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胎球蛋白-A/α2-赫里曼斯-施密德糖蛋白与慢性肾脏病患者的代谢综合征有关吗?

Is fetuin-A/alpha2-Heremans-Schmid glycoprotein associated with the metabolic syndrome in patients with chronic kidney disease?

作者信息

Axelsson Jonas, Wang Xin, Ketteler Markus, Qureshi Abdul Rashid, Heimbürger Olof, Bárány Peter, Lindholm Bengt, Nordfors Louise, Stenvinkel Peter

机构信息

Division of Renal Medicine, Department of Clinical Science, Intervention and Technology, Karolinska Institutet, Stockholm, Sweden.

出版信息

Am J Nephrol. 2008;28(4):669-76. doi: 10.1159/000121358. Epub 2008 Mar 13.

Abstract

INTRODUCTION

Components of the metabolic syndrome are highly prevalent in chronic kidney disease (CKD) patients--some of which paradoxically appear to predict an improved outcome in this population. We hypothesized that the circulating calcification inhibitor fetuin-A/AHSG, which is also a natural inhibitor of the tyrosine kinase insulin receptor, could be one factor explaining the association between increased fat mass and a survival advantage in CKD and thus conducted an explorational study to provide preliminary data to support further research into this hypothesis.

PATIENTS AND METHODS

In a cross-sectional study, we evaluated 198 CKD stage 5 patients (GFR 6.8 +/- 0.2 ml/min; 62% males, mean age 52 +/- 1 years) close to the start of renal replacement therapy. We studied circulating AHSG (ELISA) and two common functional AHSG gene polymorphisms (at amino acids Thr248Met (C-T) and Thr256Ser (C-G) using Pyrosequencing) and related these to multiple components of the metabolic syndrome.

RESULTS

Median circulating AHSG was lower (p < 0.01) in type-2 (0.22 g/l) and type-1 (0.16 g/l) diabetics as compared to non-diabetic CKD-5 patients (0.24 g/l). AHSG correlated with both total and truncal fat mass in type-2 diabetics (rho 0.37 and 0.39; p < 0.001, respectively), but not in type-1 diabetics or non-diabetics. Both SNPs significantly influenced circulating levels of AHSG, and were also associated with significant differences in serum triglycerides and HDL cholesterol. Furthermore, there were significant differences in the prevalence of metabolic syndrome criteria between the AHSG Thr256Ser (C-G) genotype groups, with a more atherogenic lipid profile in AHSG high producers (Thr/Thr homozygotes). In multivariate analysis, the association between circulating AHSG and fat mass remained significant also after adjustment for age, gender, inflammation (CRP >10 mg/l), and AHSG genotype.

CONCLUSIONS

The present, explorational, study supports further, mechanistic, studies into a physiological link between AHSG and body fat mass in patients with CKD. As we observed an association between higher fat mass and elevated AHSG levels, these preliminary results may form the basis of further study to establish if the observed associations may be one reason why obesity has been reported to constitute a survival advantage in CKD.

摘要

引言

代谢综合征的各个组成部分在慢性肾脏病(CKD)患者中高度普遍,其中一些因素似乎反常地预示着该人群预后改善。我们推测,循环钙化抑制剂胎球蛋白-A/AHSG,它也是酪氨酸激酶胰岛素受体的天然抑制剂,可能是解释CKD患者脂肪量增加与生存优势之间关联的一个因素,因此开展了一项探索性研究,以提供初步数据支持对这一假设的进一步研究。

患者与方法

在一项横断面研究中,我们评估了198例接近开始肾脏替代治疗的CKD 5期患者(肾小球滤过率6.8±0.2 ml/分钟;62%为男性,平均年龄52±1岁)。我们研究了循环中的AHSG(酶联免疫吸附测定法)以及两个常见的功能性AHSG基因多态性(使用焦磷酸测序法检测氨基酸Thr248Met(C-T)和Thr256Ser(C-G)),并将这些与代谢综合征的多个组成部分相关联。

结果

与非糖尿病CKD-5患者(0.24 g/l)相比,2型糖尿病患者(0.22 g/l)和1型糖尿病患者(0.16 g/l)的循环AHSG中位数较低(p<0.01)。在2型糖尿病患者中,AHSG与总脂肪量和躯干脂肪量均相关(rho分别为0.37和0.39;p<0.001),但在1型糖尿病患者或非糖尿病患者中无此关联。两个单核苷酸多态性均显著影响AHSG的循环水平,并且还与血清甘油三酯和高密度脂蛋白胆固醇的显著差异相关。此外,AHSG Thr256Ser(C-G)基因型组之间代谢综合征标准的患病率存在显著差异,AHSG高生产者(Thr/Thr纯合子)的脂质谱更具动脉粥样硬化性。在多变量分析中,调整年龄、性别、炎症(C反应蛋白>10 mg/l)和AHSG基因型后,循环AHSG与脂肪量之间的关联仍然显著。

结论

本探索性研究支持对CKD患者中AHSG与体脂量之间的生理联系进行进一步的机制研究。由于我们观察到较高的脂肪量与升高的AHSG水平之间存在关联,这些初步结果可能构成进一步研究的基础,以确定所观察到的关联是否可能是肥胖在CKD中被报道具有生存优势的原因之一。

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