Ameliorative effect of lixisenatide on diabetic cardiovascular damage and its enhancement via ticagrelor co-administration in rats: possible role of eNOS and NrF₂ /HO-1 signaling.

IF 1.5 4区 医学 Q4 CHEMISTRY, MEDICINAL Pharmazie Pub Date : 2024-06-01 DOI:10.1691/ph.2024.4509
M Sleem, E M Aboubakr, W R Mohamed, B A S Messiha, A Taye
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Abstract

In this study, we hypothesized that lixisenatide (LIX) and ticagrelor (TIC) could have a protective effect against type 2 diabetes mellitus (T2DM)-induced vascular damage. Furthermore, we explored the possible additional protective effect of co-administering LIX and TIC in the treatment regimen. Methods: 50 male rats were divided into five groups, each comprising 10 rats: C (control), D (T2DM rats), D + LIX (T2DM rats treated with LIX for 4 weeks), D + TIC (T2DM rats treated with TIC for 4 weeks), and D + LIX + TIC (T2DM rats treated with LIX + TIC for 4 weeks). Results: The D group showed an increase in body weight, blood glucose, hemostatic model assessment for insulin resistance (HOMA-IR), aorta reactive oxygen species (ROS), and nuclear factor kappa B (NF-κ B), along with a reduction in serum insulin, aorta superoxide dismutase (SOD), glutathione reduced (GSH), nuclear factor erythroid-2 (NrF₂), hemeoxygenase-1 (HO-1), and endothelial nitric oxide synthase (eNOS). Deterioration in the aorta histopathological condition, coupled with a noticeable impairment in vascular reactivity compared to the C group, was observed. A single administration of LIX showed a reduction in body weight, blood glucose, HOMA-IR, aorta ROS, and NF-κ B, accompanied by an increase in serum insulin, aorta SOD, GSH, NrF₂, HO-1, and eNOS. Amelioration in the aorta histopathological condition and improved vascular reactivity compared to the D group were reported. Similarly, a single administration of TIC showed a reduction in aorta ROS and NF-κ B, along with an increase in aorta SOD, GSH, NrF₂, HO-1, and eNOS. A slight amelioration was detected in the aorta histopathological condition, with improved vascular reactivity compared to the D group. The combined administration of LIX and TIC showed a reduction in aorta ROS and NF-κ B, along with an increase in aorta GSH, SOD, HO-1, and eNOS. This was combined with evident amelioration in the aorta histopathological condition and noticeable improvement in vascular reactivity compared to the single treatment with either LIX or TIC group. Conclusion: The present study introduces clear evidence that the administration of LIX and TIC can improve metabolic and vascular complications of T2DM through modulating eNOS and NrF₂ /HO-1 signaling. The combined administration of LIX and TIC produced more significant effects than a single treatment.

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利血那肽对糖尿病大鼠心血管损伤的改善作用及其通过联合应用替卡格雷而增强的效果:eNOS 和 NrF₂ /HO-1 信号传导的可能作用。
在这项研究中,我们假设利塞那肽(LIX)和替卡格雷罗(TIC)对 2 型糖尿病(T2DM)诱发的血管损伤具有保护作用。此外,我们还探讨了在治疗方案中联合使用骊(LIX)和替卡格雷(TIC)可能产生的额外保护作用。方法:将 50 只雄性大鼠分为 5 组,每组 10 只:C(对照组)、D(T2DM 大鼠)、D + LIX(T2DM 大鼠接受 LIX 治疗 4 周)、D + TIC(T2DM 大鼠接受 TIC 治疗 4 周)和 D + LIX + TIC(T2DM 大鼠接受 LIX + TIC 治疗 4 周)。结果D 组大鼠的体重、血糖、胰岛素抵抗止血模型评估(HOMA-IR)、主动脉活性氧(ROS)和核因子卡巴 B(NF-κ B)均有所增加、同时,血清胰岛素、主动脉超氧化物歧化酶(SOD)、谷胱甘肽还原酶(GSH)、核因子红细胞-2(NrF₂)、血红素氧化酶-1(HO-1)和内皮一氧化氮合酶(eNOS)也有所减少。与 C 组相比,观察到主动脉组织病理学状况恶化,血管反应性明显减弱。单次服用骊骊可降低体重、血糖、HOMA-IR、主动脉 ROS 和 NF-κ B,同时增加血清胰岛素、主动脉 SOD、GSH、NrF₂、HO-1 和 eNOS。与 D 组相比,主动脉组织病理学状况有所改善,血管反应性也有所提高。同样,单次给药 TIC 可减少主动脉 ROS 和 NF-κ B,同时增加主动脉 SOD、GSH、NrF₂、HO-1 和 eNOS。与 D 组相比,主动脉组织病理学状况略有改善,血管反应性有所提高。联合服用骊骊和 TIC 可降低主动脉 ROS 和 NF-κ B,同时增加主动脉 GSH、SOD、HO-1 和 eNOS。与单用骊蛇或 TIC 治疗组相比,主动脉组织病理学状况明显改善,血管反应性明显改善。结论:本研究提供了明确的证据,证明服用骊骊和 TIC 可通过调节 eNOS 和 NrF₂ /HO-1 信号,改善 T2DM 的代谢和血管并发症。与单一治疗相比,联合服用骊骊和 TIC 产生的效果更为显著。
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来源期刊
Pharmazie
Pharmazie 医学-化学综合
CiteScore
3.10
自引率
0.00%
发文量
56
审稿时长
1.2 months
期刊介绍: The journal DiePharmazie publishs reviews, experimental studies, letters to the editor, as well as book reviews. The following fields of pharmacy are covered: Pharmaceutical and medicinal chemistry; Pharmaceutical analysis and drug control; Pharmaceutical technolgy; Biopharmacy (biopharmaceutics, pharmacokinetics, biotransformation); Experimental and clinical pharmacology; Pharmaceutical biology (pharmacognosy); Clinical pharmacy; History of pharmacy.
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