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抗惊厥治疗及骨化三醇(1,25 - 二羟维生素D3)治疗引起的骨病

Bone disease induced by anticonvulsant therapy and treatment with calcitriol (1,25-dihydroxyvitamin D3).

作者信息

Hunt P A, Wu-Chen M L, Handal N J, Chang C T, Gomez M, Howell T R, Hartenberg M A, Chan J C

出版信息

Am J Dis Child. 1986 Jul;140(7):715-8. doi: 10.1001/archpedi.1986.02140210113038.

Abstract

To evaluate the effects of calcitriol (1,25-dihydroxyvitamin D3) therapy for the bone disease induced by long-term treatment with anticonvulsants, we reviewed the medical records of 330 institutionalized oligophrenic children and young adults under 26 years of age to identify the 144 children who required anticonvulsant therapy. Of this latter group, 52 children were found to have serum alkaline phosphatase levels elevated more than 2 SDs above normal and were enrolled into this prospective three-year study. To achieve rapid resolution of the bone disease, we elected to use calcitriol at 0.25 to 0.75 micrograms/d. After 1195 patient-months of treatment, our data suggest that the dystrophic process was reversed in 42.3% of the cases, as judged by decreases in serum alkaline phosphatase levels at six months, 65.4% of cases at 12 months, and 83.3% of cases at 13 to 18 months. By 30 months of follow-up, all patients showed significant lowering of serum alkaline phosphatase levels. The improvements were slow and gradual. Twenty-six patients in the treatment series of 52 patients initially showed signs of rickets or osteomalacia on roentgenograms of the wrists. Of these 26 patients, 12 (46%) showed improvement on roentgenograms within 24 months of the beginning of treatment. With reference to complications, hypercalcemia (calcium level, greater than 11 mg/dL [2.74 mmol/L]) was encountered at the rate of one episode per 44 patient-months of treatment. Our results strongly suggest that calcitriol is effective in healing anticonvulsant-related osteomalacia among children and youths, with a low incidence of complications.

摘要

为评估骨化三醇(1,25 - 二羟维生素D3)治疗长期使用抗惊厥药所致骨病的效果,我们查阅了330名26岁以下机构收容的智力发育迟缓儿童和青年的病历,以确定其中144名需要抗惊厥治疗的儿童。在这后一组中,发现52名儿童血清碱性磷酸酶水平高于正常均值2个标准差以上,这些儿童被纳入这项为期三年的前瞻性研究。为使骨病迅速缓解,我们选择使用剂量为0.25至0.75微克/天的骨化三醇。经过1195个患者月的治疗,我们的数据表明,根据血清碱性磷酸酶水平在6个月时下降情况判断,42.3%的病例营养不良过程得到逆转;在12个月时,65.4%的病例得到逆转;在13至18个月时,83.3%的病例得到逆转。到随访30个月时,所有患者血清碱性磷酸酶水平均显著降低。改善过程缓慢且渐进。在52例治疗组患者中,26例患者最初手腕部X线片显示有佝偻病或骨软化症迹象。在这26例患者中,12例(46%)在治疗开始后24个月内X线片显示有改善。关于并发症,高钙血症(血钙水平大于11毫克/分升[2.74毫摩尔/升])的发生率为每44个患者月出现1次。我们的结果强烈表明,骨化三醇对治愈儿童和青少年抗惊厥药相关骨软化症有效,且并发症发生率低。

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