泛醌对糖尿病大鼠炎症、糖尿病肌病和内皮病变及CBC参数影响的研究

Yousif Jameel Jbrael, B. Hamad
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引用次数: 0

摘要

氧化应激和炎症与代谢紊乱(如糖尿病)的发展有关。糖尿病相关的氧化应激是由氧化自由基的过量产生引起的,这与炎症和组织损伤的机制有关。我们的研究旨在探讨泛醌治疗对氧化应激(丙二醛(MDA))、炎症(白细胞介素6 (IL-6))、血管稳态(一氧化氮(NO))和肌病(肌红蛋白(MB))血清指标的影响,并测量链脲霉素诱导的糖尿病大鼠的血液成分参数。大鼠分为三组;阴性对照组(N)、糖尿病对照组(D)和泛素治疗糖尿病组(T)。21 D后,取血、血清,测定空腹血糖(FBG)、丙二醛(MDA)、白细胞介素6 (IL-6)、NO、MB及血液学指标。高血糖大鼠FBG水平及血清IL-6、MDA、MB水平显著升高,NO水平显著降低。高血糖状态显著降低白细胞计数(P = 0.0098),但血小板和红细胞计数降低不显著。泛醌治疗显著降低糖尿病大鼠血糖、IL-6、MDA和MB水平,提高NO水平。泛醌对WBC (P = 0.648)、RBC (P = 0.001)和RBC (P = 0.398)的影响不显著,WBC和血小板水平变化较小。我们的数据支持,补充泛醌可以减少糖尿病大鼠的促炎、氧化应激和肌病标志物,并提高NO水平。目前的研究表明,泛醌可能对糖尿病并发症有积极影响;然而,需要进一步的研究来确定将其添加到标准糖尿病治疗中时的治疗效果。
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An Investigation into the Effects of Ubiquinone on Inflammation, Diabetic Myopathy and Endotheliopathy, and CBC Parameters in Diabetic Rats
Oxidative stress and inflammation are connected to the development of metabolic disorders, such as diabetes. Diabetic-related oxidative stress is caused by the overproduction of oxidative-free radicals, which have been implicated in the mechanism of inflammation and damage to tissues. Our study aimed to investigate the effects of ubiquinone treatment on serum indicators of oxidative stress (malondialdehyde (MDA)), inflammation (interleukin 6 (IL-6)), vascular homeostasis (nitric oxide (NO)), and myopathy (myoglobin (MB))  in addition to measuring blood components parameters in streptozotocin-induced diabetic rats. Rats were separated into three groups; negative control group (N), diabetic control group (D), and ubiquinone-treated diabetic group (T).  After 21 days, the blood and serum samples were taken to evaluate fasting blood glucose (FBG), MDA, IL-6, NO, MB, and hematological parameters. In hyperglycemic rats, the levels of FBG and serum levels of IL-6, MDA, and MB significantly increased, while NO levels decreased. Hyperglycemic condition significantly lowered the count of WBC (P = 0.0098) but insignificantly decreased values of platelets and RBC. Ubiquinone treatment significantly reduced blood glucose, IL-6, MDA, and MB levels in diabetic rats and raised NO levels. The effects of ubiquinone on WBC (P = 0.648), RBC (P = 0.001), and (P = 0.398) were insignificant,  and only minor variations in WBC and platelet levels were observed. Our data support that ubiquinone supplementation could reduce proinflammation, oxidative stress, and myopathy markers and elevate NO levels in diabetic rats. The current study indicates ubiquinone may positively impact diabetic complications; however, additional research is required to determine its therapeutic benefit when added to standard diabetes treatment.
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