双膦酸盐对骨形成蛋白诱导骨骨吸收抑制作用的研究

目的研究双膦酸盐(bisphosphonate YM 175)对骨形成蛋白(bone morphogenetic protein．简称BMP)诱导骨骨吸收的抑制作用。方法 42只大白鼠背部植入BMP,诱导出异位骨后,将大白鼠分成2组,即投药组和对照组。投药组在BMP植入后第3w至第7w,双膦酸盐(YM 175)每周投药3次,剂量1(μg／kg．d)。对照组按同样的方式给予等量的生理盐水。在BMP植入第3w、 4w、7w和10w,将BMP诱导骨取出,采用TRAP和cathepsin K染色方法来观察双膦酸盐对破骨细胞的作用。结果 BMP诱导骨3w时(即未投双膦酸盐药前),在BMP植入体周边形成编织骨 (woven bone),大量破骨细胞出现在新生骨组织表面。在4 w时,双膦酸盐投药组和对照组,新生骨组织均向BMP植入体内生长,但双膦酸盐投药组的破骨细胞较对照组有减少。在10 w时,双膦酸盐投药组和对照组均可观察到骨细胞变小并且有规律地排列的板层状骨(lamellar bone)的特征。而双膦酸盐投药组,破骨细胞死亡,与对照组比较,破骨细胞数目明显减少。结论双膦酸盐对破骨细胞性骨吸收有明显的抑制作用。     

Motility and resorption: Osteoclastic activity in vitro

Summary Rabbit osteoclasts (OCs), separated mechanically from long bones, were seeded on to glass or plastic substrates or slabs of sperm whale dentine (SWD). Cells were cultured in MEM with 10% FCS with or without added salmon calcitonin (SCT) at dosages of 0.001, 0.1 and 1 IU/ml. Although most rabbit SCT-treated OCs on the non-biological substrates showed inhibition of peripheral ruffling activity and motility at dosages that stop rat OC movement, resorption still occurred on the dentine. Thus such inhibition is unreliable as a general indicator for resorptive capability. Resorption lacunae were observed at all times from 6 h onwards. Using stereophotogrammetric techniques, the following minimum values were obtained from 24 h cultures: highest hourly rate of resorption of dentine for single OC, 570 m³/h; average rate 165 m³/h; mean total volume dentine removed per Howship's lacuna complex, 3,885 m³; average value for plan area of surface attacked per OC, 1,450 m².     

A comparison of resistance and aerobic training for mass, strength and turnover of bone in growing rats

To determine the effects of resistance versus aerobic exercise on the mass, strength and turnover of bone, thirty Sprague Dawley rats (4 weeks of age) were assigned to one of three experimental groups: sedentary, running or jumping. In the jumping group, the trunk was kept upright during electrically stimulated jumping exercise for 1 h every other day. The running rats ran at speeds of 24 m/min for 1 h every other day. After 4 weeks, the jumping rats exhibited increases in the mass and strength of the lumbar vertebrae and of the mid-diaphysis of the femur (mid-femur), and increases in the cross-sectional morphology of these bones: the trabecular bone volume per bone surface, the trabecular thickness, the trabecular bone formation rate per bone surface (BFR/BS). In addition, they exhibited reduced trabecular separation and the area of osteoclast surface per bone surface. The running and sedentary rats showed no such changes. With regard to the mid-femur, in both the jumping and running rats the periosteal BFR/BS was increased. However, only the jumping rats showed a reduction in the BFR/BS at the endocortical surface. These results suggest that resistance exercise accelerates cortical drift and increases the bone mass and strength by stimulating bone formation more efficiently than does aerobic exercise. Accepted: 9 August 2000     

Osteoclast abnormalities in idiopathic osteopetrosis

Summary In order to investigate skeletal abnormalities in a case of idiopathic osteopetrosis, a bone biopsy was taken from the anterior iliac crest and prepared for ultrastructural and histochemical study. There was a drastic reduction in osteoclastic bone resorption. The ruffle border and sealing zone, which are the osteoclast cell surface markers of bone resorption, were absent. The cells were highly vacuolated, and the vacuoles contained large amounts of a residual organic material which reacted strongly with acid phosphatase. Acid phosphatase activity was never found outside the cell, and in particular, not at the brine-cell interface.This suggests that the defect in bone resorption is caused by cell membrane abnormalities and the lack of ruffle border formation, rather than the inability of the lysosomal enzymes to digest the bone matrix.     

Osteoclast formation from mouse bone marrow cells on micro/nano-scale patterned surfaces

ObjectivesOsteoclasts can sense the surface topography of materials. However, it is difficult to identify the structural factors that affect osteoclast formation and its function. Furthermore, we hypothesized that the type of osteoclast precursor cells also affects osteoclastogenesis in the materials. In this study, we investigated the effects of defined micro/nanoscale patterns on osteoclastogenesis from bone marrow cells (BMCs).MethodsVarious cyclo-olefin polymer (COP) patterns were prepared using nanoimprinting. The effects of shape, size, and height of the patterns, and the wettability of the patterned surfaces on osteoclastogenesis from BMCs were evaluated in vitro.ResultsOsteoclast formation was promoted on pillars (diameter, 1 μm or 500 nm; height, 500 nm). Notably, osteoclastogenesis from BMCs was better promoted on hydrophobic pillars than on hydrophilic pillars. In contrast, decreased osteoclast formation was observed on the nanopillars (diameter, 100 nm; height, 200 nm).ConclusionsWe demonstrated the promotion of osteoclast formation from BMCs on hydrophobic pillars with diameters of 1 μm and 500 nm. Some cellular behaviors in the patterns were dependent on the type of osteoclast precursor cells. The designed patterns are useful for designing the surface of dental implants or bone replacement materials with a controllable balance between osteoblast and osteoclast activities.     

骨疏康对1型糖尿病大鼠体外培养的破骨细胞影响的初步探讨

目的 探讨骨疏康对1型糖尿病大鼠体外培养的破骨细胞影响。方法 用RANKL和M-CSF诱导1型糖尿病大鼠的股骨骨髓进行体外培养生成类破骨细胞样细胞(OLC)。实验分为正常对照组,1型糖尿病组,正常对照+骨疏康组,1型糖尿病+骨疏康组。骨疏康的浓度为20μg/ml。细胞培养7天后,贴壁细胞固定,抗酒石酸盐酸性磷酸酶染色,破骨细胞计数。结果 1型糖尿病大鼠与正常大鼠组的破骨细胞数比较无明显差别(P>0.05);经骨疏康干预后,1型糖尿病大鼠与正常大鼠的破骨细胞数都明显减少(P<0.01)。结论 1型糖尿病早期破骨细胞形成与正常对照组无明显差异。中药骨疏康明显抑制正常大鼠和1型糖尿病大鼠的破骨细胞形成。     

罗格列酮通过抑制RANKL及p-ERK活化抑制类风湿关节炎破骨细胞的分化及功能

目的:探讨罗格列酮(RSG)对类风湿关节炎(RA)成纤维样滑膜细胞(FLS)介导的破骨细胞(Oc)分化及功能的影响及其可能机制。方法:活动期RA患者滑膜体外分离培养FLS,与健康人外周血单核细胞(MNC)共培养,不同浓度RSG(0、5、10和15μmol/L)干预,抗酒石酸酸性磷酸酶(TRAP)染色鉴定Oc并计数;甲苯胺蓝染色和图像分析系统计算骨吸收陷窝面积;Real-time PCR检测共培养体系RANKL和OPG的mRNA表达,Western blot检测RANKL、OPG、p-ERK、p-p38和p-JNK的蛋白含量。结果:与不加RSG组比较,15μmol/L RSG干预后Oc的数量明显减少(P0.01),骨吸收陷窝面积也减少(P0.05);共培养体系RANKL的mRNA及蛋白表达明显降低,OPG的mRNA及蛋白表达明显升高(P0.01);p-ERK的蛋白含量明显降低(P0.05),p-p38及p-JNK的蛋白含量则不受影响。结论:RSG通过抑制RANKL及p-ERK活化影响RA关节微环境中组织细胞与免疫细胞的相互作用,从而抑制Oc分化及骨吸收功能。     

促甲状腺素及其受体与骨质疏松关系的研究进展

骨质疏松症(OP)是严重威胁老年人身心健康的常见疾病。随着人口老年化,老年性骨质疏松症发病率逐年增加。近年来内分泌性骨质疏松日见增多,促甲状腺激素(TSH)及促甲状腺激素受体(TSHR)与骨量减少、骨质疏松的关系倍受关注。成骨细胞和破骨细胞上的促甲状腺激素受体的作用是造成这一作用的关键。而此过程还会受到2型碘化甲腺氨酸脱碘酶、肿瘤坏死因子(TNF)等的影响。同时促甲状腺激素受体存在基因多态性,对其功能存在不同程度的影响,也可能是造成骨质疏松的重要原因。通过对这个领域的深入研究为内分泌性骨质疏松的防治提供依据。     

The effects of high dose of parathyroid hormone on fetal osteoclasts and their precursors in vivo: An ultrastructural-cytochemical study

Background: It is not well known how the immediate precursors of osteoclast develop into osteoclasts in the fetus. This ultrastructural-cytochemical study was designed to clarify the formation process of the osteoclasts and their increased activities in the fetal mouse limb buds after administration of high dose parathyroid hormone (PTH). Methods: Twenty-four or forty-eight hours after the high doses of PTH were injected into amniotic fluid of the pregnant C₃H mice, the femoral limb buds of embryos were dissected out. Tartrate-resistant acid phosphatase (TRAP) reactions were performed while preparing specimens for electron microscopy. Results: Both control and PTH-given preosteoclasts and osteoclasts exhibited TRAP-positivities in dense bodies and vesicles. As effects of PTH, a binucleated preosteoclast of tandem fashion was observed. More osteoclastic hyperactivities were observed in the diaphyseal bone marrow. An osteoclast with a large cytoplasm exhibited two sets of clear zones and ruffled borders. Some osteoclasts demonstrated prominent amoeboid figures, while other osteoclasts developed large cytoplasmic vacuoles, which contained pieces of calcified chondroid bars. Conclusions: Our results revealed the progression of maturation from young preosteoclasts to osteoclasts. An existence of a peculiar binucleated preosteoclasts suggested one of the processes for multinucleation of the osteoclast. Quite remarkable osteoclastic hyperactivities were obviously the effects of high dose PTH. Our results also indicated the endophagocytic ability of the osteoclast. How PTH affected the osteoclasts and their precursors in the diaphyseal bone marrow can be speculated. © 1995 Wiley-Liss, Inc.