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Circulating and urinary transforming growth factor beta 1, Amadori albumin, and complications of type 1 diabetes: the EURODIAB prospective complications study

机译:循环和尿转化生长因子β1,amadori白蛋白和1型糖尿病并发症:EURODIaB前瞻性并发症研究

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摘要

Objective-Transforming growth factor (TGF)-beta1 is overexpressed in diabetes as a consequence of hyperglycemia and the creation of early glycated end products and may be responsible for the characteristic structural renal changes associated with diabetes. We sought to examine the role of both urinary and circulating TGF-beta1 and its promoter Amadori albumin in the vascular complications of type 1 diabetes. Research Design and Methods-The present article reports on a nested case-control study from the EURODIAB Prospective Complications Study of Europeans with type 1 diabetes. Case subjects (n=356) were all individuals with one or more complications of diabetes; control subjects (n=185) were all individuals with no evidence of complications. Results-Urinary TGF-beta1 and Amadori albumin were elevated in patients with micro- or macroalbuminuria. Standardized regression effects (SREs) for macroalbuminuria versus normoalbuminuria were 2.45 (95% CI 1.88-3.18, P=0.0001 for urinary TGF-beta1) and 1.67 (1.34-2.07, P=0.001 for Amadori albumin). The SIZE for urinary TGF-beta1 remained statistically significant when adjusted for HbA(1c) Amadori albumin, and blood pressure. Circulating TGF-beta1 was elevated in individuals with proliferative retinopathy compared with individuals without retinopathy (SRE 1.29 [1.07-1.550], P=0.007). This result was attenuated to 1.16 (0.95-1.43, P=0.2) in the multivariate model, largely because of HbA(1c). Conclusions-Elevated levels of urinary TGF-beta1 in macroalbuminuria were associated with elevations in Amadori albumin and HbA(1c) and also in blood pressure. In contrast, only circulating TGF-beta1 was related to proliferative retinopathy, and HbA(1c) largely accounted for this. These findings may indicate novel pathways for understanding mechanisms and therapeutic interventions.
机译:由于高血糖症和早期糖基化终产物的产生,目标转化生长因子(TGF)-β1在糖尿病中过表达,并且可能与糖尿病相关的特征性肾脏结构改变。我们试图检查尿液和循环中的TGF-beta1及其启动子Amadori白蛋白在1型糖尿病的血管并发症中的作用。研究设计和方法-本文报道了欧洲1型糖尿病患者EURODIAB前瞻性并发症研究中的嵌套病例对照研究。病例受试者(n = 356)均为患有一种或多种糖尿病并发症的个体。对照组(n = 185)均为无并发症迹象的个体。结果:微白蛋白尿或大白蛋白尿患者的尿中转化生长因子-β1和阿马多里白蛋白升高。大型白蛋白尿与正常白蛋白尿的标准化回归效应(SREs)为2.45(95%CI 1.88-3.18,尿中TGF-β1为P = 0.0001)和1.67(Amadori白蛋白为1.34-2.07,P = 0.001)。调整HbA(1c)Amadori白蛋白和血压后,尿液TGF-beta1的SIZE仍具有统计学意义。与没有视网膜病变的个体相比,患有增殖性视网膜病变的个体的循环TGF-β1升高(SRE 1.29 [1.07-1.550],P = 0.007)。在多变量模型中,此结果衰减至1.16(0.95-1.43,P = 0.2),这主要是由于HbA(1c)。结论大白蛋白尿中尿TGF-β1水平升高与Amadori白蛋白和HbA(1c)升高以及血压升高有关。相比之下,只有循环的TGF-beta1与增生性视网膜病变有关,而HbA(1c)占了大部分。这些发现可能表明了解机制和治疗干预的新途径。

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