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骨形态发生蛋白-2的活性受分泌型磷蛋白24kd调节,后者是一种细胞外假受体,其基因定位于对骨质量很重要的人类基因组区域。

Bone morphogenetic protein-2 activity is regulated by secreted phosphoprotein-24 kd, an extracellular pseudoreceptor, the gene for which maps to a region of the human genome important for bone quality.

作者信息

Brochmann Elsa J, Behnam Keyvan, Murray Samuel S

机构信息

Geriatric Research, Education and Clinical Center (11-E), VA Greater Los Angeles Healthcare System, Sepulveda, CA 91343, USA.

出版信息

Metabolism. 2009 May;58(5):644-50. doi: 10.1016/j.metabol.2009.01.001.

DOI:10.1016/j.metabol.2009.01.001
PMID:19375587
Abstract

The material properties of bone are the sum of the complex and interrelated anabolic and catabolic processes that modulate formation and turnover. The 2q33-37 region of the human genome contains quantitative trait loci important in determining the broadband ultrasound attenuation (an index of trabecular microarchitecture, bone elasticity, and susceptibility to fracture) of the calcaneus, but no genes of significance to bone metabolism have been identified in this domain. Secreted phosphoprotein-24 kd (SPP24 or SPP2) is a novel and relatively poorly characterized growth hormone-regulated gene that maps to 2q37. The purpose of this review is to summarize the status of research related to spp24 and how it regulates bone morphogenetic protein (BMP) bioactivity in bone. SPP24 codes for an extracellular matrix protein that contains a high-affinity BMP-2-binding transforming growth factor-beta receptor II homology 1 loop similar to those identified in fetuin and the receptor itself. SPP24 is transcribed primarily in the liver and bone. High levels of spp24 (a hydroxyapatite-binding protein) are found in bone, and small amounts are found in fetuin-mineral complexes. Full-length secretory spp24 inhibits ectopic bone formation, and overexpression of spp24 reduces murine bone mass and density. Spp24 is extremely labile to proteolysis, a process that regulates its bioactivity in vivo. For example, an 18.5-kd degradation product of spp24, designated spp18.5, is pro-osteogenic. A synthetic cyclized Cys(1)-to-Cys(19) disulfide-bonded peptide (BMP binding peptide) corresponding to the transforming growth factor-beta receptor II homology 1 domain of spp24 and spp18.5 binds BMP-2 and increases the rate and magnitude of BMP-2-mediated ectopic bone formation. Thus, the mechanism of action of spp18.5 and spp24 may be to regulate the local bioavailability of BMP cytokines. SPP24 is regulated by growth hormone and 3 major families of transcription factors (nuclear factor of activated T cells, CCAAT/enhancer-binding protein, Cut/Cux/CCAAT displacement protein) that regulate mesenchymal cell proliferation, embryonic patterning, and terminal differentiation. The gene contains at least 2 single nucleotide polymorphisms. Given its mechanism of action and sequence variability, SPP24 may be an interesting candidate for future studies of the genetic regulation of bone mass, particularly during periods of BMP-mediated endochondral bone growth, development, and fracture healing.

摘要

骨的材料特性是调节骨形成和更新的复杂且相互关联的合成代谢和分解代谢过程的总和。人类基因组的2q33 - 37区域包含对确定跟骨宽带超声衰减(小梁微结构、骨弹性和骨折易感性的指标)很重要的数量性状基因座,但在该区域尚未鉴定出对骨代谢有重要意义的基因。分泌型磷蛋白24kd(SPP24或SPP2)是一种新的且特征相对较少的生长激素调节基因,定位于2q37。本综述的目的是总结与spp24相关的研究现状以及它如何调节骨中骨形态发生蛋白(BMP)的生物活性。SPP24编码一种细胞外基质蛋白,该蛋白含有一个高亲和力BMP - 2结合转化生长因子 - β受体II同源性1环,类似于胎球蛋白和受体本身中鉴定出的环。SPP24主要在肝脏和骨骼中转录。在骨中发现高水平的spp24(一种羟基磷灰石结合蛋白),在胎球蛋白 - 矿物质复合物中发现少量。全长分泌型spp24抑制异位骨形成,spp24的过表达降低小鼠的骨量和骨密度。Spp24对蛋白水解极其不稳定,这一过程在体内调节其生物活性。例如,spp24的一种18.5kd降解产物,命名为spp18.5,具有促骨生成作用。一种与spp24和spp18.5的转化生长因子 - β受体II同源性1结构域相对应的合成环化Cys(1)至Cys(19)二硫键连接肽(BMP结合肽)结合BMP - 2并增加BMP - 2介导的异位骨形成的速率和幅度。因此,spp18.5和spp24的作用机制可能是调节BMP细胞因子的局部生物利用度。SPP24受生长激素和3个主要转录因子家族(活化T细胞核因子、CCAAT/增强子结合蛋白、Cut/Cux/CCAAT置换蛋白)调节,这些转录因子调节间充质细胞增殖、胚胎模式形成和终末分化。该基因至少包含2个单核苷酸多态性。鉴于其作用机制和序列变异性,SPP24可能是未来骨量遗传调控研究的一个有趣候选对象,特别是在BMP介导的软骨内骨生长发育和骨折愈合期间。

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