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Children with nephrotic syndrome have greater bone area but similar volumetric bone mineral density to healthy controls

机译:患有肾病综合征的儿童的骨骼面积更大,但与健康对照组的骨骼矿物质密度相似

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Background: Glucocorticoid use has been associated with an increased fracture risk and reduced bone mineral density (BMD), particularly in the trabecular compartment. However the contribution of the underlying inflammatory disease process to these outcomes is poorly understood. Childhood nephrotic syndrome (NS) typically follows a relapsing-remitting course often requiring recurrent courses of glucocorticoids, but with low systemic inflammation during remission. NS therefore represents a useful clinical model to investigate the effects of glucocorticoids on BMD and bone geometry in childhood. Methods: Children with NS were compared to age and sex matched healthy controls. Body composition and areal BMD (whole body, lumbar spine and hip) were assessed by DXA. Peripheral quantitative computed tomography (pQCT) scans were obtained at metaphyseal (4%) and diaphyseal (66%) sites of the tibia to determine volumetric BMD and bone cross-sectional geometry. Lifetime cumulative glucocorticoid exposure was calculated from medical records. Results: 29 children with NS (55% male, age 10.7±3.1years) were compared to 29 healthy controls (55% male, age 11.0±3.0years). The children with NS were of similar height SDS to controls (p=0.28), but were heavier (0.65±1.28SDS vs -0.04±0.89SDS, p=0.022) and had greater body fat percentage SDS (0.31±1.01 vs -0.52±1.10, p=0.008). Tibial trabecular and cortical vBMD were similar between the two groups but bone cross-sectional area (CSA) was significantly greater in children with NS at both the metaphysis (954±234mm2 vs 817±197mm2, p=0.002) and diaphysis (534.9±162.7mm2 vs 463.2±155.5mm2, p=0.014). Endosteal and periosteal circumferences were greater in children with NS than controls (both p0.01), resulting in reduced cortical thickness (2.4±0.7mm vs 2.8±0.7mm, p=0.018), but similar cortical CSA (p=0.22). The differences in cortical geometry were not statistically significant when weight was included as a confounding factor. There were no associations between cumulative steroid exposure, duration of NS or number of relapses and any bone parameter. Conclusions: Tibial bone CSA is increased in children with NS. We speculate that this is a compensatory response to increased body weight. Defects in trabecular BMD were not identified in this cohort of children with NS.
机译:背景:糖皮质激素的使用与骨折风险增加和骨矿物质密度(BMD)降低有关,尤其是在小梁腔内。然而,人们对潜在的炎性疾病过程对这些结果的贡献知之甚少。儿童肾病综合征(NS)通常遵循复发缓解型病程,通常需要糖皮质激素的复发病程,但缓解期的全身炎症较低。因此,NS代表了一种有用的临床模型,可用于研究糖皮质激素对儿童BMD和骨骼几何形状的影响。方法:将NS患儿与年龄和性别相匹配的健康对照者进行比较。通过DXA评估身体成分和面积BMD(全身,腰椎和臀部)。在胫骨干meta端(4%)和干端(66%)部位进行了外周定量计算机断层扫描(pQCT)扫描,以确定体积BMD和骨骼横截面几何形状。根据病历计算终生累积糖皮质激素暴露。结果:将29例NS患儿(男性55%,年龄10.7±3.1岁)与29例健康对照组(55%男性,11.0±3.0岁)进行了比较。 NS患儿的SDS高度与对照组相似(p = 0.28),但较重(0.65±1.28SDS vs -0.04±0.89SDS,p = 0.022),体脂百分比SDS较高(0.31±1.01 vs -0.52) ±1.10,p = 0.008)。两组的胫骨小梁和皮质vBMD相似,但是NS患儿的干physi端(954±234mm2 vs 817±197mm2,p = 0.002)和骨干(534.9±162.7)的骨截面积(CSA)明显更大。平方毫米vs 463.2±155.5平方毫米,p = 0.014)。 NS患儿的骨膜周和骨膜周长比对照组大(均p <0.01),导致皮质厚度减少(2.4±0.7mm vs 2.8±0.7mm,p = 0.018),但皮质CSA相似(p = 0.22)。当将体重作为混杂因素时,皮层几何形状的差异没有统计学意义。累积类固醇暴露,NS持续时间或复发次数与任何骨骼参数之间没有关联。结论:NS患儿胫骨CSA升高。我们推测这是对体重增加的补偿性反应。在这个NS患儿队列中未发现小梁BMD的缺陷。

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