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Predictors of bone density in ambulatory patients on antiepileptic drugs.

机译:使用抗癫痫药物的非卧床患者的骨密度预测指标。

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BACKGROUND AND AIM: Antiepileptic drugs are associated with bone loss and fractures. Data in children is scarce and the impact of new therapies and of low vitamin D is not clear. This study assessed predictors of bone mineral density (BMD) in 225 ambulatory patients with epilepsy. METHODS: BMD and detailed clinical information were obtained from 137 adults mean age of 31 years, on therapy for a mean of 11.7 years, and 88 children mean age of 13 years, on therapy for an average of 4.7 years. RESULTS: Hypovitaminosis D was common in epileptic patients. BMD was reduced in adults but not children with epilepsy, by 0.3-0.6 SD depending on the skeletal site measured, compared to controls. Duration of treatment, but not vitamin D levels, was negatively correlated with BMD at the hip in adults. Bone density was reduced with the use of both enzyme and non-enzyme-inducing drugs, with both mono- and polytherapy, and was most severely reduced at the spine and hip with the use of enzyme-inducing drugs. In the multivariate analyses, polytherapy in children and duration of therapy and enzyme-inducing drugs in adults were independent predictors of BMD. CONCLUSION: Antiepileptic drug therapy is associated with low bone density at clinically relevant skeletal sites, projecting into a possible doubling of fracture risk. Age, therapy duration, polypharmacy and the use of enzyme-inducing drugs were risk factors. Newer drugs may be associated with deleterious effects on bone. Skeletal monitoring with varying intervals, depending on the individual risk profile, is indicated.
机译:背景与目的:抗癫痫药与骨质流失和骨折有关。儿童的数据稀少,新疗法和低维生素D的影响尚不清楚。这项研究评估了225名非卧床癫痫患者的骨矿物质密度(BMD)的预测因子。方法:BMD和详细的临床信息来自137位成年人的平均年龄,平均接受治疗11.7岁,88位儿童平均年龄的13岁,接受平均治疗4.7岁。结果:维生素D缺乏症在癫痫患者中很常见。与对照相比,根据测量的骨骼部位,成人而不是癫痫儿童的BMD降低了0.3-0.6 SD。成人的髋关节BMD与治疗时间长短(而不是维生素D水平)负相关。单一疗法和多重疗法同时使用酶和非酶诱导药物可降低骨密度,而使用酶诱导药物可最严重地降低脊柱和臀部的骨密度。在多变量分析中,儿童的多联疗法以及成人的治疗时间和酶诱导药物是BMD的独立预测因子。结论:抗癫痫药物治疗与临床相关骨骼部位的骨密度低有关,预计可能使骨折风险增加一倍。年龄,治疗时间,多药房和使用酶诱导药物是危险因素。新型药物可能与对骨骼的有害作用有关。指示了根据各个风险状况以不同间隔进行的骨骼监视。

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