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在去卵巢小鼠甲状旁腺激素治疗期间对骨矿物质密度进行的重复体内测定。

Repeated in vivo determinations of bone mineral density during parathyroid hormone treatment in ovariectomized mice.

作者信息

Andersson N, Lindberg M K, Ohlsson C, Andersson K, Ryberg B

机构信息

AstraZeneca R&D, Mölndal, Sweden.

出版信息

J Endocrinol. 2001 Sep;170(3):529-37. doi: 10.1677/joe.0.1700529.

Abstract

The recent development of different genetically modified mice with potentially interesting bone phenotypes has increased the demand for effective non-invasive methods to evaluate effects on bone of mice during growth and development, and for drug evaluation. In the present study, the skeleton was analyzed by repeated in vivo scans using dual energy X-ray absorptiometry (DXA) and peripheral quantitative computed tomography (pQCT). Ovariectomized (ovx) mice treated with parathyroid hormone (PTH) were used as an animal model to evaluate these two techniques at different times after the onset of treatment. Female mice (6 weeks of age) were allocated randomly to four groups: (1) sham-operated+vehicle; (2) ovx+vehicle; (3) sham-operated+PTH(1-84) 150 microg/kg per day; (4) ovx+PTH. Six weeks after ovariectomy the drug treatment began and was continued for 8 weeks. The total body bone mineral content (BMC) and total body areal bone mineral density (BMD) were measured by DXA. Ovariectomy reduced total body BMC and total body areal BMD by 6.2+/-1.7% and 2.6+/-0.9% respectively. No effect of PTH on total body BMC was seen during the treatment period. The trabecular volumetric BMD was measured by pQCT. Ovariectomy reduced the trabecular volumetric BMD by 52+/-6.7%. The pQCT technique detected a clear effect on trabecular volumetric BMD after 2 weeks of PTH treatment (ovx 94+/-29% and sham-operated 46+/-10% more than vehicle-treated). The cortical bone was measured in a mid-diaphyseal pQCT scan of the tibia. Ovariectomy reduced the cortical BMC by 9+/-2%. PTH treatment for 8 weeks increased cortical BMC in ovx mice. In conclusion, the pQCT technique is more sensitive than the DXA technique in the detection of bone loss after ovariectomy and increased bone mass after PTH treatment in mice. Notably, the pQCT, but not the DXA, technique detected a dramatic effect as early as after 2 weeks of PTH treatment. Dynamic pQCT measurements will be useful for monitoring skeletal changes during growth and development, and for drug evaluation in mice.

摘要

近年来,不同的具有潜在有趣骨表型的转基因小鼠不断出现,这使得人们对于在小鼠生长发育过程中评估对骨骼的影响以及进行药物评估的有效非侵入性方法的需求日益增加。在本研究中,通过使用双能X线吸收法(DXA)和外周定量计算机断层扫描(pQCT)进行反复的体内扫描来分析骨骼。将接受甲状旁腺激素(PTH)治疗的去卵巢(ovx)小鼠作为动物模型,在治疗开始后的不同时间评估这两种技术。将6周龄的雌性小鼠随机分为四组:(1)假手术+赋形剂;(2)去卵巢+赋形剂;(3)假手术+PTH(1-84)150微克/千克/天;(4)去卵巢+PTH。去卵巢6周后开始药物治疗,并持续8周。通过DXA测量全身骨矿物质含量(BMC)和全身面积骨矿物质密度(BMD)。去卵巢使全身BMC和全身面积BMD分别降低了6.2±1.7%和2.6±0.9%。在治疗期间未观察到PTH对全身BMC有影响。通过pQCT测量小梁体积骨密度。去卵巢使小梁体积骨密度降低了52±6.7%。pQCT技术在PTH治疗2周后检测到对小梁体积骨密度有明显影响(去卵巢组比赋形剂治疗组高94±29%,假手术组比赋形剂治疗组高46±10%)。在胫骨骨干中段的pQCT扫描中测量皮质骨。去卵巢使皮质BMC降低了9±2%。对去卵巢小鼠进行8周的PTH治疗可增加皮质BMC。总之,在检测小鼠去卵巢后的骨质流失以及PTH治疗后的骨量增加方面,pQCT技术比DXA技术更敏感。值得注意的是,pQCT技术早在PTH治疗2周后就检测到了显著效果,而DXA技术则未检测到。动态pQCT测量对于监测小鼠生长发育过程中的骨骼变化以及进行药物评估将是有用的。

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