Genetic drivers of age-related changes in urinary magnesium excretion.

IF 2.5 4区生物学 Q3 CELL BIOLOGY

Physiological genomics Pub Date : 2024-09-01 Epub Date: 2024-07-22 DOI:10.1152/physiolgenomics.00119.2023

Wouter H van Megen, Jeroen H F de Baaij, Gary A Churchill, Olivier Devuyst, Joost G J Hoenderop, Ron Korstanje

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引用次数: 0

Abstract

Although age-dependent alterations in urinary magnesium (Mg²⁺) excretion have been described, the underlying mechanism remains elusive. As heritability significantly contributes to variations in urinary Mg²⁺ excretion, we measured urinary Mg²⁺ excretion at different ages in a cohort of genetically variable Diversity Outbred (DO) mice. Compared with animals aged 6 mo, an increase in Mg²⁺ excretion was observed at 12 and 18 mo. Quantitative trait locus (QTL) analysis revealed an association of a locus on chromosome 10 with Mg²⁺ excretion at 6 mo of age, with Oit3 (encoding oncoprotein-induced transcript 3; OIT3) as our primary candidate gene. To study the possible role of OIT3 in renal Mg²⁺ handling, we generated and characterized Oit3 knockout (Oit3^-/-) mice. Although a slightly lower serum Mg²⁺ concentration was present in male Oit3^-/- mice, this effect was not observed in female Oit3^-/- mice. In addition, urinary Mg²⁺ excretion and the expression of renal magnesiotropic genes were unaltered in Oit3^-/- mice. For animals aged 12 and 18 mo, QTL analysis revealed an association with a locus on chromosome 19, which contains the gene encoding TRPM6, a known Mg²⁺ channel involved in renal Mg²⁺ reabsorption. Comparison with RNA sequencing (RNA-Seq) data revealed that Trpm6 mRNA expression is inversely correlated with the QTL effect, implying that TRPM6 may be involved in age-dependent changes in urinary Mg²⁺ excretion in mice. In conclusion, we show here that variants in Oit3 and Trpm6 are associated with urinary Mg²⁺ excretion at distinct periods of life, although OIT3 is unlikely to affect renal Mg²⁺ handling.NEW & NOTEWORTHY Aging increased urinary magnesium (Mg²⁺) excretion in mice. We show here that variation in Oit3, a candidate gene for the locus associated with Mg²⁺ excretion in young mice, is unlikely to be involved as knockout of Oit3 did not affect Mg²⁺ excretion. Differences in the expression of the renal Mg²⁺ channel TRPM6 may contribute to the variation in urinary Mg²⁺ excretion in older mice.

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尿镁排泄量与年龄相关变化的遗传驱动因素。

虽然尿镁（Mg2+）排泄量的变化与年龄有关，但其潜在机制仍然难以捉摸。由于遗传性对尿液 Mg2+ 排泄的变化有很大影响，我们在一组遗传多变的多样性杂交（DO）小鼠中测量了不同年龄段的尿液 Mg2+ 排泄。与 6 个月大的小鼠相比，12 个月和 18 个月大的小鼠的 Mg2+ 排泄量有所增加。定量性状位点（QTL）分析表明，10号染色体上的一个位点与6月龄小鼠的Mg2+排泄有关，Oit3（编码肿瘤蛋白诱导转录本3；OIT3）是我们的主要候选基因。为了研究 OIT3 在肾脏 Mg2+ 处理中可能发挥的作用，我们产生了 Oit3 基因敲除（Oit3-/-）小鼠并对其进行了鉴定。虽然雄性 Oit3-/- 小鼠的血清 Mg2+ 浓度略低，但在雌性 Oit3-/- 小鼠中却观察不到这种影响。此外，Oit3-/-小鼠尿液中 Mg2+ 的排泄和肾脏促镁基因的表达也未发生变化。对于 12 个月和 18 个月的小鼠，QTL 分析显示其与 19 号染色体上的一个基因座有关，该基因座包含编码 TRPM6 的基因，TRPM6 是一种已知的 Mg2+ 通道，参与肾脏 Mg2+ 重吸收。与 RNAseq 数据比较发现，Trpm6 mRNA 表达与 QTL 效应成反比，这意味着 TRPM6 可能参与了小鼠尿 Mg2+ 排泄随年龄而发生的变化。总之，我们在此表明，Oit3和Trpm6的变异与生命中不同时期的尿Mg2+排泄有关，尽管OIT3不太可能影响肾脏的Mg2+处理。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Physiological genomics 生物-生理学

CiteScore

6.10

自引率

0.00%

发文量

审稿时长

4-8 weeks

期刊介绍： The Physiological Genomics publishes original papers, reviews and rapid reports in a wide area of research focused on uncovering the links between genes and physiology at all levels of biological organization. Articles on topics ranging from single genes to the whole genome and their links to the physiology of humans, any model organism, organ, tissue or cell are welcome. Areas of interest include complex polygenic traits preferably of importance to human health and gene-function relationships of disease processes. Specifically, the Journal has dedicated Sections focused on genome-wide association studies (GWAS) to function, cardiovascular, renal, metabolic and neurological systems, exercise physiology, pharmacogenomics, clinical, translational and genomics for precision medicine, comparative and statistical genomics and databases. For further details on research themes covered within these Sections, please refer to the descriptions given under each Section.