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2 型糖尿病伴或不伴远端感觉运动多发性神经病患者的皮肤晚期糖基化终产物。

Skin Advanced Glycation End Products among Subjects with Type 2 Diabetes Mellitus with or without Distal Sensorimotor Polyneuropathy.

机构信息

Diabetes Centre-Diabetic Foot Clinic, Second Department of Internal Medicine, Democritus University of Thrace, University Hospital of Alexandroupolis, Greece.

Department of Medical Statistics, Medical School, Democritus University of Thrace, Alexandroupolis, Greece.

出版信息

J Diabetes Res. 2021 Nov 28;2021:6045677. doi: 10.1155/2021/6045677. eCollection 2021.

Abstract

MATERIALS AND METHODS

We included 132 subjects (88 men) with a mean age of 64.57 years and median T2DM duration of 14.5 years. Skin AGEs were measured with AGE reader mu connect (Diagnoptics) on the dominant arm. The device enables single and automated triplicate measurements: both of these were performed. DSPN was diagnosed through the neuropathy disability score (NDS). Small nerve fibre function was assessed by temperature and pinprick sensation on the foot. Bilateral measurement of the vibration perception threshold (VPT) on the hallux was carried out by using a neurothesiometer (Horwell Scientific Laboratory Supplies).

RESULTS

Single and triplicate AGE measurements were positively correlated with each other (Pearson's correlation coefficient = 0.991, 95%CI = 0.987-0.994, < 0.001). AGEs were higher among subjects with vs. those without DSPN ( < 0.001). Furthermore, they were higher among subjects with reduced vs. normal temperature sensation ( < 0.001), among subjects with reduced vs. normal pinprick sensation ( = 0.002), among those with abnormal vs. normal monofilament examination ( < 0.001), and among those with abnormal vs. normal VPT ( < 0.001). AGEs were correlated with NDS, VPT, and monofilament score.

CONCLUSIONS

In T2DM, skin AGEs are increased in the presence of DSPN. This holds true both for large and for small nerve function impairment. Moreover, AGEs are correlated with DSPN severity.

摘要

材料与方法

我们纳入了 132 名受试者(88 名男性),平均年龄为 64.57 岁,中位 T2DM 病程为 14.5 年。使用 AGE reader mu connect(Diagnoptics)在优势手臂上测量皮肤 AGEs。该设备可以进行单次和自动重复三次测量:我们进行了这两种测量。DSPN 通过神经病变残疾评分(NDS)诊断。通过足部温度和刺痛感评估小纤维神经功能。使用神经感觉计(Horwell Scientific Laboratory Supplies)对大脚趾的振动感觉阈值(VPT)进行双侧测量。

结果

单次和重复三次 AGE 测量结果呈正相关(Pearson 相关系数 = 0.991,95%CI = 0.987-0.994,<0.001)。与无 DSPN 受试者相比,有 DSPN 受试者的 AGEs 更高(<0.001)。此外,与温度感觉正常的受试者相比,温度感觉降低的受试者 AGEs 更高(<0.001),与刺痛感正常的受试者相比,刺痛感降低的受试者 AGEs 更高(=0.002),与感觉正常的受试者相比,感觉异常的受试者 AGEs 更高(<0.001),与 VPT 正常的受试者相比,VPT 异常的受试者 AGEs 更高(<0.001)。AGEs 与 NDS、VPT 和单丝评分相关。

结论

在 T2DM 中,存在 DSPN 时皮肤 AGEs 增加。这不仅适用于大神经功能障碍,也适用于小神经功能障碍。此外,AGEs 与 DSPN 严重程度相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/39d2/8645371/c3973d3883de/JDR2021-6045677.001.jpg

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