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使用稳定同位素²⁵Mg研究婴儿镁代谢的可行性。

Feasibility of using the stable isotope 25Mg to study Mg metabolism in infants.

作者信息

Schuette S A, Ziegler E E, Nelson S E, Janghorbani M

机构信息

Department of Medicine, University of Chicago, Illinois 60637.

出版信息

Pediatr Res. 1990 Jan;27(1):36-40. doi: 10.1203/00006450-199001000-00013.

DOI:10.1203/00006450-199001000-00013
PMID:2296469
Abstract

The feasibility of using isotopic techniques to study Mg absorption and metabolism was explored in three full-term human infants. 25Mg (98.8 atom %) was administered orally as an in vivo tracer. Fractional 25Mg absorption, isotope retention, endogenous fecal Mg losses, and apparent Mg exchangeable pool size were then determined under three conditions of isotope administration: 1) 20 mg 25Mg, with single feeding; 2) 20 mg 25Mg, distributed over a 24-h period; and 3) 60 mg 25Mg, over a 24-h period. Mg isotope ratios were determined by inductively coupled plasma mass spectrometry. Fractional absorption was increased in all three infants after distributed versus bolus administration at the 20 mg dose; mean (+/- SD) fractional absorption was 64.0 +/- 3.9 versus 54.3 +/- 5.9%, respectively. 25Mg retention was also more in all three infants after distributed administration (55.8 +/- 3.0 versus 44.3 +/- 1.3% of dose). At the 60-mg 25Mg dose, compared to 20 mg, fractional absorption was reduced but absolute isotope absorption more than doubled in all infants; urine isotope losses represented a similar fraction of the absorbed dose, thus, 25Mg retention also more than doubled. Compared to the results of the isotope studies, net Mg absorption and balance were uninfluenced by total Mg intake. Isotope retention with distributed isotope administration resulted in measurable isotopic enrichment of plasma and erythrocytes at 72 h (i.e. plasma isotope enrichment was 6.3-10.2 and 19.2-23.5% for the 20- and 60-mg dose, respectively). With these doses, apparent Mg exchangeable pool size ranged from 5.5 to 7.6 mmol/kg body wt; these values showed a decrease with age both within and between infants.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在三名足月健康婴儿中探索了使用同位素技术研究镁吸收和代谢的可行性。口服给予25Mg(98.8原子%)作为体内示踪剂。然后在三种同位素给药条件下测定25Mg的分数吸收、同位素保留、内源性粪便镁损失以及表观镁可交换池大小:1)单次喂食20mg 25Mg;2)20mg 25Mg在24小时内分次给予;3)60mg 25Mg在24小时内分次给予。通过电感耦合等离子体质谱法测定镁同位素比率。在20mg剂量下,与单次大剂量给药相比,分次给药后所有三名婴儿的分数吸收均增加;平均(±标准差)分数吸收分别为64.0±3.9%和54.3±5.9%。分次给药后所有三名婴儿的25Mg保留也更多(分别为给药剂量的55.8±3.0%和44.3±1.3%)。在60mg 25Mg剂量下,与20mg相比,分数吸收降低,但所有婴儿的绝对同位素吸收增加了一倍多;尿液同位素损失占吸收剂量的比例相似,因此,25Mg保留也增加了一倍多。与同位素研究结果相比,总镁摄入量对净镁吸收和平衡没有影响。分次给予同位素后,72小时时血浆和红细胞出现可测量的同位素富集(即20mg和60mg剂量下血浆同位素富集分别为6.3 - 10.2%和19.2 - 23.5%)。在这些剂量下,表观镁可交换池大小为5.5至7.6mmol/kg体重;这些值在婴儿内部和婴儿之间均随年龄降低。(摘要截断于250字)

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