首页> 外文期刊>Orthodontics & craniofacial research >Abnormal craniofacial development and expression patterns of extracellular matrix components in transgenic Del1 mice harboring a deletion mutation in the type II collagen gene
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Abnormal craniofacial development and expression patterns of extracellular matrix components in transgenic Del1 mice harboring a deletion mutation in the type II collagen gene

机译:II型胶原基因缺失突变的转基因Del1小鼠颅面发育异常和细胞外基质成分表达模式

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Objective To analyze the effect of a type II collagen mutation on craniofacial development in transgenic Del1 mice. Design Samples from homozygous (+/+) and heterozygous (+/-) transgenic Del1 mice harboring mutations in the type II collagen gene as well as non-transgenic (-/-) littermates were collected at days 12.5, 14.5, 16.5 and 18.5 of gestation. The cartilaginous and bony elements of the craniofacial skeleton were analyzed after staining with alcian blue, alizarin red S and von Kossa. The expression patterns of type II, IX and X collagens and aggrecan were analyzed by immunohistochemistry and in situ hybridization. Results Several abnormalities were observed in the craniofacial skeleton of transgenic Del1 mice. These include an overall retardation of chondrogenesis and osteogenesis in Del1 +/+ mice, and to a lesser extent also in Del1+/- mice. Characteristic findings in Del1 +/+ mice included a reduced anterioposterior length, a smaller size of the mandible, a palatal cleft and a downward bending snout. We also detected retarded ossification of calvarial bones in Del1 +/+ and +/- mice when compared with Del1 -/- mice. A surprising finding was the presence of both type II and X collagens and their mRNAs in the periosteum of the cranial base. Conclusion The present study confirms the important role of type II collagen mutation in craniofacial development and growth. In addition to affecting endochondral ossification, the type II collagen mutation also disturbs intramembranous ossification in the developing craniofacial skeleton.
机译:目的分析II型胶原蛋白突变对转基因Del1小鼠颅面发育的影响。在第12.5、14.5、16.5和18.5天收集来自II型胶原基因突变的纯合(+ / +)和杂合(+/-)转基因Del1小鼠以及非转基因(-/-)同窝仔的设计样品妊娠用阿尔辛蓝,茜素红S和von Kossa染色后,对颅面骨骼的软骨和骨成分进行了分析。通过免疫组织化学和原位杂交分析II,IX和X型胶原蛋白和聚集蛋白聚糖的表达模式。结果转基因Del1小鼠的颅面骨骼中观察到一些异常。这些包括在Del1 + / +小鼠中软骨生成和成骨的总体延迟,在Del1 +/-小鼠中也较小。 Del1 + / +小鼠的特征性发现包括前后长度减少,下颌骨尺寸变小,a裂和鼻弯向下。与Del1-/-小鼠相比,我们还检测到Del1 + / +和+/-小鼠的颅骨骨化延迟。令人惊讶的发现是颅底骨膜中同时存在II型和X型胶原蛋白及其mRNA。结论本研究证实了II型胶原突变在颅面发育和生长中的重要作用。除了影响软骨内骨化外,II型胶原蛋白突变还干扰正在发育的颅面骨骼中的膜内骨化。

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