神经性关节病(Charcot's)破坏的解剖位置与年龄和性别匹配的骨质密度降低之间的关系。

IF 0.5 4区 医学 Q4 ORTHOPEDICS
Craig J Verdin, Georgeanne G Botek, John David Miller, James D Kingsley, Danny Plyler
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引用次数: 0

摘要

背景:有文献记载,糖尿病会对骨矿密度产生全身性影响。最近有文献评估了夏科神经性关节病的发生与局部骨矿密度降低之间的关系;然而,骨质疏松症/骨质疏松与夏科发病之间是否存在关联,甚至与神经性关节病的发病部位之间是否存在关联,目前尚不清楚:我们对 39 名患者进行了回顾性鉴定和评估,这些患者有 41 只脚(4 只双侧)有夏科氏病史,并在 15 年内接受了骨矿密度扫描。对人口统计学、放射学和骨矿密度信息进行了分析:结果:进行骨密度扫描时,患者的平均年龄为(53.44 ± 8.09)岁,确诊为夏科病时的平均年龄为(52.77 ± 8.19)岁。4只脚被认为是桑德斯-弗莱克伯格I型(9.3%),17只脚是桑德斯-弗莱克伯格II型(39.5%),10只脚是桑德斯-弗莱克伯格III型(23.3%),12只脚是桑德斯-弗莱克伯格IV/V型(27.9%)。研究发现,后足区域的神经性关节病变(桑德斯-弗莱克伯格 IV/V 型)与骨质疏松症和髋关节骨质疏松症有关,且发生在骨质疏松症和髋关节骨质疏松症之前,表现为较低的 Z 值(P = 0.05)。夏科神经性关节病与骨健康状况不佳或股骨颈、前臂或腰椎骨矿物质密度下降无关:我们认为,目前的研究结果表明,骨质疏松症/骨质疏松可能与神经性关节病的发病部位有关。有鉴于此,我们得出结论:糖尿病骨骼脆弱症患者可能会受益于治疗潜在的骨质疏松,以预防夏科神经关节病的发生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Association of Anatomical Location of Neuroarthropathic (Charcot's) Destruction with Age-and Sex-Matched Bone Mineral Density Reduction.

Background: It is well documented that diabetes has a systemic impact on bone mineral density. Recent literature has evaluated the relationship between the development of Charcot neuroarthropathy and reduced local bone mineral density; however, it is not clear if there is an association between osteoporosis/osteopenia and Charcot onset, or, even further, location of neuroarthropathic breakdown.

Methods: We retrospectively identified and assessed 39 patients with 41 feet (4 bilateral) with a history of Charcot breakdown who underwent a bone mineral density scan over a 15-year period. Demographic, radiographic, and bone mineral density information was analyzed.

Results: The average patient age at the time of bone mineral density scan was 53.44 ± 8.09 years, and 52.77 ± 8.19 years at the time of Charcot diagnosis. Four feet were considered Sanders-Frykberg I (9.3%), 17 were Sanders-Frykberg II (39.5%), ten were Sanders-Frykberg III (23.3%), and 12 were Sanders-Frkyberg IV/V (27.9%). Neuroarthropathic breakdown of the rearfoot region (Sanders-Frykberg IV/V) was found to be associated and preceded by osteoporosis and osteopenia at the hip as demonstrated by a lower Z-score (P = 0.05). Charcot neuroarthropathy was not associated with poor bone health or loss of bone mineral density at the femoral neck, forearm, or lumbar spine.

Conclusions: We believe that the present findings suggest a possible relationship between osteoporosis/osteopenia and the location of CN development. With these findings in mind, we conclude that patients with diabetic skeletal fragility may benefit from treatment of underlying poor bone mineral density to prevent the onset of Charcot neuroarthropathy.

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来源期刊
CiteScore
1.10
自引率
0.00%
发文量
128
审稿时长
6-12 weeks
期刊介绍: The Journal of the American Podiatric Medical Association, the official journal of the Association, is the oldest and most frequently cited peer-reviewed journal in the profession of foot and ankle medicine. Founded in 1907 and appearing 6 times per year, it publishes research studies, case reports, literature reviews, special communications, clinical correspondence, letters to the editor, book reviews, and various other types of submissions. The Journal is included in major indexing and abstracting services for biomedical literature.
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