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人体测量学指标、预测的内脏脂肪组织和慢性炎症的生物标志物。

Anthropometric measures, predicted visceral adipose tissue and biomarkers of chronic inflammation.

机构信息

HRB Centre for Health and Diet Research, School of Public Health, University College Cork, Cork, Ireland.

School of Public Health, Physiotherapy and Sports Science, University College Dublin, Dublin 4, Ireland.

出版信息

Eur J Clin Invest. 2024 Feb;54(2):e14104. doi: 10.1111/eci.14104. Epub 2023 Oct 9.

Abstract

BACKGROUND

Evidence has linked low-grade systemic inflammation and visceral adipose tissue (VAT) with development of chronic conditions. Cytokines and select proteins released by VAT may promote a low-grade inflammatory response. A number of equations have been developed to estimate VAT levels. In this study, we compared predicted VAT equation relationships with biomarkers of inflammation.

METHODS

This was a cross-sectional study of 2038 men and women aged 46-73 years. Correlation and linear regression analyses were performed to examine inflammatory biomarker relationships with four commonly assessed anthropometric measures and 10 predicted VAT equations.

RESULTS

Compared with anthropometric measures, predicted VAT equations were found to explain a greater proportion of variance in CRP (R  = .075, p = .001), IL-6 (R  = .060, p = .001), TNF-α (R  = .017, p = .005), resistin (R  = .011, p = .012), monocyte (R  = .027, p = .001), eosinophil (R  = .012, p = .01) and basophil (R  = .015, p = .002) levels in males, and a greater variance in concentrations of C3 (R  = .175, p = .001), IL-6 (R  = .090, p = .001), TNF-α (R  = .036, p = .001), adiponectin (R  = .121, p = .001), the adiponectin-to-leptin ratio (R  = .444, p = .001), resistin (R  = .025, p = .001), white blood cell count (R  = .057, p = .001), neutrophils (R  = .061, p = .001) and lymphocytes (R  = .020, p = .001) in females.

CONCLUSION

Equations for assessing VAT levels might be useful to characterise metabolic health. Further studies that examine predicted VAT relationships with disease and mortality outcomes are warranted.

摘要

背景

有证据表明,低度全身炎症和内脏脂肪组织(VAT)与慢性疾病的发展有关。VAT 释放的细胞因子和某些蛋白质可能会引发低度炎症反应。目前已经开发出许多方程式来估计 VAT 水平。在这项研究中,我们比较了预测 VAT 方程与炎症生物标志物的关系。

方法

这是一项横断面研究,共纳入 2038 名年龄在 46-73 岁的男性和女性。进行相关性和线性回归分析,以研究炎症生物标志物与四种常用的人体测量学指标和 10 种预测 VAT 方程之间的关系。

结果

与人体测量学指标相比,预测 VAT 方程能够更好地解释 CRP(R=0.075,p=0.001)、IL-6(R=0.060,p=0.001)、TNF-α(R=0.017,p=0.005)、抵抗素(R=0.011,p=0.012)、单核细胞(R=0.027,p=0.001)、嗜酸性粒细胞(R=0.012,p=0.01)和嗜碱性粒细胞(R=0.015,p=0.002)水平的变异。在男性中,预测 VAT 方程还能更好地解释 C3(R=0.175,p=0.001)、IL-6(R=0.090,p=0.001)、TNF-α(R=0.036,p=0.001)、脂联素(R=0.121,p=0.001)、脂联素与瘦素的比值(R=0.444,p=0.001)、抵抗素(R=0.025,p=0.001)、白细胞计数(R=0.057,p=0.001)、中性粒细胞(R=0.061,p=0.001)和淋巴细胞(R=0.020,p=0.001)水平的变异。在女性中,预测 VAT 方程也能更好地解释以上生物标志物的水平。

结论

评估 VAT 水平的方程可能有助于描述代谢健康状况。进一步研究预测 VAT 与疾病和死亡率的关系是必要的。

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