The role of neurohumoral factors in the persistence of aseptic bone inflammation in patients with diabetic neuroosteoarthropathy

IF 0.7 Q4 ENDOCRINOLOGY & METABOLISM Diabetes Mellitus Pub Date : 2022-11-30 DOI:10.14341/dm12961
E. L. Zaitseva, M. M. Kalandiya, A. Y. Tokmakova, N. Malysheva, L. Nikankina, G. Galstyan
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Abstract

BACKGROUND: Diabetic neuroosteoarthropathy (DNOAP, Charcot foot) is a relatively rare complication of diabetes mellitus (DM), which can lead not only to impaired support function of the lower limb in such patients, but also to high amputation. DNOAP is characterized by persistent aseptic inflammation of the bone structures of the foot, which creates significant ­difficulties in planning therapeutic measures. In the medical literature, there are data demonstrating the role of individual ­cytokines and neurohumoral factors in the prolongation of the inflammatory process in diabetes, however, there are currently very few studies that determine reliable markers of aseptic inflammation in DNOAP.AIM: To study the effect of neurohumoral factors and advanced glycation end products on the activity of aseptic inflammation in the bone structures of the foot in patients with type 2 diabetes mellitus (DM2) and diabetic neuroosteoarthropathy.MATERIALS AND METHODS. The study included 88 patients with type 2 diabetes (45 men, 43 women). Group 1 consisted of patients with DM2 and inactive DNOAP (n= 43), group 2 (n= 45) consisted of patients with DM2 and distal diabetic neuropathy without osteoarticular pathology. The diagnosis of diabetic neuropathy was based on the analysis of the clinical picture and indicators of peripheral sensitivity. Diagnosis of DNOAP and determination of its stage was based on clinical data, the results of infrared thermometry and radiology tests of the foot bones. General clinical assessment was used, radiology tests (X-ray, MRI), evaluation of CRP, calprotectin, copeptin, glutathione peroxidase 1 (GP1).RESULTS. According to the results of examination and palpation of the feet, as well as the analysis of the temperature gradient of the skin of the affected and contralateral limb (infrared thermometry), DNOAP was detected and the stage of this complication was determined. The diagnosis of the chronic stage of DNOAP was confirmed by the results of MRI and the clinical picture (no difference in skin temperature on the symmetrical areas of the feet). According to the results of laboratory analysis, a statistically significant difference in copeptin values was revealed — in group 1 — 0.232 µg/ml [0.147; 0.342], in group 2 — 0.115 µg/ml [0.065; 0.203] (p>0.05) and CRP — in group 1 — 7.113 mg/l [2.453; 16.505], in group 2 — 2.187 mg/l [1.131; 5.567] (p>0.05), leukocyte levels in the groups did not differ significantly: group 1 — 7.86 [6.40; 9.00]*10^9, group 2 — 7.00 [6.00; 8.15] (p>0.05). There was a trend towards an increase in the level of calprotectin and glutathione peroxidase-1 in the DNOAP group, however, the differences were not significant. calprotectin — in group 1 — 1.948 [1.229; 2.969], in group 2 — 1.692 [1.16; 2.514] μg/ml and glutathione peroxidase-1 in group 1 — 24.72 [20.1; 31.82], in group 2 — 22.98 [18.94; 31.2] ng/ml.CONCLUSION. In the study, statistically significant differences were obtained in the levels of copeptin and C-reactive protein: in patients with DNOAP, their values were significantly higher, which indicates the persistence of the aseptic inflammatory process in the bone tissue of patients even in the chronic stage of DNOAP. These data may help in deciding whether to use one or another method of unloading the affected joints, which will affect the clinical prognosis. The study of neurohumoral markers of arthropathy in the blood serum of patients with DM2 is carried out for the first time, and therefore it is difficult to compare with the results of other authors. It can be assumed that copeptin and CRP are significant markers of persistent inflammation of the osteoarticular structures of the foot in DNOAP.
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神经体液因子在糖尿病神经骨关节病患者无菌性骨炎症持续中的作用
背景:糖尿病神经骨关节病(DNOAP, Charcot足)是糖尿病(DM)的一种相对罕见的并发症,它不仅会导致患者下肢支持功能受损,还会导致高位截肢。DNOAP的特点是足部骨结构的持续性无菌性炎症,这给制定治疗措施带来了很大的困难。在医学文献中,有数据表明个体-细胞因子和神经体液因子在糖尿病炎症过程延长中的作用,然而,目前很少有研究确定DNOAP无菌性炎症的可靠标志物。目的:探讨神经体液因子和晚期糖基化终产物对2型糖尿病(DM2)合并糖尿病神经骨关节病患者足部无菌性炎症活性的影响。材料和方法。该研究包括88名2型糖尿病患者(45名男性,43名女性)。1组为DM2合并无活性DNOAP患者(n= 43), 2组为无骨关节病变的DM2合并远端糖尿病神经病变患者(n= 45)。糖尿病性神经病变的诊断是基于临床表现和外周敏感性指标的分析。DNOAP的诊断和分期是根据临床资料、足部红外测温和影像学检查结果确定的。采用一般临床评价、影像学检查(x线、MRI)、CRP、钙保护蛋白、copeptin、谷胱甘肽过氧化物酶1 (GP1)的评价。根据足部检查和触诊结果,以及患肢和对侧肢体皮肤温度梯度分析(红外测温),检测DNOAP并确定该并发症的分期。经MRI检查及临床表现(足部对称部位皮肤温度无差异)证实为慢性DNOAP。根据实验室分析结果,copeptin值差异有统计学意义- 1组- 0.232µg/ml [0.147;0.342], 2组- 0.115µg/ml [0.065;1组CRP -为7.113 mg/l [2.453;16.505], 2组- 2.187 mg/l [1.131;5.567] (p>0.05),各组白细胞水平差异无统计学意义:1组- 7.86 [6.40;9.00]*10^9,第2组- 7.00 [6.00;8.15) (p > 0.05)。DNOAP组钙保护蛋白和谷胱甘肽过氧化物酶-1水平有升高的趋势,但差异不显著。Calprotectin - 1组- 1.948 [1.229;2.969],第2组- 1.692 [1.16;2.514] g/ml, 1组谷胱甘肽过氧化物酶-1 [20.1;31.82],第二组- 22.98 [18.94;31.2 ng / ml.CONCLUSION。本研究中,copeptin和c反应蛋白水平差异有统计学意义:在DNOAP患者中,copeptin和c反应蛋白的值明显较高,这表明即使在DNOAP慢性期,患者骨组织中的无菌性炎症过程仍持续存在。这些数据可能有助于决定是否使用一种或另一种方法卸载受影响的关节,这将影响临床预后。对DM2患者血清中关节病神经体液标志物的研究尚属首次,因此难以与其他作者的结果进行比较。可以认为copeptin和CRP是DNOAP足部骨关节结构持续炎症的重要标志物。
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来源期刊
Diabetes Mellitus
Diabetes Mellitus ENDOCRINOLOGY & METABOLISM-
CiteScore
1.90
自引率
40.00%
发文量
61
审稿时长
7 weeks
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