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铁储存与糖尿病的相互作用:铁储存与血红素加氧酶的活性和微卫星多态性与 2 型糖尿病有关。

Cross-talk between body iron stores and diabetes: iron stores are associated with activity and microsatellite polymorphism of the heme oxygenase and type 2 diabetes.

机构信息

Micronutrient Laboratory, Nutrition Institute and Food Technology (INTA), Department of Medicine, Medicine Faculty, University of Chile, El Líbano 5524, Macul, Santiago, Chile.

出版信息

Biol Trace Elem Res. 2011 Nov;143(2):625-36. doi: 10.1007/s12011-010-8895-7. Epub 2010 Nov 16.

Abstract

To assess the relationship between the length of (GT)n repeats in HO-1 gene promoter and heme oxygenase (HO) enzymatic activity in mononuclear cells with iron (Fe) stores in type 2 diabetic mellitus (DM2) patients and metabolic syndrome (MS) subjects, we studied 163 patients with DM2, 185 with MS, and 120 controls subjects. We evaluated iron status (hemoglobin and serum Fe, ferritin, and transferrin receptor), and we determined the length of (GT)n repeats in HO-1 gene promoter by capillary electrophoresis and HO enzymatic activity in mononuclear cells and assessed the relationship between these results and Fe stores. Only 1/163, 6/185, and 7/120 had iron deficiency anemia in DM2 patients, MS subjects, and controls, respectively. No iron overload (ferritin>200 μg/L) was detected in all the subjects studied. DM2 patients had higher iron deposits, total body iron, and heme oxygenase activity (a suggestion of high oxidative stress condition) than MS subjects and controls. In DM2, we found a positive association between serum iron and HO activity. There were no difference in allelic frequency between the three groups; however, among DM2 and MS patients, the frequency of short/medium (SM) genotype of (GT)n repetition was increased and medium/medium (MM) genotype of (GT)n repetition was lower than controls. These results imply that DM2 patients and individuals with MS carrying SM repeats might have higher susceptibility to develop diabetes consequences. This increased susceptibility could be Fe-mediated oxidative stress.

摘要

为了评估 2 型糖尿病(DM2)患者和代谢综合征(MS)患者单核细胞中血红素加氧酶(HO)基因启动子中(GT)n 重复长度与亚铁血红素氧合酶(HO)酶活性之间的关系,以及铁(Fe)储存之间的关系,我们研究了 163 例 DM2 患者、185 例 MS 患者和 120 例对照患者。我们评估了铁状态(血红蛋白和血清 Fe、铁蛋白和转铁蛋白受体),通过毛细管电泳测定 HO-1 基因启动子中(GT)n 重复的长度,并测定单核细胞中 HO 酶活性,并评估这些结果与 Fe 储存之间的关系。仅在 1/163、6/185 和 7/120 的 DM2 患者、MS 患者和对照组患者中发现缺铁性贫血。在所有研究对象中均未检测到铁过载(铁蛋白>200μg/L)。DM2 患者的铁沉积、总铁和血红素氧合酶活性高于 MS 患者和对照组(提示存在高氧化应激状态)。在 DM2 中,我们发现血清铁与 HO 活性之间存在正相关。三组之间的等位基因频率没有差异;然而,在 DM2 和 MS 患者中,(GT)n 重复的短/中(SM)基因型的频率增加,而中/中(MM)基因型的频率低于对照组。这些结果表明,携带 SM 重复的 DM2 患者和 MS 患者可能更容易发生糖尿病后果。这种增加的易感性可能是 Fe 介导的氧化应激。

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