Downey M E, Holliday L S, Aguirre J I, Wronski T J
Department of Physiological Sciences, University of Florida, PO Box 100144, JHMHC, Gainesville, FL 32610-0144, USA.
Bone. 2009 Feb;44(2):266-74. doi: 10.1016/j.bone.2008.10.041. Epub 2008 Oct 25.
Prostaglandin E2 receptor subtype 4 agonists (EP4A) and basic fibroblast growth factor (FGF2) stimulate bone formation, but their effects on bone resorption are controversial. To provide additional insight into the skeletal effects of EP4A and FGF2, their regulation of expression of genes associated with bone formation and resorption in aged ovariectomized (OVX) rats and in cultured mouse bone marrow cells was determined. RNA was isolated from lumbar vertebrae of OVX rats (16 months of age) treated daily for 3 weeks with FGF2 or EP4A and processed for quantitative real time-PCR analyses. mRNA expression for the receptor activator of NF-kappaB ligand (RANKL) and cathepsin K (CTSK), but not osteoprotegerin (OPG), were upregulated by both FGF2 and EP4A. Addition of FGF2 and EP4A to the medium of cultured mouse bone marrow cells increased the formation of tartrate resistant acid phosphatase (TRAP) positive cells, upregulated the expression of RANKL and CTSK, and downregulated expression for OPG. EP4A also increased the formation of actin rings, an indicator of osteoclast activation, in a dose dependent manner in osteoclasts cultured on bone slices and triggered the formation of pits as revealed by a pitting assay. Gene expression for osterix (OSX) and IGF-2, genes associated with bone formation, was significantly greater in FGF2-treated OVX rats compared with EP4A-treated OVX rats. These findings at the molecular level are consistent with previous tissue-level histomorphometric findings, and at the doses tested, support the contention that FGF2 has a stronger bone anabolic effect than EP4A. The results of these in vivo and in vitro analyses clarify the effects of FGF2 and EP4A on bone formation and resorption, and provide insight into differences in the efficacy of two potential bone anabolic agents for restoration of lost bone mass in the osteopenic, estrogen-deplete skeleton.
前列腺素E2受体亚型4激动剂(EP4A)和碱性成纤维细胞生长因子(FGF2)可刺激骨形成,但其对骨吸收的影响存在争议。为了进一步深入了解EP4A和FGF2对骨骼的影响,研究了它们对老年去卵巢(OVX)大鼠和培养的小鼠骨髓细胞中与骨形成和吸收相关基因表达的调控。从16月龄的OVX大鼠腰椎中分离RNA,这些大鼠每日用FGF2或EP4A处理3周,然后进行定量实时PCR分析。FGF2和EP4A均上调了核因子κB受体激活蛋白配体(RANKL)和组织蛋白酶K(CTSK)的mRNA表达,但未上调骨保护素(OPG)的表达。向培养的小鼠骨髓细胞培养基中添加FGF2和EP4A可增加抗酒石酸酸性磷酸酶(TRAP)阳性细胞的形成,上调RANKL和CTSK的表达,并下调OPG的表达。EP4A还以剂量依赖性方式增加了在骨切片上培养的破骨细胞中肌动蛋白环的形成,肌动蛋白环是破骨细胞激活的指标,并且通过蚀斑试验显示EP4A触发了蚀斑的形成。与EP4A处理的OVX大鼠相比,FGF2处理的OVX大鼠中与骨形成相关的osterix(OSX)和IGF-2基因表达明显更高。这些分子水平的发现与先前组织水平的组织形态计量学发现一致,并且在所测试的剂量下,支持FGF2比EP4A具有更强的骨合成代谢作用这一观点。这些体内和体外分析的结果阐明了FGF2和EP4A对骨形成和吸收的影响,并深入了解了两种潜在的骨合成代谢药物在恢复骨质疏松、雌激素缺乏骨骼中丢失的骨量方面疗效的差异。