Departments of Pathology Orthopaedic Surgery, Yamagata University School of Medicine, Yamagata, Japan.
Pathol Int. 2011 Oct;61(10):565-71. doi: 10.1111/j.1440-1827.2011.02706.x. Epub 2011 Aug 9.
The heterozygous germline mutation of runt-related protein 2 (RUNX2) causes cleidocranial dysplasia. To clarify the involvement of RUNX2 in human osteogenesis, fetal bones and various bone tumors were immunohistochemically examined. During both membranous and endochondral ossification in the fetus (n= 8), RUNX2 was expressed not only in osteoblastic cells but also in surrounding mesenchymal cells and early stage chondrocytes. Such an expression pattern was recapitulated in bone tumors: RUNX2 was unequivocally expressed in osteosarcoma (n= 20) and fibrous dysplasia (n= 10), regardless of the site of occurrence, cell morphology or amount of neoplastic osteoid. RUNX2 expression was limited to less differentiated cells in chondrogenic tumors (n= 20). We further analyzed whether RUNX2 expression was regulated by bone morphogenetic protein-2 (BMP-2), which is critical for osteoblastic differentiation. With real-time polymerase chain reaction, the RUNX2 mRNA level was correlated with BMP-2 mRNA level, and both levels were significantly higher in three osteosarcoma cell lines than in three chondrosarcoma cell lines. With treatment of recombinant BMP-2, the RUNX2 mRNA level was significantly altered in these cell lines. RUNX2 expression is constitutive in developing and neoplastic human osteogenesis, and is most likely to be regulated by BMP-2.
Runt 相关转录因子 2(RUNX2)的杂合胚系突变可导致颅骨锁骨发育不全。为了阐明 RUNX2 参与人类成骨作用的机制,我们对胎儿骨骼和各种骨肿瘤进行了免疫组织化学检查。在胎儿的膜内和软骨内成骨过程中(n=8),RUNX2 不仅在成骨细胞中表达,而且在周围的间充质细胞和早期软骨细胞中也表达。这种表达模式在骨肿瘤中得到了重现:在骨肉瘤(n=20)和纤维结构不良(n=10)中,RUNX2 均明确表达,而不论肿瘤发生的部位、细胞形态或肿瘤性类骨质的数量如何。在软骨性肿瘤(n=20)中,RUNX2 表达仅限于分化程度较低的细胞。我们进一步分析了 RUNX2 表达是否受骨形态发生蛋白-2(BMP-2)调控,因为 BMP-2 对于成骨细胞分化至关重要。通过实时聚合酶链反应,我们发现 RUNX2 mRNA 水平与 BMP-2 mRNA 水平相关,并且在三个骨肉瘤细胞系中的水平均明显高于三个软骨肉瘤细胞系中的水平。用重组 BMP-2 处理后,这些细胞系中的 RUNX2 mRNA 水平发生了明显改变。在人类发育和成骨肿瘤中,RUNX2 表达是组成性的,并且很可能受 BMP-2 调控。
