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干扰素α和帕米膦酸治疗肥大细胞病继发骨折所致骨质疏松症。

Interferon alpha and pamidronate in osteoporosis with fracture secondary to mastocytosis.

机构信息

Department of Rheumatology, CHU Purpan, Toulouse, France.

出版信息

Am J Med. 2011 Aug;124(8):776-8. doi: 10.1016/j.amjmed.2011.02.038.

Abstract

BACKGROUND

The mechanism of osteoporosis with fracture secondary to mastocytosis is little known, and its treatment is poorly codified.

METHODS

Ten patients with a mean age of 52.5 years with systemic mastocytosis and osteoporotic fractures were treated with interferon alpha 1.5 million U 3 times per week, combined with monthly pamidronate infusions (1 mg/kg) for 2 years, followed by pamidronate infusions every 3 months.

RESULTS

Before treatment, the mean number of vertebral fractures was 3.5, spinal T-score was -3±1, hip T-score was -1.9±0.7, serum C-terminal telopeptide was 357±258 pg/mL (N=80-800), bone alkaline phosphatase was 20±3.2 IU (N=8-25), and tryptase was 49±36 μg/mL (N<10). Interferon alpha was discontinued in 2 patients because of poor tolerance. Mean follow-up was 60 months. No patient developed a fracture under treatment. In the 8 patients treated with interferon alpha and pamidronate, the mean annual increase in spinal bone mineral density was 12.6%±5.6% and 1.93% in hip bone mineral density. Serum C-terminal telopeptide decreased by 66%, bone alkaline phosphatase decreased by 25%, and tryptase decreased by 34%. In the 2 patients treated with pamidronate alone, mean annual bone mineral density increase was 2.4%±0.1% at the spine and 0%±01% at the hip.

CONCLUSION

Osteoporosis secondary to mastocytosis mainly affects trabecular bone, and markers of bone remodeling are normal. Combined treatment with low doses of interferon and pamidronate markedly increased bone density.

摘要

背景

伴有骨折的肥大细胞增多症性骨质疏松的发病机制尚不清楚,其治疗也尚未规范。

方法

10 名平均年龄为 52.5 岁的系统性肥大细胞增多症合并骨质疏松性骨折患者接受每周 3 次、150 万 U 的干扰素α治疗,联合每月帕米膦酸 1mg/kg 输注 2 年,随后每 3 个月输注帕米膦酸。

结果

治疗前,平均椎体骨折数为 3.5 个,脊柱 T 评分-3±1,髋部 T 评分-1.9±0.7,血清 C 端肽 357±258pg/ml(80-800),骨碱性磷酸酶 20±3.2IU(8-25),类胰蛋白酶 49±36μg/ml(<10)。2 例患者因不耐受而停用干扰素α。平均随访时间为 60 个月。治疗期间无患者发生骨折。在接受干扰素α和帕米膦酸治疗的 8 例患者中,脊柱骨密度的年平均增长率为 12.6%±5.6%,髋部骨密度的年平均增长率为 1.93%。血清 C 端肽下降 66%,骨碱性磷酸酶下降 25%,类胰蛋白酶下降 34%。在单独接受帕米膦酸治疗的 2 例患者中,脊柱和髋部的年平均骨密度增长率分别为 2.4%±0.1%和 0%±01%。

结论

肥大细胞增多症相关性骨质疏松主要影响松质骨,骨重塑标志物正常。低剂量干扰素与帕米膦酸联合治疗可显著增加骨密度。

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