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胎儿小鼠下颌骨髁突软骨形成起始阶段Runx2、Osterix和Sox9的原位杂交研究

An in situ hybridization study of Runx2, Osterix, and Sox9 at the onset of condylar cartilage formation in fetal mouse mandible.

作者信息

Shibata Shunichi, Suda Naoto, Suzuki Shoichi, Fukuoka Hiroki, Yamashita Yasuo

机构信息

Maxillofacial Anatomy, Department of Maxillofacial Biology, Tokyo Medical and Dental University, Japan.

出版信息

J Anat. 2006 Feb;208(2):169-77. doi: 10.1111/j.1469-7580.2006.00525.x.

Abstract

Mandibular condylar cartilage is the principal secondary cartilage, differing from primary cartilage in its rapid differentiation from progenitor cells (preosteoblasts/skeletoblasts) to hypertrophic chondrocytes. The expression of three transcription factors related to bone and cartilage formation, namely Runx2, Osterix and Sox9, was investigated at the onset of mouse mandibular condylar cartilage formation by in situ hybridization. Messenger RNAs for these three molecules were expressed in the condylar anlage, consisting of preosteoblasts/skeletoblasts, at embryonic day (E)14. Hypertrophic chondrocytes appeared at E15 as soon as cartilage tissue appeared. Runx2 mRNA was expressed in the embryonic zone at the posterior position of the newly formed cartilage, in the bone collar and in the newly formed cartilage, but expression intensity in the newly formed cartilage was slightly weaker. Osterix mRNA was also expressed in the embryonic zone and in the bone collar, but was at markedly lower levels in the newly formed cartilage. Sox9 mRNA was continuously expressed from the embryonic zone to the newly formed cartilage. At this stage, Sox5 mRNA was expressed only in the newly formed cartilage. These results suggest that reduced expression of Osterix in combination with Sox9-Sox5 expression is important for the onset of condylar (secondary) cartilage formation.

摘要

下颌髁突软骨是主要的次级软骨,与初级软骨不同,它从祖细胞(前成骨细胞/骨骼母细胞)快速分化为肥大软骨细胞。通过原位杂交技术,在小鼠下颌髁突软骨形成开始时,研究了与骨和软骨形成相关的三种转录因子Runx2、Osterix和Sox9的表达情况。在胚胎期(E)14,这三种分子的信使核糖核酸在由前成骨细胞/骨骼母细胞组成的髁突原基中表达。一旦软骨组织出现,肥大软骨细胞在E15时出现。Runx2信使核糖核酸在新形成软骨后部的胚胎区、骨环和新形成的软骨中表达,但在新形成软骨中的表达强度稍弱。Osterix信使核糖核酸也在胚胎区和骨环中表达,但在新形成软骨中的水平明显较低。Sox9信使核糖核酸从胚胎区到新形成的软骨持续表达。在此阶段,Sox5信使核糖核酸仅在新形成的软骨中表达。这些结果表明,Osterix表达降低与Sox9 - Sox5表达相结合,对髁突(次级)软骨形成的开始很重要。

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