Attenuation of Experimental Cholesterol Gallstone Formation by Manganese Chloride in Mice: Role of NF-κβ Pathways.

IF 3.4 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Biological Trace Element Research Pub Date : 2025-08-01 Epub Date: 2024-12-23 DOI:10.1007/s12011-024-04467-z

A T Salami, J C Orji, U Akpamu, T O Iyiola, S B Olaleye

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Abstract

Manganese (Mn), a trace element, has been documented to exert an important role in the metabolism of cholesterol. Cholesterol gallstone (CG) pathogenesis is directly linked to biliary cholesterol imbalance which could be due to diabetes complications or mismanagement. NF-κβ pathway, an inflammatory regulator, has been implicated in metabolic disease especially in the context of diabetes and gallstone formation. However, the management of cholesterol gallstones due to diabetes with trace elements is vague. This study investigates the probable role of manganese during CG formation due to diabetes complications. Eighty female Swiss mice were grouped: I (control), II (untreated CG), III and IV (normal mice treated 0.37 mg/kg and 0.74 mg/kg Mn, respectively), V and VI (CG treated 0.37 mg/kg and 0.74 mg/kg Mn, respectively), and VII and VIII (CG treated 75 mg/7 kg and 350 mg/kg aspirin, respectively). Experimental CG was induced with cholesterol-rich diets after alloxan-induced diabetes. On sacrifice, blood collected was evaluated for complete hematological analysis and biochemistry while the excised liver was assayed for biochemical variables. Results were subjected to one-way ANOVA values were expressed as Mean ± SEM and significant at p ≤ 0.05. Manganese treatment significantly increased packed cell volume, RBC count, and hemoglobin with decreased platelet and leukocyte counts, liver enzymes (AST, ALT, and ALP), BUN, and creatinine levels in CG groups compared with untreated CG. Blood glucose, plasma low-density lipoproteins, and liver malodialdehyde levels were significantly reduced while liver nitric-oxide, sulfhydryl, and glutathione levels increased significantly in manganese-treated groups compared with untreated CG. Manganese significantly increased fecal iron contents in normal mice by the 2nd week. Hepatocytes and gallbladder histology appear normal in manganese-treated groups. Liver NF-Kβ immunoreactivity was downregulated in manganese-treated CG groups. Manganese attenuated experimental hyperglycemia-induced cholesterol gallstone by ameliorating liver oxidative stress and NF-Kβ inflammatory pathway.

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氯化锰对小鼠实验性胆固醇胆石形成的抑制作用：NF-κβ通路的作用。

锰（Mn）是一种微量元素，已被证明在胆固醇代谢中发挥重要作用。胆固醇胆结石（CG）的发病机制与胆道胆固醇失衡直接相关，而胆道胆固醇失衡可能是由于糖尿病并发症或管理不善所致。NF-κβ通路是一种炎症调节因子，与代谢性疾病，特别是糖尿病和胆结石形成有关。然而，用微量元素治疗糖尿病引起的胆固醇胆结石的方法尚不明确。本研究探讨了锰在糖尿病并发症引起的CG形成过程中的可能作用。80只雌性瑞士小鼠分为：I（对照组）、II（未服用CG）、III和IV（正常小鼠分别服用0.37 mg/kg和0.74 mg/kg Mn）、V和VI （CG分别服用0.37 mg/kg和0.74 mg/kg Mn）、VII和VIII （CG分别服用75 mg/7 kg和350 mg/kg阿司匹林）。四氧嘧啶诱导糖尿病后，高胆固醇饮食诱导实验性CG。在献祭时，采集的血液进行完整的血液学分析和生化分析，同时对切除的肝脏进行生化变量分析。结果进行单因素方差分析，以Mean±SEM表示，p≤0.05为显著性。与未处理的CG相比，锰处理显著增加了CG组的堆积细胞体积、红细胞计数和血红蛋白，降低了血小板和白细胞计数、肝酶（AST、ALT和ALP）、BUN和肌酐水平。与未处理的CG相比，锰处理组的血糖、血浆低密度脂蛋白和肝脏丙二醛水平显著降低，而肝脏一氧化氮、巯基和谷胱甘肽水平显著升高。到第二周，锰显著增加了正常小鼠的粪便铁含量。锰处理组肝细胞和胆囊组织学表现正常。锰处理的CG组肝脏NF-Kβ免疫反应性下调。锰通过改善肝脏氧化应激和NF-Kβ炎症途径减轻实验性高血糖诱导的胆固醇胆结石。

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

Biological Trace Element Research 生物-内分泌学与代谢

CiteScore

8.70

自引率

10.30%

发文量

459

审稿时长

2 months

期刊介绍： Biological Trace Element Research provides a much-needed central forum for the emergent, interdisciplinary field of research on the biological, environmental, and biomedical roles of trace elements. Rather than confine itself to biochemistry, the journal emphasizes the integrative aspects of trace metal research in all appropriate fields, publishing human and animal nutritional studies devoted to the fundamental chemistry and biochemistry at issue as well as to the elucidation of the relevant aspects of preventive medicine, epidemiology, clinical chemistry, agriculture, endocrinology, animal science, pharmacology, microbiology, toxicology, virology, marine biology, sensory physiology, developmental biology, and related fields.