Platelet-Rich Plasma (PRP) Mitigates Kidney Dysfunction in Alloxan-Induced Diabetic Mice via Modulation of Renal Iron Regulatory Genes.

IF 2.1 4区 生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Biochemical Genetics Pub Date : 2024-07-26 DOI:10.1007/s10528-024-10871-w
Humaira Allay Ali, Muddasir Hassan Abbasi, Tasleem Akhtar, Amin Arif, Mehreen Anjum, Sana Fatima, Rabia Mehmood, Adil Farooq, Nadeem Sheikh, Muhammad Babar Khawar
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Abstract

Kidney dysfunction is a prevalent complication of diabetes mellitus, contributing significantly to diabetes-related morbidity and mortality. We aim to explore whether platelet-rich plasma administration can modulate iron regulation mechanism within the kidney, thereby mitigating renal dysfunction associated with diabetes. Albino mice with an average body weight of 20 ± 5 g were randomly divided into five groups (N = 50; n = 10): Control Group, PRP Group, diabetic group (DG), treated group A (TA), and treated group B (TB). A single intraperitoneal dose of alloxan (160 mg/kg of body weight) was administered to mice in the DG and in both treated groups. Upon confirmation of diabetes, the DG was left untreated, while PRP treatment (0.5 ml/kg of body weight) was administered to the TA and TB groups for two and four weeks, respectively. Histological examinations of kidney tissues revealed notable signs of damage in DG, which were subsequently improved upon PRP treatment. Likewise, PRP treatment restored the changes in liver enzymes, oxidative stress biomarkers and serum electrolytes in both treated groups. Furthermore, there was an observed upregulation of iron regulatory genes, such as Renin, Epo, Hepc, Kim1, and Hfe, in the DG, accompanied by a downregulation of Tfr1 and Fpn; however, Dmt1 and Dcytb1 expression remained unaltered. Treatment with PRP restored the expression of iron regulatory genes in both treated groups. This study concluded that PRP treatment effectively restored the renal histochemistry and the expression of renal iron regulatory genes in an alloxan-induced diabetic mice model.

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富血小板血浆 (PRP) 通过调节肾脏铁调节基因缓解阿脲诱导糖尿病小鼠的肾功能障碍
肾功能障碍是糖尿病的一种常见并发症,严重影响糖尿病相关疾病的发病率和死亡率。我们的目的是探讨给予富血小板血浆是否能调节肾脏内的铁调节机制,从而缓解与糖尿病相关的肾功能障碍。将平均体重为 20±5 克的白化小鼠随机分为五组(N = 50;n = 10):对照组、PRP 组、糖尿病组(DG)、治疗 A 组(TA)和治疗 B 组(TB)。给糖尿病组和治疗组的小鼠腹腔注射单剂量阿脲(160 毫克/千克体重)。确认糖尿病后,DG 组不进行治疗,而 TA 组和 TB 组则分别进行为期两周和四周的 PRP 治疗(0.5 毫升/千克体重)。肾组织的组织学检查显示,DG 有明显的损伤迹象,PRP 治疗后症状得到改善。同样,PRP 治疗也恢复了两个治疗组的肝酶、氧化应激生物标志物和血清电解质的变化。此外,在 DG 中观察到铁调控基因(如 Renin、Epo、Hepc、Kim1 和 Hfe)上调,同时 Tfr1 和 Fpn 下调;但 Dmt1 和 Dcytb1 的表达保持不变。使用 PRP 治疗可恢复两组铁调控基因的表达。本研究的结论是,PRP 治疗可有效恢复阿脲诱导的糖尿病小鼠模型的肾脏组织化学和肾脏铁调节基因的表达。
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来源期刊
Biochemical Genetics
Biochemical Genetics 生物-生化与分子生物学
CiteScore
3.90
自引率
0.00%
发文量
133
审稿时长
4.8 months
期刊介绍: Biochemical Genetics welcomes original manuscripts that address and test clear scientific hypotheses, are directed to a broad scientific audience, and clearly contribute to the advancement of the field through the use of sound sampling or experimental design, reliable analytical methodologies and robust statistical analyses. Although studies focusing on particular regions and target organisms are welcome, it is not the journal’s goal to publish essentially descriptive studies that provide results with narrow applicability, or are based on very small samples or pseudoreplication. Rather, Biochemical Genetics welcomes review articles that go beyond summarizing previous publications and create added value through the systematic analysis and critique of the current state of knowledge or by conducting meta-analyses. Methodological articles are also within the scope of Biological Genetics, particularly when new laboratory techniques or computational approaches are fully described and thoroughly compared with the existing benchmark methods. Biochemical Genetics welcomes articles on the following topics: Genomics; Proteomics; Population genetics; Phylogenetics; Metagenomics; Microbial genetics; Genetics and evolution of wild and cultivated plants; Animal genetics and evolution; Human genetics and evolution; Genetic disorders; Genetic markers of diseases; Gene technology and therapy; Experimental and analytical methods; Statistical and computational methods.
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