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糖尿病性活跃性夏科氏神经关节病中炎症和破骨细胞生成的差异缓解对足部长期结局的影响。

Long-term foot outcomes following differential abatement of inflammation and osteoclastogenesis for active Charcot neuroarthropathy in diabetes mellitus.

机构信息

Department of Endocrinology, PGIMER, Chandigarh, India.

Tameside and Glossop Integrated Care NHS Foundation Trust, Ashton on Lyne, United Kingdom.

出版信息

PLoS One. 2021 Nov 8;16(11):e0259224. doi: 10.1371/journal.pone.0259224. eCollection 2021.

Abstract

AIMS

Inflammatory osteolysis is sine-qua-non of active Charcot neuroarthropathy (CN) causing decreased foot bone mineral density (BMD) and fractures. We aimed to explore the effect of anti-inflammatory or anti-resorptive agents for effect on foot bone mineral content (BMC) and consequent long-term outcomes of foot deformities, fractures and amputation.

METHODS

Forty-three patients with active CN (temperature difference >2°C from normal foot) were evaluated. Patients were off-loaded with total contact cast and randomized to receive either methylprednisolone (1gm) (group A), zoledronate (5mg) (group B) or placebo (100ml normal saline) (group C) once monthly infusion for three consecutive months. Change in foot BMC was assessed at 6 months or at remission and followed subsequently up to 4 years for the incidence of new-onset fracture, deformities, or CN recurrence.

RESULTS

Thirty-six participants (24 male, 12 female) were randomized (11 in group A, 12 group B, 13 group C). The mean age was 57.7± 9.9 years, duration of diabetes 12.3± 5.8 years and symptom duration 6.5± 2.8 weeks. BMC increased by 36% with zoledronate (p = 0.02) but reduced by 13% with methylprednisolone (p = 0.03) and 9% (p = 0.09) with placebo at remission. There were no incident foot fractures, however, two patients sustained ulcers, and 3 had new-onset or worsening deformities and none required amputation during 3.36 ± 0.89 years of follow-up.

CONCLUSION

Bisphosphonate for active CN is associated with an increase in foot bone mineral content as compared to decrease with steroids or total contact cast but long-term outcomes of foot deformities, ulceration and amputation are similar.

TRIAL REGISTRATION

ClinicalTrials.gov: NCT03289338.

摘要

目的

炎症性溶骨性骨破坏是活跃性夏科氏神经关节病(CN)的必要条件,会导致足部骨矿物质密度(BMD)降低和骨折。我们旨在探讨抗炎或抗吸收药物对足部骨矿物质含量(BMC)的影响,以及对足部畸形、骨折和截肢的长期后果。

方法

评估了 43 例活动性 CN(与正常足部的温差>2°C)患者。患者使用全接触石膏进行减压,并随机分为接受甲泼尼龙(1gm)(A 组)、唑来膦酸(5mg)(B 组)或安慰剂(100ml 生理盐水)(C 组)每月一次连续三个月输注。在 6 个月或缓解时评估足部 BMC 的变化,并随后随访 4 年,以评估新发骨折、畸形或 CN 复发的发生率。

结果

36 名参与者(24 名男性,12 名女性)被随机分组(A 组 11 名,B 组 12 名,C 组 13 名)。平均年龄为 57.7±9.9 岁,糖尿病病程为 12.3±5.8 年,症状持续时间为 6.5±2.8 周。唑来膦酸使 BMC 增加 36%(p=0.02),而甲泼尼龙使 BMC 减少 13%(p=0.03),安慰剂使 BMC 减少 9%(p=0.09),在缓解时。虽然没有新发足部骨折,但有 2 例患者发生溃疡,3 例患者出现新的或加重的畸形,无 1 例患者在 3.36±0.89 年的随访中需要截肢。

结论

与皮质类固醇或全接触石膏相比,双膦酸盐治疗活动性 CN 可使足部骨矿物质含量增加,但足部畸形、溃疡和截肢的长期结果相似。

试验注册

ClinicalTrials.gov:NCT03289338。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a27/8575293/08469744c1b4/pone.0259224.g001.jpg

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