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Evaluation of Cross-Sectional and Longitudinal Changes in Volumetric Bone Mineral Density in Postmenopausal Women Using Single- versus Dual-Energy Quantitative Computed Tomography

机译:使用单能量和双能量定量计算机断层扫描技术评估绝经后妇女的体积骨矿物质密度的横截面和纵向变化

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摘要

Central quantitative computed tomography (QCT) is increasingly used in clinical trials and practice to assess bone mass or strength and to evaluate longitudinal changes in response to drug treatment. Current studies utilize single-energy (SE) QCT scans, which may be confounded both by the amount of bone marrow fat at baseline and changes in marrow fat over time. However, the extent to which marrow fat changes either underestimate volumetric BMD (vBMD) measurements at baseline or under-/overestimate longitudinal changes in vivo in humans remains unclear. To address this issue, 197 early postmenopausal women [median age (IQR) 56.7 (54.4–58.7) years] underwent spine and hip QCT scans at baseline and 3 years using a 128-slice dual-source dual-energy (DE) scanner. The scans were analyzed as either SE scans (100 kVp) or DE scans (100 kVp and 140 kVp), with the latter accounting for bone marrow fat. At baseline, vertebral trabecular vBMD was (median) 17.6% lower (P < 0.001) while femur neck (FN) cortical vBMD was only 3.2% lower (P < 0.001) when assessed by SE vs DE scanning. SE scanning overestimated the 3 year rate of bone loss for trabecular bone at the spine by 24.2% (P < 0.001 vs DE rates of loss) but only by 8.8% for changes in FN cortical vBMD (P < 0.001 vs DE rates of loss). The deviation between SE and DE rates of bone loss in trabecular vBMD became progressively greater as the rate of bone loss increased. These findings demonstrate that SE QCT scans underestimate trabecular vBMD and substantially overestimate rates of age-related bone loss due to ongoing conversion of red to yellow marrow. Further, the greater the rate of bone loss, the greater the overestimation of bone loss by SE scans. Although our findings are based on normal aging, recent evidence from animal studies demonstrates that the skeletal anabolic drugs teriparatide and romozosumab may markedly reduce marrow fat, perhaps accounting for the disproportionate increases in trabecular vBMD by SE QCT as compared to dual-energy x-ray absorptiometry with these agents. As such, future studies using recently available DE scanning technology that has satisfactory precision and radiation exposure are needed to evaluate changes in trabecular vBMD independent of changes in marrow fat with aging and drugs that may alter marrow fat composition.
机译:中央定量计算机断层扫描(QCT)在临床试验和实践中越来越多地用于评估骨量或强度,并评估响应药物治疗的纵向变化。当前的研究利用单能(CT)QCT扫描,这可能与基线时的骨髓脂肪量和骨髓脂肪随时间的变化而混淆。然而,尚不清楚基线时骨髓脂肪的变化程度低估了体内BMD(vBMD)的测量值或体内纵向变化的低/高估了。为了解决这个问题,使用128层双源双能(DE)扫描仪对197名绝经后早期妇女[中位年龄(IQR)56.7(54.4-58.7)岁]进行了基线和3年的脊柱和髋部QCT扫描。扫描以SE扫描(100 kVp)或DE扫描(100 kVp和140 kVp)进行分析,后者考虑了骨髓脂肪。在基线时,通过SE与DE扫描评估,椎骨小梁vBMD(中位数)降低了17.6%(P <0.001),而股骨颈(FN)皮质vBMD仅降低了3.2%(P <0.001)。 SE扫描高估了脊柱小梁骨的3年骨丢失率24.2%(P <0.001 vs DE丢失率),而FN皮质vBMD的变化仅高出8.8%(P <0.001 vs DE丢失率) 。随着骨丢失率的增加,小梁vBMD中骨丢失率的SE和DE之间的偏差逐渐增大。这些发现表明,SE QCT扫描低估了小梁vBMD,并由于高估了由红骨髓转化为黄骨髓而大大高估了与年龄相关的骨丢失率。此外,骨丢失率越高,SE扫描对骨丢失的高估就越大。尽管我们的发现基于正常的衰老,但动物研究的最新证据表明,骨骼合成代谢药物特立帕肽和romozosumab可能显着减少骨髓脂肪,这可能是SE QCT与双能X射线相比导致小梁vBMD不成比例增加的原因。用这些试剂进行吸光光度法。因此,需要使用具有令人满意的精度和放射线暴露能力的最近可用的DE扫描技术进行未来研究,以评估小梁vBMD的变化,而与老化和可能改变骨髓脂肪成分的药物的变化无关。

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