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发现并验证与肥胖相关的新型中性粒细胞活化标志物。

Discovery and Validation of a Novel Neutrophil Activation Marker Associated with Obesity.

机构信息

Georgia Prevention Institute, Augusta University, Augusta, Gerogia, USA.

Georgia Cancer Center, Augusta University, Augusta, Georgia, USA.

出版信息

Sci Rep. 2019 Mar 5;9(1):3433. doi: 10.1038/s41598-019-39764-4.

Abstract

Obesity is accompanied by low-grade systemic inflammation that etiologically contributes to obesity-induced cardiovascular disease (CVD). Growing evidence supports that neutrophil, the most abundant type of leukocytes in human, is most likely to be the target peripheral leukocyte subtype initiating the inflammatory cascade in obesity. However, few studies have systematically assessed the genome wide changes in neutrophils associated with obesity. In this study, a hypothesis-free OMIC approach (i.e. the discovery phase) and a target approach (i.e. the validation phase) were used to identify obesity related neutrophil activation markers and their roles on CVD risks. In the discovery phase, genome wide DNA methylation, RNA-sequencing and quantitative proteomics were obtained from purified neutrophils (12 obese vs. 12 lean). In the validation phase, gene expression levels of the promising genes from the OMIC platforms were measured in 81 obese cases vs. 83 lean controls, and the association between the expression levels and CVD risks were evaluated. Significant difference was found for one gene, alkaline phosphatase, liver/bone/kidney (ALPL), across 3 OMIC platforms. In the validation phase, the gene expression levels of ALPL in leukocytes were significantly higher in obese compared with lean subjects (p < 0.05). Within the obese population, we observed that ALPL expression level showed significantly positive association with CVD risk factors (p < 0.05) including systolic blood pressure, diastolic blood pressure, mean arterial pressure, carotid intima-media thickness and borderline significance with fasting insulin (p = 0.08). This study identified one novel marker ALPL of neutrophil activation in response to obesity and provided evidence that obesity induced change in ALPL expression was associated with CVD risk factors.

摘要

肥胖伴有低度系统性炎症,从病因学上促进了肥胖引起的心血管疾病(CVD)。越来越多的证据支持,中性粒细胞,即人类中最丰富的白细胞类型,最有可能是引发肥胖中炎症级联反应的外周白细胞亚型的靶标。然而,很少有研究系统地评估与肥胖相关的中性粒细胞的全基因组变化。在这项研究中,采用了无假设的 OMIC 方法(即发现阶段)和靶向方法(即验证阶段)来识别与肥胖相关的中性粒细胞激活标志物及其在 CVD 风险中的作用。在发现阶段,从纯化的中性粒细胞(12 例肥胖与 12 例瘦)中获得了全基因组 DNA 甲基化、RNA 测序和定量蛋白质组学数据。在验证阶段,在 81 例肥胖病例与 83 例瘦对照中测量了 OMIC 平台中有前途的基因的基因表达水平,并评估了表达水平与 CVD 风险之间的关联。在 3 个 OMIC 平台上,有一个基因,碱性磷酸酶,肝/骨/肾(ALPL),发现了显著差异。在验证阶段,白细胞中的 ALPL 基因表达水平在肥胖组中明显高于瘦对照组(p<0.05)。在肥胖人群中,我们观察到 ALPL 表达水平与 CVD 危险因素(p<0.05)呈显著正相关,包括收缩压、舒张压、平均动脉压、颈动脉内膜中层厚度,与空腹胰岛素呈边缘显著相关(p=0.08)。这项研究鉴定了一种新型的中性粒细胞激活标志物 ALPL 对肥胖的反应,并提供了证据表明肥胖诱导的 ALPL 表达变化与 CVD 危险因素有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/867d/6400958/9e8a542a0ee3/41598_2019_39764_Fig1_HTML.jpg

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