Dietary addition of magnesium hydride nanoparticles: a breakthrough in combating high-fat diet-induced chronic kidney disease.

IF 3 Q2 MEDICINE, RESEARCH & EXPERIMENTAL

Medical Gas Research Pub Date : 2025-09-01 Epub Date: 2025-04-17 DOI:10.4103/mgr.MEDGASRES-D-24-00090

Hongtao Lu, Wanqiu Chen, Yajing Ying, Deqian Gu, Rui Li, Xiangtong Li, Jin Cheng, Xuejun Sun, Yinyin Zhang, Wenrui Liu, Hui Shen

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Abstract

A substantial body of evidence indicates a positive correlation between dyslipidemia and an elevated risk of chronic kidney disease, with renal interstitial fibrosis frequently serving as a common pathway in the advanced stages of chronic kidney disease progression. Hydrogen has anti-inflammatory and antioxidant properties, and magnesium hydride nanoparticle is a material with high hydrogen storage capacity. Magnesium hydride -fortified feed is capable of releasing hydrogen gas steadily and continuously within the digestive tract. A 12-week high-fat diet significantly elevated the serum urea and creatinine levels in mice. In contrast, dietary addition of magnesium hydride demonstrated a notable protective effect against pathological conditions. Additionally, magnesium hydride -fortified feed was found to reduce renal fibrosis and thereby improve renal function. In support of these findings, an in vitro study utilizing human kidney cortical proximal tubule epithelial cells (HK-2 cells) exposed to palmitic acid under conditions mimicking a high-fat diet confirmed the renoprotective effects of magnesium hydride. Furthermore, the primary target phosphatase and tensin homologue deleted on chromosome 10 and the molecular mechanisms underlying the effects of magnesium hydride, specifically its ability to inhibit the transforming growth factor-beta -Smad family member 2 and 3 (Smad2/3) axis through downregulating the expression of phosphatase and tensin homologue deleted on chromosome 10, were elucidated. Additionally, overexpression of Hes family BHLH transcription factor 1 can negate the beneficial effects of magnesium hydride, suggesting that Hes family BHLH transcription factor 1 may serve as an upstream regulatory target in the context of the effects of magnesium hydride. In conclusion, this study demonstrated that magnesium hydride functions as a safe and effective hydrogen source capable of inhibiting the activation of the transforming growth factor-beta/Smad2/3 and protein kinase B/mechanistic target of rapamycin pathways by increasing the expression of phosphatase and tensin homologue deleted on chromosome 10. This mechanism counteracts the progression of high-fat diet-induced chronic renal damage.

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膳食中添加氢化镁纳米颗粒：对抗高脂肪饮食引起的慢性肾脏疾病的突破。

大量证据表明，血脂异常与慢性肾脏疾病风险升高之间存在正相关，肾间质纤维化通常是慢性肾脏疾病进展晚期的常见途径。氢具有抗炎和抗氧化的特性，氢化镁纳米颗粒是一种储氢能力高的材料。氢化镁强化饲料能够在消化道内稳定、持续地释放氢气。12周的高脂肪饮食显著提高了小鼠的血清尿素和肌酐水平。相反，饲料中添加氢化镁对病理状况有显著的保护作用。此外，氢化镁强化饲料可减少肾纤维化，从而改善肾功能。为了支持这些发现，一项利用人肾皮质近端小管上皮细胞（HK-2细胞）在模拟高脂肪饮食的条件下暴露于棕榈酸的体外研究证实了氢化镁的肾保护作用。此外，我们还阐明了10号染色体上缺失的主要目标磷酸酶和紧张素同源物以及氢化镁作用的分子机制，特别是其通过下调10号染色体上缺失的磷酸酶和紧张素同源物的表达来抑制转化生长因子- β -Smad家族成员2和3 （Smad2/3）轴的能力。此外，Hes家族BHLH转录因子1的过表达可以抵消氢氧化镁的有益作用，这表明Hes家族BHLH转录因子1可能是氢氧化镁作用背景下的上游调控靶点。综上所述，本研究表明，氢化镁作为一种安全有效的氢源，能够通过增加10号染色体上缺失的磷酸酶和紧张素同源物的表达，抑制雷帕霉素途径的转化生长因子- β /Smad2/3和蛋白激酶B/机制靶点的激活。这一机制抵消了高脂肪饮食引起的慢性肾损害的进展。

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来源期刊

Medical Gas Research MEDICINE, RESEARCH & EXPERIMENTAL-

CiteScore

5.10

自引率

13.80%

发文量

期刊介绍： Medical Gas Research is an open access journal which publishes basic, translational, and clinical research focusing on the neurobiology as well as multidisciplinary aspects of medical gas research and their applications to related disorders. The journal covers all areas of medical gas research, but also has several special sections. Authors can submit directly to these sections, whose peer-review process is overseen by our distinguished Section Editors: Inert gases - Edited by Xuejun Sun and Mark Coburn, Gasotransmitters - Edited by Atsunori Nakao and John Calvert, Oxygen and diving medicine - Edited by Daniel Rossignol and Ke Jian Liu, Anesthetic gases - Edited by Richard Applegate and Zhongcong Xie, Medical gas in other fields of biology - Edited by John Zhang. Medical gas is a large family including oxygen, hydrogen, carbon monoxide, carbon dioxide, nitrogen, xenon, hydrogen sulfide, nitrous oxide, carbon disulfide, argon, helium and other noble gases. These medical gases are used in multiple fields of clinical practice and basic science research including anesthesiology, hyperbaric oxygen medicine, diving medicine, internal medicine, emergency medicine, surgery, and many basic sciences disciplines such as physiology, pharmacology, biochemistry, microbiology and neurosciences. Due to the unique nature of medical gas practice, Medical Gas Research will serve as an information platform for educational and technological advances in the field of medical gas.