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软骨衍生形态发生蛋白和成骨蛋白-1对成骨作用有不同的调节作用。

Cartilage-derived morphogenetic proteins and osteogenic protein-1 differentially regulate osteogenesis.

作者信息

Erlacher L, McCartney J, Piek E, ten Dijke P, Yanagishita M, Oppermann H, Luyten F P

机构信息

Craniofacial and Skeletal Diseases Branch, National Institute of Dental Research, National Institutes of Health, Bethesda, Maryland, USA.

出版信息

J Bone Miner Res. 1998 Mar;13(3):383-92. doi: 10.1359/jbmr.1998.13.3.383.

DOI:10.1359/jbmr.1998.13.3.383
PMID:9525338
Abstract

Cartilage-derived morphogenetic proteins-1 and -2 (CDMP-1 and CDMP-2) are members of the bone morphogenetic protein (BMP) family, which play important roles in embryonic skeletal development. We studied the biological activities of recombinant CDMP-1 and CDMP-2 in chondrogenic and osteogenic differentiation and investigated their binding properties to type I and type II serine/threonine kinase receptors. In vivo, CDMP-1 and CDMP-2 were capable of inducing dose-dependently de novo cartilage and bone formation in an ectopic implantation assay. In vitro studies using primary chondrocyte cultures showed that both CDMP-1 and CDMP-2 stimulated equally de novo synthesis of proteoglycan aggrecan in a concentration-dependent manner. This activity was equipotent when compared with osteogenic protein-1 (OP-1). In contrast, CDMPs were less stimulatory than OP-1 in osteogenic differentiation as evaluated by alkaline phosphatase activity and expression levels of bone markers in ATDC5, ROB-C26, and MC3T3-E1 cells. CDMP-2 was the least osteogenic in these assays. Receptor binding studies of CDMP-1 and CDMP-2 revealed that both have affinity for the BMP receptor type IB (BMPR-IB) and BMPR-II, and weakly for BMPR-IA. Moreover, using a promoter/reporter construct, transcriptional activation signal was transduced by BMPR-IB in the presence of BMPR-II upon CDMP-1 and CDMP-2 binding. Our data show that distinct members of the BMP family differentially regulate the progression in the osteogenic lineage, and this may be due to their selective affinity for specific receptor complexes.

摘要

软骨衍生形态发生蛋白-1和-2(CDMP-1和CDMP-2)是骨形态发生蛋白(BMP)家族的成员,它们在胚胎骨骼发育中起重要作用。我们研究了重组CDMP-1和CDMP-2在软骨形成和成骨分化中的生物学活性,并研究了它们与I型和II型丝氨酸/苏氨酸激酶受体的结合特性。在体内,CDMP-1和CDMP-2在异位植入试验中能够剂量依赖性地诱导从头软骨和骨形成。使用原代软骨细胞培养物的体外研究表明,CDMP-1和CDMP-2均以浓度依赖性方式同等程度地刺激蛋白聚糖聚集蛋白聚糖的从头合成。与成骨蛋白-1(OP-1)相比,该活性相当。相反,通过碱性磷酸酶活性以及ATDC5、ROB-C26和MC3T3-E1细胞中骨标志物的表达水平评估,CDMPs在成骨分化中的刺激作用比OP-1小。在这些试验中,CDMP-2的成骨作用最小。CDMP-1和CDMP-2的受体结合研究表明,二者对骨形态发生蛋白受体IB型(BMPR-IB)和BMPR-II均具有亲和力,而对BMPR-IA的亲和力较弱。此外,使用启动子/报告基因构建体,在CDMP-1和CDMP-2结合后,BMPR-IB在BMPR-II存在的情况下转导转录激活信号。我们的数据表明,BMP家族的不同成员对成骨谱系的进展有不同的调节作用,这可能是由于它们对特定受体复合物的选择性亲和力所致。

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