Research Unit Molecular Epidemiology, Helmholtz Zentrum München, German Research Center for Environmental Health, Neuherberg, Germany.
Institute of Epidemiology, Helmholtz Zentrum München, German Research Center for Environmental Health, Neuherberg, Germany.
Cardiovasc Diabetol. 2021 May 20;20(1):111. doi: 10.1186/s12933-021-01299-2.
The metabolic syndrome (MetS), defined by the simultaneous clustering of cardio-metabolic risk factors, is a significant worldwide public health burden with an estimated 25% prevalence worldwide. The pathogenesis of MetS is not entirely clear and the use of molecular level data could help uncover common pathogenic pathways behind the observed clustering.
Using a highly multiplexed aptamer-based affinity proteomics platform, we examined associations between plasma proteins and prevalent and incident MetS in the KORA cohort (n = 998) and replicated our results for prevalent MetS in the HUNT3 study (n = 923). We applied logistic regression models adjusted for age, sex, smoking status, and physical activity. We used the bootstrap ranking algorithm of least absolute shrinkage and selection operator (LASSO) to select a predictive model from the incident MetS associated proteins and used area under the curve (AUC) to assess its performance. Finally, we investigated the causal effect of the replicated proteins on MetS using two-sample Mendelian randomization.
Prevalent MetS was associated with 116 proteins, of which 53 replicated in HUNT. These included previously reported proteins like leptin, and new proteins like NTR domain-containing protein 2 and endoplasmic reticulum protein 29. Incident MetS was associated with 14 proteins in KORA, of which 13 overlap the prevalent MetS associated proteins with soluble advanced glycosylation end product-specific receptor (sRAGE) being unique to incident MetS. The LASSO selected an eight-protein predictive model with an (AUC = 0.75; 95% CI = 0.71-0.79) in KORA. Mendelian randomization suggested causal effects of three proteins on MetS, namely apolipoprotein E2 (APOE2) (Wald-Ratio = - 0.12, Wald-p = 3.63e-13), apolipoprotein B (APOB) (Wald-Ratio = - 0.09, Wald-p = 2.54e-04) and proto-oncogene tyrosine-protein kinase receptor (RET) (Wald-Ratio = 0.10, Wald-p = 5.40e-04).
Our findings offer new insights into the plasma proteome underlying MetS and identify new protein associations. We reveal possible casual effects of APOE2, APOB and RET on MetS. Our results highlight protein candidates that could potentially serve as targets for prevention and therapy.
代谢综合征(MetS)是一种由心血管代谢危险因素同时聚集而定义的疾病,是一个具有全球重大公共卫生意义的疾病,其全球患病率估计为 25%。MetS 的发病机制尚不完全清楚,利用分子水平的数据可以帮助揭示观察到的聚集背后的共同发病途径。
我们使用高度多重化的适配体亲和蛋白质组学平台,在 KORA 队列(n=998)中检查了血浆蛋白与现患和新发 MetS 之间的关联,并在 HUNT3 研究(n=923)中复制了我们对现患 MetS 的结果。我们应用了调整年龄、性别、吸烟状态和体力活动的逻辑回归模型。我们使用最小绝对收缩和选择算子(LASSO)的bootstrap 排序算法从新发 MetS 相关蛋白中选择一个预测模型,并使用曲线下面积(AUC)评估其性能。最后,我们使用两样本 Mendelian 随机化研究了复制蛋白对 MetS 的因果效应。
现患 MetS 与 116 种蛋白相关,其中 53 种在 HUNT 中得到了复制。其中包括先前报道的蛋白,如瘦素,以及新的蛋白,如 N 端结构域含有蛋白 2 和内质网蛋白 29。KORA 中的新发 MetS 与 14 种蛋白相关,其中可溶性晚期糖基化终产物特异性受体(sRAGE)是唯一与新发 MetS 相关的蛋白。LASSO 选择了一个由 8 种蛋白组成的预测模型,其 AUC(=0.75;95%CI=0.71-0.79)在 KORA 中。Mendelian 随机化表明,三种蛋白对 MetS 具有因果效应,即载脂蛋白 E2(APOE2)(Wald-Ratio=-0.12,Wald-p=3.63e-13)、载脂蛋白 B(APOB)(Wald-Ratio=-0.09,Wald-p=2.54e-04)和原癌基因酪氨酸蛋白激酶受体(RET)(Wald-Ratio=0.10,Wald-p=5.40e-04)。
我们的研究结果为 MetS 潜在的血浆蛋白质组学提供了新的见解,并确定了新的蛋白关联。我们揭示了 APOE2、APOB 和 RET 对 MetS 可能的因果影响。我们的研究结果突出了一些潜在的蛋白候选物,这些候选物可能成为预防和治疗的靶点。
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