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首页> 外文期刊>Journal of the American College of Nutrition >Bone metabolic abnormalities associated with well-controlled type 1 diabetes (IDDM) in young adult women: a disease complication often ignored or neglected.
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Bone metabolic abnormalities associated with well-controlled type 1 diabetes (IDDM) in young adult women: a disease complication often ignored or neglected.

机译:与年轻成年女性控制良好的1型糖尿病(IDDM)相关的骨代谢异常:这种疾病并发症通常被忽略或忽视。

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摘要

OBJECTIVES: This investigation on a homogenous cohort of young adult Caucasian type 1 diabetic (IDDM) patients (1) aimed at studying the occurrence of low bone mineral density (BMD) at an early stage prior to menopause (i.e., during the first decade after peak bone mass) and (2) elucidating the possible mechanisms underlying IDDM-induced bone complication. METHODS: Twenty-seven female patients with insulin-treated and well-controlled diabetes, without renal complications, and 32 well-matched healthy controls, aged between 30 and 40 years and fulfilling rigorous inclusion criteria to minimize bone-confounding factors, were enrolled. Areal BMD was evaluated by dual energy X-ray absorptiometry at axial (lumbar spine) and appendicular (femur) sites, using diagnostic WHO reference (T-scores). Osteoblast functions, bone metabolism, related key minerals, and 2 osteoclast-stimulating calciotropic hormones regulating their serum levels were assessed biochemically. RESULTS: The number of cases with low BMD (T-score below -1.1 SD) was almost 2-fold greater (p < 0.01) in the IDDM group. BMD was significantly lower in this group for 3 lumbar sites (p < 0.01) and femur Ward's triangle (p < 0.05). Bone formation was reduced, as evidenced by the suppressions of osteocalcin (OC; p < 0.01) and IGF-I (p < 0.001). However, bone alkaline phosphatase (bALP) was induced (p < 0.01), in contrast to what is usually observed in cases of reduced bone formation. Correlated total ALP activity was also significantly increased. There was no change in the specific marker of bone resorption (urinary deoxypyridinoline). Serum calcium was significantly elevated, particularly after adjustment for albumin (p < 0.001), despite lower 1,25(OH)(2)D(3) (p < 0.001) and no elevation of PTH. All significant bone-related biochemical changes were significantly correlated with glycosylated hemoglobin, a clinical indicator of long-term glycemic control, indicating a direct effect of the disease. CONCLUSIONS: Bone loss in the IDDM group results from a decrease in bone formation rather than an increase of bone resorption. The induction of bALP is indicative of impaired osteoblast differentiation and maturation, which delayed (down-regulated) later stages of matrix mineralization, as evidenced by lower OC and BMD.
机译:目的:本研究针对年轻的白种人高加索1型糖尿病(IDDM)成人患者的同质队列(1),旨在研究绝经前早期(即,之后的第一个十年)低骨矿物质密度(BMD)的发生峰值骨量)和(2)阐明IDDM引起的骨并发症的可能机制。方法:招募了27名女性患者,他们接受了胰岛素治疗且控制良好的糖尿病,无肾脏并发症,另外32名健康匹配的健康对照者,年龄在30至40岁之间,并且符合严格的入选标准,以最小化骨混杂因素。使用诊断性WHO参考(T评分),通过双能X线骨密度仪在轴向(腰椎)和阑尾(股骨)部位评估骨密度。生化评估成骨细胞功能,骨代谢,相关关键矿物质和2种刺激破骨细胞的促钙激素调节其血清水平。结果:IDDM组中低BMD(T分数低于-1.1 SD)的病例数几乎增加了2倍(p <0.01)。在该组中,对于3个腰部部位(p <0.01)和股骨沃德三角形(p <0.05),BMD显着降低。骨钙蛋白(OC; p <0.01)和IGF-I(p <0.001)的抑制证明了骨形成的减少。然而,与减少骨形成的情况通常观察到的相反,诱导了骨碱性磷酸酶(bALP)(p <0.01)。相关的总ALP活性也显着增加。骨吸收的特异性标志物(尿脱氧吡啶并啉)没有变化。血清钙显着升高,特别是在调整白蛋白后(p <0.001),尽管1,25(OH)(2)D(3)较低(p <0.001)并且PTH没有升高。所有与骨骼相关的重要生化变化均与糖基化血红蛋白显着相关,糖化血红蛋白是长期血糖控制的临床指标,表明该疾病的直接作用。结论:IDDM组的骨丢失是由于骨形成减少而不是骨吸收增加引起的。 bALP的诱导表明成骨细胞的分化和成熟受损,这延迟(下调了)基质矿化的后期阶段,如较低的OC和BMD所证明。

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