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首页> 外文期刊>Free radical research >Serum selenium predicts levels of F2-isoprostanes and prostaglandin F2a in a 27 year follow-up study of Swedish men.
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Serum selenium predicts levels of F2-isoprostanes and prostaglandin F2a in a 27 year follow-up study of Swedish men.

机译:在一项为期27年的瑞典男性追踪研究中,血清硒可预测F2-异前列腺素和前列腺素F2a的水平。

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摘要

Low concentrations of selenium (Se) predict mortality and cardiovascular diseases in some populations. The effect of Se on in vivo indicators of oxidative stress and inflammation, two important features of atherosclerosis, in human populations is largely unexplored. This study investigated the longitudinal association between serum selenium (s-Se) and a golden standard indicator of oxidative stress in vivo (8-iso-prostaglandin F2a, a major F2-isoprostane), an indicator of cyclooxygenase (COX)-mediated inflammation (prostaglandin F2a), high sensitive C-reactive protein (hsCRP), interleukin-6 (IL-6) and serum amyloid A protein (SAA) in a follow-up study of 27 years. The s-Se was measured in 615 Swedish men at 50 years of age in a health investigation. The status of oxidative stress and inflammation was evaluated in a re-investigation 27 years later by quantification of urinary 8-iso-PGF2a and 15-keto-dihydro- PGF2a (a major metabolite of PGF2a) and serum hsCRP, SAA and IL-6. Men in the highest quartile of s-Se at age 50 had decreased levels of 8-iso-PGF2a compared to all lower quartiles and decreased levels of PGF2a compared to all lower quartiles at follow-up. These associations were independent of BMI, diabetes, hyperlipidemia, hypertension, smoking, a-tocopherol and ss-carotene at baseline. The s-Se was not associated with hsCRP, SAA or IL-6 at follow-up. In conclusion, high concentrations of s-Se predict reduced levels of oxidative stress and subclinical COX-mediated (but not cytokine-mediated) inflammation in a male population. The associations between Se, oxidative stress and inflammation, respectively, might be related to the proposed cardiovascular protective property of Se.
机译:低浓度的硒(Se)可以预测某些人群的死亡率和心血管疾病。硒对人体中的氧化应激和炎症(动脉粥样硬化的两个重要特征)体内指标的影响尚待探索。这项研究调查了血清硒(s-Se)与体内氧化应激的黄金标准指标(8-异前列腺素F2a,主要的F2-异前列腺素)之间的纵向联系,该指标是环氧合酶(COX)介导的炎症的指标(在长达27年的随访研究中,研究对象包括前列腺素F2a,高敏C反应蛋白(hsCRP),白介素6(IL-6)和血清淀粉样蛋白A(SAA)。在一项健康调查中,对615位50岁的瑞典男性进行了s-Se测量。在27年后的一次重新研究中,通过定量尿中的8-异-PGF2a和15-酮-二氢-PGF2a(PGF2a的主要代谢产物)以及血清hsCRP,SAA和IL-6来评估氧化应激和炎症的状态。 s-Se最高四分位数的男性在50岁时与所有较低四分位数相比降低了8-iso-PGF2a的水平,与随访时所有较低四分位数相比降低了PGF2a的水平。这些关联在基线时独立于BMI,糖尿病,高脂血症,高血压,吸烟,α-生育酚和β-胡萝卜素。随访时,s-Se与hsCRP,SAA或IL-6无关。总之,高浓度的s-Se可预测男性人群中氧化应激水平的降低和亚临床COX介导的(而非细胞因子介导的)炎症。硒,氧化应激和炎症之间的相关性可能与硒对心血管的保护作用有关。

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