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首页> 外文期刊>Developmental Immunology: Journal of Immunology Research >Circulating Immune Complexes among Diabetic Children
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Circulating Immune Complexes among Diabetic Children

机译:糖尿病儿童中的循环免疫复合物

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摘要

Insulin dependent diabetes mellitus (IDDM) is an autoimmune disease associated with the presence of different types of autoantibodies. The presence of these antibodies and the corresponding antigens in the circulation leads to the formation of circulating immune complexes (CIC). CIC are known to persist in the blood for long periods of time. Such CIC following deposition in the small blood vessels have the potential to lead to microangiopathy with debilitating clinical consequences. The aim of our pilot study was to investigate whether a correlation exists between CIC and the development of microvascular complications in diabetic children. Isolation of a new glycoprotein complement inhibition factor (CIF) from the parasitic plantCuscuta europeaseed, which appears to bind specifically to complement component C3 has provided an unique tool for the measurement of immune complexes by means of ELISA-type techniques (CIF-ELISA). We studied the levels of CIC (IgG, IgM and IgA) in 58 diabetic children (mean age 12.28±4.04 years, diabetes duration 5.3±3.7 years), 29 of them had vascular complications (group 1) and the other 29 were without vascular complications (group 2). As controls, we studied sera samples from 21 healthy children (mean age 13.54±4.03 years). Sera from the diabetic patients showed statistically significant higher levels of CIC IgG (p=0.03) than sera from the control group. In sera from group 1 values of CIC IgG showed statistically significant higher levels than controls (0.720±0.31 vs. 0.46±0.045; p=0.011) Sera from 59% of the patients were positive for CIC IgG, 36% for CIC IgM and 9% for CIC IgA. Among 26 patients with microalbuminuria, sera from 17/26 (65%) were positive for CIC IgG, 8/26 (31%) for CIC IgM and 2/26 (8%) for CIC IgA. CIC IgG correlated with HbA1c (r=0.51;p=0.005) and microalbuminuria (r=0.42,p=0.033). CIC IgA correlated with age (r=0.44,p=0.03). CIC IgM correlated with the duration of diabetes (r=0.63,p=0.02). These findings suggest that elevated levels of CIC IgG are associated with the development of early diabetic nephropathy.
机译:胰岛素依赖型糖尿病(IDDM)是一种自身免疫性疾病,与不同类型的自身抗体有关。这些抗体和相应抗原在循环系统中的存在导致循环免疫复合物(CIC)的形成。已知CIC在血液中会长期存在。在小血管中沉积后的这种CIC有可能导致微血管病变,并破坏临床效果。我们的初步研究的目的是调查在糖尿病儿童中CIC与微血管并发症的发展之间是否存在相关性。从寄生植物欧洲化的Cuscuta中分离出一种新糖蛋白补体抑制因子(CIF),该因子似乎与补体成分C3特异性结合,为通过ELISA型技术(CIF-ELISA)测量免疫复合物提供了独特的工具。我们研究了58名糖尿病儿童(平均年龄12.28±4.04岁,糖尿病病程5.3±3.7岁)的CIC(IgG,IgM和IgA)水平,其中29例患有血管并发症(第1组),另外29例没有血管并发症并发症(第2组)。作为对照,我们研究了21名健康儿童(平均年龄13.54±4.03岁)的血清样本。糖尿病患者的血清显示CIC IgG的统计学水平显着高于对照组的血清(p = 0.03)。在第1组血清中,CIC IgG的值显示出比对照组更高的统计学显着水平(0.720±0.31对0.46±0.045; p = 0.011),来自59%的患者的血清CIC IgG阳性,CIC IgM的阳性率为36%,9 CIC IgA的百分比。在26例微量白蛋白尿患者中,血清CIC IgG阳性的比例为17/26(65%),CIC IgM的血清阳性率为8/26(31%),CIC IgA的血清为2/26(8%)。 CIC IgG与HbA1c(r = 0.51; p = 0.005)和微量白蛋白尿(r = 0.42,p = 0.033)相关。 CIC IgA与年龄相关(r = 0.44,p = 0.03)。 CIC IgM与糖尿病持续时间相关(r = 0.63,p = 0.02)。这些发现表明,CIC IgG水平升高与早期糖尿病肾病的发展有关。

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