2型糖尿病周围神经病变的危险因素及相关炎性反应因子分析

摘要
图/表
参考文献
相关文章 (15)

全文: PDF (701 KB) RICH HTML
输出: BibTeX | EndNote (RIS)

摘要目的分析2型糖尿病周围神经病变(diabetic peripheral neuropathy,DPN)的患病情况,并研究其相关危险因素及炎性因子。方法选择2015-01至2016-07临床确诊为2型糖尿病的住院患者,根据DPN诊断标准分为糖尿病周围神经病变组(n=224)及糖尿病非周围神经病变组(n=116),分别检查两组是否合并糖尿病视网膜病变(diabetic retinopathy,DR)、是否合并糖尿病外周血管病变(diabetic peripheral vascular,DPV),并分析年龄、体重、身体质量指数(BMI)、病程、生化指标炎性反应因子与DPN的相关性。对每个指标进行单因素分析,然后进行非条件多因素Logistic分析。结果 (1)糖尿病周围神经病变组(n=224),糖尿病非周围神经病变组(n=116),糖尿病周围神经病变患病率为65.9%;(2)糖尿病周围神经病变组中合并外周血管病变的患者比例(69%)明显高于糖尿病非周围神经病变组(50%),经χ²检验,差异有统计学意义(χ²=5.723,P<0.05);(3)在所分析的各项因素中,糖尿病周围神经病变组的病程、HbA₁c、LDL-C、IL-6、TNF-α、SIL-2R与糖尿病非周围神经病变组的比较,差异有统计学意义(tw 2.084～3.407,P<0.05),其余因素比较差异无统计学意义。(4)Logistic多因素分析:病程、HbA₁c、LDL-C、TNF-α、SIL-2R,以及是否合并外周血管病变均是DPN的独立危险因素(OR:0.455～1.655,P<0.05)。结论随着病程的延长,外周血管的病变,血糖、血脂的升高,以及相关炎性因子的异常,都会使糖尿病神经病变的病情加重。

	服务

	把本文推荐给朋友
	加入我的书架
	加入引用管理器
	E-mail Alert
	RSS
	作者相关文章
	郭杨
	宋晓
	侍晓云
	王莉

关键词 ： 2型糖尿病, 糖尿病周围神经病变, 危险因素, 炎性反应因子

Abstract：Objective Analyze the prevalence situation of Diabetic Peripheral Neuropathy in type 2 diabetes mellitus, study the related risk factors and inflammatory factors.Methods From January 2015 to July 2016,according to DPN diagnostic criteria ,the patients were diagnosed as type 2 diabeteswere divided into diabetic peripheral neuropathy group and non group. Respectively,check whether combined with diabetic retinopathy and peripheral vascular disease, then analysis of age, weight, BMI, course of disease,biochemical indicator,meanwhile, analyse single factor of each index, and then Logistic multivariate analysis.Results (1)The prevalence of diabetic peripheral neuropathy in the study population was 65.9%; (2)The number of combined with peripheral vascular disease in the diabetic peripheral neuropathy group(69%) was significantly higher than that in non diabetic peripheral neuropathy group (50%),through the χ² test,the difference was statistically significant (χ²=5.723,P<0.05); (3)compared with non group,in the analysis of various factors,the HbA₁c、LDL-C、IL-6、TNF-α、SIL-2R and disease course of diabetic peripheral neuropathy group was statistically significant (t=2.084~3.407,P<0.05).But there was no statistically significant difference compared to other factors.(4)Logistic multivariate analysis:Course、HbA₁c、LDL-C、TNF-α、SIR-2R and combined with peripheral vascular disease are independent risk factors for DPN (OR=0.455~1.655,P<0.05).Conclusions The extension of the disease course, peripheral vascular disease, and blood glucose, blood lipid levels and related inflammatory factors of abnormal, will make diabetic neuropathy exacerbations.

Key words： type 2 diabetes mellitus diabetic peripheral neuropathy risk factors inflammatory factors

收稿日期: 2016-10-09

ZTFLH:

R589.1

通讯作者: 侍晓云,E-mail:shixiaoyun1983@126.com

作者简介: 郭杨,硕士研究生。

引用本文:

郭杨, 宋晓, 侍晓云, 王莉. 2型糖尿病周围神经病变的危险因素及相关炎性反应因子分析[J]. 武警医学, 2017, 28(3): 283-286. GUO Yang, SONG Xiao, SHI Xiaoyun, and WANG Li. Risk factors and related inflammatory factors analysis of diabetic peripheral neuropathy in patients with ty. Med. J. Chin. Peop. Armed Poli. Forc., 2017, 28(3): 283-286.

链接本文:

http://journal08.magtechjournal.com/Jwk_wjyx/CN/ 或 http://journal08.magtechjournal.com/Jwk_wjyx/CN/Y2017/V28/I3/283

[1]	王国民,徐宁,尹冬,等.糖尿病周围神经病变的诊断和治疗新进展[J].中国全科医学,2012,15(5):1661-1663.
[2]	马学毅.糖尿病神经病变的诊断与治疗[J].中国糖尿病杂志,2002,10( 5):300-302.
[3]	Xu Y,Wang L,He J.Prevalence and control of diabetes in Chineseadults[J].JAMA,2013,310(9):948-959.
[4]	朱东,鲁丽利,张剑丰,等.糖尿病患者免疫功能改变与预防肺部感染的临床研究[J].中华医院感染学杂志,2015,25(8):1790-1792.
[5]	Vincent A M, Hayes J M, McLean L L, et al. Dyslipidemia-induced neuropathy in mice: the role of oxLDL/LOX-1[J].Diabetes,2009,58(10):2376-2385.
[6]	Coulson W F. Statin neuropathy[J].Fam Pract,2011,60(4):182-184.
[7]	Chong P H, Boskovich A, Stevkovic N. Statin-associated peripheral neuropathy: review of the literature[J].Pharmacotherapy,2004,24(9):1194-1203.
[8]	Gaist D, Jeppesen U, Andersen M, et al.Statins and risk of polyneuropathy: a case-control study[J].Neurology,2002,58(9):1333-1337.
[9]	Singh R, Kishore L, Kaur N. Diabetic peripheral neuropathy: current perspective and future directions[J].Phar Res,2014,80(2):21-35.
[10]	Fromont A, De Seze J, Fleury M C, et al. Inflammatory demyelinating events following treatment with anti-tumor necrosis factor[J].Cytokine,2009,45(2):55-57.
[11]	Barak V, Selmi C, Schlesinger M, et al. Serum inflammatory cytokines, complement components, and soluble interleukin 2 receptor in primary biliary cirrhosis[J].Autoimmun,2009,33(3-4):178-182.
[12]	Garcia Ruiz P, Canora L, ebrato J, et al. Soluble interleukin-2 and tumor necrosis factor receptor in liver cirrhosis[J].Med Clin (Barc),2004,122(12):441-443.
[13]	Joshi S V, Tambwekar S R, Khadalia K, et al. Role of inflammatory marker interleukin 6 (IL-6) and insulin in diabetes and diabetic neuropathy [J].Bom Hosp,2008,50(3):466-471.
[14]	Halvatsiotis I, Tsiotra P C, Ikonomidis I, et al. Genetic variation in the adiponectin receptor 2 (ADIPOR2) gene is associated with coronary artery disease and increased ADIPOR2 expression in peripheral monocytes[J].Car Dia,2010,23(2):9-10.