抗 RANKL 抗体治疗糖尿病和慢性肾病患者的活动性夏科足神经骨关节病。

Foot & ankle international Pub Date : 2024-10-01 Epub Date: 2024-08-26 DOI:10.1177/10711007241268147

Ashu Rastogi, Raveena Singh, Jayaditya Ghosh, Rajat Gupta

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引用次数: 0

摘要

背景：夏科神经性骨关节病（CNO）的特点是破骨细胞活性增加，而抗骨质吸收剂可以抑制这种活性。慢性肾脏病（CKD）患者不能使用双膦酸盐，但可以考虑使用抗核因子-B配体受体激活剂（抗 RANKL）抗体--地诺单抗。我们研究了地诺单抗治疗活动性 CNO 的方法：方法：在研究期间，我们发现了 446 名患有单侧活动性足 CNO 并伴有 CKD 的糖尿病患者，其中 78 人最终入选。患者在接受 60 毫克地诺单抗（单剂量，皮下注射）治疗的同时，还接受了标准治疗（SoC），即全接触石膏治疗（TCC）（A 组；n = 26）或仅接受标准治疗（SoC）（B 组；n = 52）。患者每 4 周接受一次随访，直至 CNO 缓解，随后每 8 周接受一次随访，直至缓解后 48 周。结果：A 组和 B 组的中位年龄分别为 56.5 (48.8-65) 岁和 57 (48.5-61.2) 岁，P = .57；糖尿病病程分别为 16 (10-25.3) 年和 14.9 (10-19) 年，P = .151；估计肾小球滤过率分别为 44.8 (21.1-65.6) mL/min/1.73 m2 和 45.7 (32.9-55.7) mL/min/1.73 m2，P = .771。患足和对侧足发病时的中位温差分别为 3.4 °C（2.7-6.9）和 3.2 °C（2.2-4.0），P = .119。A组所有患者（100%）均获得缓解，B组为42例（80.8%）（P = .006）（危险比为0.52，95% CI：0.32-0.87；P = .012）。两组的中位缓解时间相似（分别为 15 [11-25] 周和 17.5 [14-31.5] 周，P = .229）。25-羟维生素 D3 >14 ng/mL与缓解显著相关（OR 9.5，95% CI 1.04-87.5，P = .045）：结论：在SoC（TCC）中加入抗RANKL抗体可使更多糖尿病和慢性肾脏病患者的活动性足CNO得到缓解。

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Anti-RANKL Antibody For Active Charcot Foot Neuro-Osteoarthropathy in Patients with Diabetes and Chronic Kidney Disease.

Background: Charcot neuroosteoarthropathy (CNO) is characterized with increased osteoclastic activity that can be curbed with antiresorptive agents. Chronic kidney disease (CKD) precludes bisphosphonates but anti-receptor activator of nuclear factor-B ligand (anti-RANKL) antibody, denosumab, can be contemplated in CKD. We investigated denosumab for active CNO of foot in CKD for CNO remission.

Methods: During the study period, 446 persons of diabetes with unilateral, active CNO of foot and CKD were identified and 78 were finally enrolled. Patients received either 60 mg denosumab (single-dose, subcutaneous) along with standard of care (SoC) as total contact cast (TCC) (group A; n = 26) or SoC (group B; n = 52) only. Patients were followed every 4 weeks until CNO remission and subsequently every 8 weeks until 48 weeks following remission. Remission was defined as temperature difference <2 °C between 2 feet confirmed twice (4 weeks apart) with clinical resolution of signs of inflammation. The primary outcome studied was proportion of patients achieving remission within 48 weeks and the time to remission.

Results: Median age was 56.5 (48.8-65) and 57 (48.5-61.2) years, P = .57; duration of diabetes 16 (10-25.3) and 14.9 (10-19) years, P = .151; and estimated glomerular filtration rate 44.8 (21.1-65.6) and 45.7 (32.9-55.7) mL/min/1.73 m², P = .771, in group A and B, respectively. Median temperature difference at presentation between the affected and opposite foot was 3.4 °C (2.7-6.9) and 3.2 °C (2.2-4.0), P = .119, respectively. All patients achieved remission in group A (100%) compared with 42 (80.8%) in group B (P = .006) (hazard ratio 0.52, 95% CI: 0.32-0.87; P = .012). The median time to remission was similar in the 2 groups (15 [11-25] and 17.5 [14-31.5] weeks, P = .229, respectively). 25-Hydroxyvitamin D₃ >14 ng/mL was significantly associated (OR 9.5, 95% CI 1.04-87.5, P = .045) with remission.

Conclusion: Anti-RANKL antibody added to SoC (TCC) induces remission of active foot CNO in greater proportions of patients with diabetes and CKD.

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Foot & ankle international

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