Evaluation of Conophor Nut (Tetracarpidium conophorum) Protein Isolates, Hydrolysate and Ethanolic Extract Ameliorating Potential on Hepatological and Renal Dysfunction of Streptozocin-induced Diabetic Wistar Rats

Olubukola Yinka Odekunle, O. Ijarotimi, I. Oluwalana
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Abstract

Aim: This study aimed at extracting bioactive components from conophor nut as a probable nutraceutic in the treatment of diabetes. Place and Duration: Food Chemistry Laboratory, Department of Food Science and Technology, and Biochemistry Laboratory of the Federal University of Technology, Akure, from June 2023 to September 2023. Methodology: Protein isolate (CNPI) was produced via alkaline solubilisation of defatted conophor nut flour using NaOH. Hydrolysate was prepared by fermentation using Lactobacillus fermentum BGT10 for 24, 48 and 72 hours (CNPH24, CNPH48, CNPH72) respectively while the ethanolic extract (CNE) was prepared by steeping defatted conophor nut flour in 95% ethanol. Diabetic model rats were subjected to hyperlipidemic diet for 4 weeks and then induced by single intraperitoneal injection of freshly prepared solution of streptozotocin (35 mg/kg). The rats were randomly divided into 18 groups of five (5) rats each; negative control group, diabetic control group, reference (positive) control group as well as the treatment group; CNE, CNPH24, CNPH48, CNPH72 and CNPI administered dose dependently namely, 250, 500 and 1000 mg/kg body weight. Oxidative stress was evaluated in liver and kidney by antioxidant markers, and also kidney functions were determined in diabetic control and treated rats. Results: When compared with diabetic rats, oral administration of treatments at a concentration of 1000 mg/kg daily for 28 days showed significant reduction in biochemical parameters of liver and kidney for CNE, CNPH24, CNPH48, CNPH72 and CNPI respectively. Furthermore, the treatment resulted in significant increase in SOD, GSH, GST and CAT and decrease in MDA in the liver and kidney respectively. Conclusion: Results from the study suggest that CNE, CNPH24, CNPH48, CNPH72 and CNPI may effectively normalize dysfunctional antioxidant status in streptozotocin-induced diabetics in a dose-dependent manner.
评估芋螺果仁(Tetracarpidium conophorum)蛋白分离物、水解物和乙醇提取物对链脲佐辛诱导的糖尿病 Wistar 大鼠肝肾功能障碍的改善潜力
目的:本研究旨在从锥栗中提取生物活性成分,作为治疗糖尿病的一种可能的营养保健品。地点和时间:2023 年 6 月至 2023 年 9 月,阿库雷联邦理工大学食品科学与技术系食品化学实验室和生物化学实验室。研究方法:蛋白质分离物(CNPI)是通过使用 NaOH 碱溶解脱脂锥栗果粉生产的。水解物通过使用乳酸杆菌发酵体 BGT10 发酵 24、48 和 72 小时分别制备(CNPH24、CNPH48、CNPH72),乙醇提取物(CNE)通过将脱脂锥栗果粉浸泡在 95% 的乙醇中制备。对糖尿病模型大鼠进行为期 4 周的高脂血症饮食,然后向其腹腔内注射新鲜制备的链脲佐菌素溶液(35 毫克/千克)。大鼠被随机分为 18 组,每组 5 只;阴性对照组、糖尿病对照组、参照(阳性)对照组和治疗组;CNE、CNPH24、CNPH48、CNPH72 和 CNPI 的给药剂量分别为 250、500 和 1000 毫克/千克体重。通过抗氧化标记物评估肝脏和肾脏的氧化应激,同时测定糖尿病对照组和治疗组大鼠的肾功能。结果与糖尿病大鼠相比,连续 28 天每天口服 1000 毫克/千克浓度的 CNE、CNPH24、CNPH48、CNPH72 和 CNPI 处理剂可显著降低肝脏和肾脏的生化指标。此外,治疗还导致肝脏和肾脏中的 SOD、GSH、GST 和 CAT 显著增加,MDA 下降。结论研究结果表明,CNE、CNPH24、CNPH48、CNPH72 和 CNPI 可有效改善链脲佐菌素诱导的糖尿病患者的抗氧化功能障碍,且具有剂量依赖性。
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