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铜暴露与铜代谢的潜在生物标志物。

Copper exposure and potential biomarkers of copper metabolism.

作者信息

Araya Magdalena, Olivares Manuel, Pizarro Fernando, González Mauricio, Speisky Hernán, Uauy Ricardo

机构信息

Institute of Nutrition and Food Technology (INTA), University of Chile, Jose Pedro Alessandri 5540, Macul, Santiago II, Chile.

出版信息

Biometals. 2003 Mar;16(1):199-204. doi: 10.1023/a:1020723117584.

Abstract

Relevant biological effects associated with mild to moderate copper deficiency and copper excess are unknown. It is difficult to identify markers of these early changes because limits of the homeostatic range are still undefined and early changes may represent adaptive responses that do not imply necessarily risk of damage. We report here a series of studies carried out to shed light on the responses within the homeostatic range, by assessing classic parameters of copper status in humans at different copper exposure. In adult healthy volunteers that had an estimated daily intake of 0.9 mg Cu/day (approximately 15 microg/kg/d), exposure to additional 50-60 microg of copper/kg/day for three months or up to 150 microg/kg/d for two months resulted in no significant changes of SOD activity in erythrocytes, of copper concentration (in serum, erythrocytes and mononuclear cells) and of serum ceruloplasmin (ANOVA). Neither were found differences by gender or age. As in previous studies in infants, the non-ceruloplasmin copper fraction was positively correlated to serum copper (r = 0.58). Assessing variations on copper absorption, infants supplemented/not supplemented with oral copper (80 ug/kg/14 days), at age 1 and 3 months, showed copper absorption close to 80% at both ages; no effect was observed for age or supplementation, suggesting that either these concentrations do not elicit regulatory mechanisms or that at this age down regulation for copper absorption is not efficient. These studies indicate that in the range of the copper homeostasis area the markers tested are not suitable to detect mild changes (within the homeostatic range) of copper metabolism.

摘要

与轻度至中度铜缺乏和铜过量相关的相关生物学效应尚不清楚。由于稳态范围的界限仍未明确,且早期变化可能代表适应性反应,不一定意味着有损伤风险,因此很难识别这些早期变化的标志物。我们在此报告了一系列研究,旨在通过评估不同铜暴露水平下人体铜状态的经典参数,来阐明稳态范围内的反应。在估计每日铜摄入量为0.9毫克/天(约15微克/千克/天)的成年健康志愿者中,每天额外摄入50 - 60微克铜/千克,持续三个月,或每天摄入高达150微克铜/千克,持续两个月,红细胞中超氧化物歧化酶(SOD)活性、铜浓度(血清、红细胞和单核细胞中的)以及血清铜蓝蛋白均无显著变化(方差分析)。按性别或年龄也未发现差异。与之前对婴儿的研究一样,非铜蓝蛋白铜部分与血清铜呈正相关(r = 0.58)。评估铜吸收的变化时,1个月和3个月大时补充/未补充口服铜(80微克/千克/14天)的婴儿,两个年龄段的铜吸收均接近80%;未观察到年龄或补充剂的影响,这表明要么这些浓度不会引发调节机制,要么在这个年龄段铜吸收的下调效率不高。这些研究表明,在铜稳态范围内,所测试的标志物不适合检测铜代谢的轻度变化(在稳态范围内)。

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