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氧化应激在肌肉减少症中增加,并与肌肉减少症肥胖症相关的心血管疾病风险相关。

Oxidative stress is increased in sarcopenia and associated with cardiovascular disease risk in sarcopenic obesity.

机构信息

Department of Medical and Surgical Sciences, University of Foggia, Italy.

Department of Medical and Surgical Sciences, University of Foggia, Italy.

出版信息

Maturitas. 2018 Mar;109:6-12. doi: 10.1016/j.maturitas.2017.12.002. Epub 2017 Dec 5.


DOI:10.1016/j.maturitas.2017.12.002
PMID:29452783
Abstract

OBJECTIVES: To define whether circulating markers of oxidative stress correlate with sarcopenia in terms of glutathione balance and oxidative protein damage, and whether these biomarkers are associated with risk of cardiovascular disease (CVD). STUDY DESIGN: Population-based cross-sectional study. 115 out of 347 elderly subjects were classified as non-sarcopenic non-obese (NS-NO), sarcopenic non-obese (S-NO), non-sarcopenic obese (NS-O), and sarcopenic obese (S-O). MAIN OUTCOME MEASUREMENTS: Sarcopenia was defined as a relative skeletal muscle mass index (RASM) <7.25kg/m for men or <5.67kg/m for women, while obesity was diagnosed in those presenting with% fat >27 for men or >38 for women. The CVD risk was estimated by the carotid intima-media thickness (IMT) and the Framingham score. Blood reduced glutathione (GSH), oxidized glutathione (GSSG), plasma malondialdehyde-(MDA) and 4-hydroxy-2,3-nonenal-(HNE) protein adducts were analyzed. RESULTS: Significantly greater blood GSSG/GSH ratio and plasma MDA/HNE protein adducts were observed in sarcopenic than in non-sarcopenic patients. A logistic regression model showed a close relationship between serum HNE and MDA adducts and sarcopenia (OR=1.133, 95% CI 1.057-1.215, and OR=1.592, 95% CI 1.015-1.991, respectively). Linear and logistic regression analysis evidenced strong associations between the IMT or the Framingham CVD risk category and blood GSSG/GSH or serum HNE protein adducts in the S-O group. CONCLUSION: Circulating markers of oxidative stress are increased in sarcopenia and related to CVD risk in sarcopenic obesity, suggesting that redox balance analysis would be a useful part of a multidimensional evaluation in aging. Further research is encouraged to support interventional strategies to correct redox imbalance, which might contribute to the prevention or at least limitation of sarcopenia and its co-morbidities.

摘要

目的:确定氧化应激的循环标志物是否与谷胱甘肽平衡和氧化蛋白损伤有关,以及这些生物标志物是否与心血管疾病(CVD)风险相关。 研究设计:基于人群的横断面研究。347 名老年人中,有 115 人被分类为非肌少症非肥胖(NS-NO)、肌少症非肥胖(S-NO)、非肌少症肥胖(NS-O)和肌少症肥胖(S-O)。 主要观察指标:肌少症的定义为相对骨骼肌质量指数(RASM)<7.25kg/m 男性或<5.67kg/m 女性,而肥胖则定义为男性体脂百分比>27%或女性体脂百分比>38%。CVD 风险通过颈动脉内膜中层厚度(IMT)和弗雷明汉评分来估计。分析血液还原型谷胱甘肽(GSH)、氧化型谷胱甘肽(GSSG)、血浆丙二醛(MDA)和 4-羟基-2,3-壬烯醛(HNE)蛋白加合物。 结果:与非肌少症患者相比,肌少症患者的血液 GSSG/GSH 比值和血浆 MDA/HNE 蛋白加合物明显更高。逻辑回归模型显示,血清 HNE 和 MDA 加合物与肌少症密切相关(OR=1.133,95%CI 1.057-1.215 和 OR=1.592,95%CI 1.015-1.991)。线性和逻辑回归分析表明,在 S-O 组中,IMT 或弗雷明汉 CVD 风险类别与血液 GSSG/GSH 或血清 HNE 蛋白加合物之间存在很强的关联。 结论:氧化应激的循环标志物在肌少症中增加,并与肌少症肥胖的 CVD 风险相关,提示氧化还原平衡分析将成为衰老多维评估的有用部分。鼓励进一步研究支持纠正氧化还原失衡的干预策略,这可能有助于预防或至少限制肌少症及其合并症的发生。

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