, but unaltered levels of the genes encoding the dentin matrix proteins. Moreover, Fam20a ablation resulted in a great decrease in FAM20C protein level, but it did not alter the intracellular localization of FAM20C protein in ameloblasts and odontoblasts. These results indicate that FAM20A is essential for amelogenesis, but is dispensable for dentinogenesis.
机译:编码序列相似性20的基因中的突变,成员A(FAM20A)在人体中引起Amelogesis渗透(AI)。然而,FAM20A在AMELOCAESES和牙进发生中的角色易于理解。在这项研究中,我们通过SOX2-CRE转基因小鼠交叉FAM20A(FL / FL)小鼠来产生FAM20A敲除(SOX2-CRE; FAM20A(FL / FL))小鼠模型,其中FAM20A在牙科上皮和牙科中烧蚀间充质。我们发现这些小鼠开发了一种类似于FAM20A突变的人AI的牙釉质表型,但没有明显的牙本质缺陷。来自SOX2-CRE的下颌切牙中的分泌阶段Amelobrasts; FAM20A(FL / FL)小鼠较短并从牙釉质基质中脱离,随后失去了它们的极性,变得紊乱并形成了许多球形细胞外基质代替正常的牙釉质。在分子水平,SOX2-CRE; FAM20A(FL / FL)小鼠显着降低了编码牙釉质基质蛋白的基因的表达水平,但是未经干预的牙本质基质蛋白的基因水平。此外,FAM20A消融导致FAM20C蛋白质水平的巨大降低,但它没有改变Ameloblasts和Odontoblast中FAM20C蛋白的细胞内定位。这些结果表明,FAM20A对AMELO发生至关重要,但对于牙本发生是必不可少的。

著录项

  • 来源
    《Journal of molecular histology 》 |2019年第6期| 共11页
  • 作者单位

    Texas A&

    M Univ Coll Dent Dept Biomed Sci 3302 Gaston Ave Room 436 Dallas TX 75246 USA;

    Texas A&

    M Univ Coll Dent Dept Biomed Sci 3302 Gaston Ave Room 436 Dallas TX 75246 USA;

    Texas A&

    M Univ Coll Dent Dept Biomed Sci 3302 Gaston Ave Room 436 Dallas TX 75246 USA;

    Texas A&

    M Univ Coll Dent Dept Biomed Sci 3302 Gaston Ave Room 436 Dallas TX 75246 USA;

    Texas A&

    M Univ Coll Dent Dept Biomed Sci 3302 Gaston Ave Room 436 Dallas TX 75246 USA;

    Texas A&

    M Univ Coll Dent Dept Biomed Sci 3302 Gaston Ave Room 436 Dallas TX 75246 USA;

    Texas A&

    M Univ Coll Dent Dept Biomed Sci 3302 Gaston Ave Room 436 Dallas TX 75246 USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 普通生物学 ;
  • 关键词

    Tooth development; Enamel; Dentin; Biomineralization; Cell differentiation; Genetics;

    机译:牙齿发育;牙釉质;牙本质;生物丙酸;细胞分化;遗传学;

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