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Bone health in pediatric rheumatic disease.

机译:小儿风湿病的骨骼健康。

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PURPOSE OF REVIEW: Children with chronic rheumatic disease have decreased bone mass. In adults, lowered bone mineral density is associated with increased fracture risk. This morbidity is undetermined in pediatric rheumatic disease as osteoporosis has not been well-defined in children. This review compares methods for determining bone mass in children, examines insights into molecular mechanisms of bone metabolism, and discusses the prevention and treatment of decreased bone mass in children. RECENT FINDINGS: Peak bone mass, attained during adolescence and early adulthood, is critical in determining fracture risk. Studies of children with chronic rheumatic disease demonstrate decreased bone mineral density, and potentially lowered peak bone mass. Dual energy x-ray absorptiometry is the most commonly used technique for monitoring bone mineral density and should be interpreted utilizing age-appropriate Z-scores. Recent studies suggest quantitative ultrasound may be as reliable as dual energy x-ray absorptiometry and lacks radiation exposure. The molecular mechanisms by which inflammation alters bone mineral density involve receptor activator of nuclear factor kappaB ligand (RANKL)/osteoprotegerin, tumor necrosis factor-alpha, and interleukin-1. Limited data on the use of bisphosphonates and calcitonin in children suggest they are safe and effective, but should be used cautiously. SUMMARY: Children with chronic rheumatic disease should have bone mass monitored by dual energy x-ray absorptiometry Z-scores. Targeting the RANKL/osteoprotegerin pathway may lead to therapies that improve bone health in this population. More studies on the role of bisphosphonates and calcitonin must be pursued to establish guidelines for use in pediatric patients with chronic rheumatic disease. For now, supplemental calcium and vitamin D should be implemented in these children.
机译:审查目的:患有慢性风湿病的儿童的骨量减少。在成年人中,骨矿物质密度降低与骨折风险增加相关。小儿风湿病的发病率尚未确定,因为儿童的骨质疏松症尚未明确定义。这篇综述比较了确定儿童骨量的方法,研究了对骨代谢分子机制的见解,并讨论了预防和治疗儿童骨量减少的方法。最近的发现:在青春期和成年早期达到的峰值骨量对于确定骨折风险至关重要。对患有慢性风湿病的儿童的研究表明,骨矿物质密度降低,峰值骨量可能降低。双能X射线吸收法是监测骨矿物质密度最常用的技术,应使用适合年龄的Z值进行解释。最近的研究表明,定量超声可能与双能X射线吸收法一样可靠,并且缺乏辐射暴露。炎症改变骨矿物质密度的分子机制涉及核因子κB配体(RANKL)/骨保护素,肿瘤坏死因子-α和白介素-1的受体激活剂。关于儿童使用双膦酸盐和降钙素的有限数据表明,它们是安全有效的,但应谨慎使用。摘要:患有慢性风湿病的儿童应通过双能X线骨密度仪Z值监测骨量。靶向RANKL /骨保护素途径可能导致改善该人群骨骼健康的疗法。必须对双膦酸盐和降钙素的作用进行更多研究,以建立在患有慢性风湿病的小儿患者中使用的指南。目前,这些儿童应补充钙和维生素D。

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