Identifying biochemical changes in the kidney using proton nuclear magnetic resonance in an adenine diet chronic kidney disease mouse model.

IF 2.7 4区 医学 Q2 BIOPHYSICS NMR in Biomedicine Pub Date : 2024-09-04 DOI:10.1002/nbm.5257
Tyrone L R Humphries, Glenda C Gobe, Aaron J Urquhart, Robert J Ellis, Graham J Galloway, David A Vesey, Ross S Francis
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Abstract

This study aimed to investigate the metabolic changes in the kidneys in a murine adenine-diet model of chronic kidney disease (CKD). Kidney fibrosis is the common pathological manifestation across CKD aetiologies. Sustained inflammation and fibrosis cause changes in preferred energy metabolic pathways in the cells of the kidney. Kidney cortical tissue from mice receiving a control or adenine-supplemented diet for 8 weeks (late inflammation and fibrosis) and 12 weeks (8 weeks of treatment followed by 4 weeks recovery) were analysed by 2D-correlated nuclear magnetic resonance spectroscopy and compared with histopathology and biomarkers of kidney damage. Tissue metabolite and lipid levels were assessed using the MestreNova software. Expression of genes related to inflammation, fibrosis, and metabolism were measured using quantitative polymerase chain reaction. Animals showed indicators of severely impaired kidney function at 8 and 12 weeks. Significantly increased fibrosis was present at 8 weeks but not in the recovery group suggesting some reversal of fibrosis and amelioration of inflammation. At 8 weeks, metabolites associated with glycolysis were increased, while lipid signatures were decreased. Genes involved in fatty acid oxidation were decreased at 8 weeks but not 12 weeks while genes associated with glycolysis were significantly increased at 8 weeks but not at 12 weeks. In this murine model of CKD, kidney fibrosis was associated with the accumulation of triglyceride and free lactate. There was an up-regulation of glycolytic enzymes and down-regulation of lipolytic enzymes. These metabolic changes reflect the energy demands associated with progressive kidney disease where there is a switch from fatty acid oxidation to that of glycolysis.

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利用质子核磁共振识别腺嘌呤饮食慢性肾病小鼠模型中肾脏的生化变化。
本研究旨在探讨小鼠慢性肾脏病(CKD)腺嘌呤饮食模型中肾脏的代谢变化。肾脏纤维化是慢性肾脏病各种病因的共同病理表现。持续的炎症和纤维化会导致肾脏细胞首选的能量代谢途径发生变化。通过二维相关核磁共振波谱分析了接受对照组或腺嘌呤补充饮食 8 周(晚期炎症和纤维化)和 12 周(治疗 8 周后恢复 4 周)的小鼠肾皮质组织,并与组织病理学和肾损伤生物标志物进行了比较。组织代谢物和脂质水平使用 MestreNova 软件进行评估。使用定量聚合酶链反应测量了与炎症、纤维化和新陈代谢有关的基因表达。动物的肾功能在 8 周和 12 周时出现了严重受损的迹象。在 8 周时,纤维化明显加重,但在恢复组中没有出现这种情况,这表明纤维化在一定程度上发生了逆转,炎症也有所改善。8 周时,与糖酵解相关的代谢物增加,而脂质特征减少。参与脂肪酸氧化的基因在 8 周时减少,但在 12 周时没有减少,而与糖酵解相关的基因在 8 周时显著增加,但在 12 周时没有增加。在这种小鼠慢性肾脏病模型中,肾脏纤维化与甘油三酯和游离乳酸的积累有关。糖酵解酶上调,脂肪分解酶下调。这些代谢变化反映了进行性肾病对能量的需求,即从脂肪酸氧化转向糖酵解。
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来源期刊
NMR in Biomedicine
NMR in Biomedicine 医学-光谱学
CiteScore
6.00
自引率
10.30%
发文量
209
审稿时长
3-8 weeks
期刊介绍: NMR in Biomedicine is a journal devoted to the publication of original full-length papers, rapid communications and review articles describing the development of magnetic resonance spectroscopy or imaging methods or their use to investigate physiological, biochemical, biophysical or medical problems. Topics for submitted papers should be in one of the following general categories: (a) development of methods and instrumentation for MR of biological systems; (b) studies of normal or diseased organs, tissues or cells; (c) diagnosis or treatment of disease. Reports may cover work on patients or healthy human subjects, in vivo animal experiments, studies of isolated organs or cultured cells, analysis of tissue extracts, NMR theory, experimental techniques, or instrumentation.
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