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首页> 外文期刊>Journal of trace elements in medicine and biology: Organ of the Society for Minerals and Trace Elements (GMS) >Comparing functional metabolic effects of marginal and sufficient selenium supply in sheep
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Comparing functional metabolic effects of marginal and sufficient selenium supply in sheep

机译:比较绵羊边际和充足硒供应的功能性代谢效应

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This study was performed to characterise key data of long-term ovine Se metabolism and to work out the best biomarker of Se status. An upgrade from marginal (<0.05. mg Se/kg diet, 'Se-') to sufficient (0.2. mg Se/kg diet, 'Se+') nutritional Se supply using sodium selenite was monitered biweekly by analysing Se concentration, glutathione peroxidase (Gpx) activity and routine biochemistry in blood/serum over 2 years. Se, Cu, Zn, cytosolic Gpx and thioredoxin reductase (TrxR) activity were measured in the liver (biopsies/post-mortem). Se, Gpx, TrxR, glutathione-S-transferase-alpha (aGST) and iodothyronine deiodinase (Dio1) were analysed in the kidney, heart muscle and thyroid. Relative mRNA expression of hepatic aGST1 and Gpx1 was determined.Improvement of Se supply strongly increased serum and liver Se concentration within 10 and 20 days, respectively followed by a plateau. Whereas the achievement of a maximum whole blood Gpx activity was reached after 3 months, serum Gpx3 activity increased with high variations. Hepatic Gpx activity reached a maximum during days 100-200, decreasing thereafter. Distinct group differences in Se and cytosolic Gpx activity were evident in all organs (except Se in kidney). TrxR and Dio1 activity was affected only in the liver. The Se- sheep showed an ongoing decrease in serum Se concentration within 2 years, whereas liver Se remained almost unaffected. High relative Gpx1 mRNA expression in the Se+ group was consensual to high hepatic Gpx activity. Relative mRNA expression of hepatic aGST1 was higher in the Se- sheep. Clinical signs and abnormalities in routine biochemistry were absent.In summary, the best biomarker of Se deprivation and nutritional Se upgrade, respectively was Se in serum. Moreover, hepatic Se concentrations reliably reflected the upgrade of Se supply within days. Whole blood Gpx reacts slowly depending on newly formed erythrocytes restricting its diagnostic use. Vital organs are affected by Se deficiency due to a decrease of cytosolic Gpx activity attenuating the antioxidative system. Cellular up-regulation of aGST1 mRNA expression in the Se- group is assumed to partially compensate for the decreased antioxidant defence due to a loss in Gpx activity. This sheep model appears advantageous for long-term studies on sub-clinical metabolic effects in experimental modifiable nutritional Se supply.
机译:进行这项研究是为了表征绵羊长期硒代谢的关键数据,并找出硒状态的最佳生物标志物。通过分析硒浓度,谷胱甘肽过氧化物酶,每两周监测一次使用亚硒酸钠从少量(<0.05。mg Se / kg饮食,“ Se-”)的营养补充(0.2。mg Se / kg饮食,“ Se +”)的增加。 (Gpx)活动和2年以上血液/血清中的常规生物化学。测定了肝脏中的硒,铜,锌,胞质Gpx和硫氧还蛋白还原酶(TrxR)的活性(活检/验尸)。在肾脏,心肌和甲状腺中分析了Se,Gpx,TrxR,谷胱甘肽-S-转移酶-α(aGST)和碘甲状腺素脱碘酶(Dio1)。测定了肝aGST1和​​Gpx1的相对mRNA表达。硒供应的改善分别在10和20天内分别使血清和肝脏中的硒浓度升高,随后达到平台期。在3个月后达到最大全血Gpx活性的同时,血清Gpx3活性却有很大的变化。肝Gpx活性在100-200天达到最高,此后下降。在所有器官(肾脏中的硒除外)中,硒和胞质Gpx活性的明显组差异均明显。 TrxR和Dio1活性仅在肝脏中受到影响。绵羊在2年内显示血清Se浓度持续下降,而肝脏Se几乎未受影响。 Se +组中较高的相对Gpx1 mRNA表达与较高的肝Gpx活性有关。绵羊肝aGST1的相对mRNA表达较高。缺乏常规生化反应的临床体征和异常。总之,最佳的硒剥夺和营养性硒升级的最佳生物标志物是血清中的硒。此外,肝中硒的浓度可靠地反映了几天之内硒供应的增加。全血Gpx反应缓慢,具体取决于新形成的红细胞,从而限制了其诊断用途。硒缺乏会影响生命器官,这是由于胞质Gpx活性降低导致抗氧化系统减弱。 Se-基团中aGST1 mRNA表达的细胞上调被认为部分补偿了由于Gpx活性降低而导致的抗氧化防御能力下降。这种绵羊模型对于长期研究可调节营养硒的亚临床代谢效应似乎是有利的。

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