Effective-Component Compatibility of Bufei Yishen Formula III Suppresses Mitochondrial Oxidative Damage in COPD: Via Pkm2/Nrf2 Pathway.

IF 2.7 3区 医学 Q2 RESPIRATORY SYSTEM
Yang Liu, Lanxi Zhang, Jie Zhao, Ruilong Lu, Xuejie Shao, Kexin Xu, Jiansheng Li, Yange Tian
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Abstract

Purpose: The main objective of this study was to explore the mechanism of effective component compatibility of Bufei Yishen formula III (ECC-BYF III) in inhibiting mitochondrial oxidative stress in a rat model of chronic obstructive pulmonary disease (COPD).

Methods: A549 cells exposed to cigarette smoke extract (CSE) were used to establish a model of mitochondrial oxidative damage. The cells were treated with the plasmid encoding Pkm2 and the enzymes and proteins involved in oxidative stress and mitochondrial function were measured. A rat model of COPD was established using CS and bacteria. Two different treatments were established, ECC-BYF III (5.5 mg/kg/d) and N-acetylcysteine (54 mg/kg/day). Animals were tested for pulmonary function (Vt, PEF, FVC, FEV0.1s and Cdyn) after eight weeks of therapy and were sacrificed. Pulmonary H&E staining was performed, and the total superoxide dismutase (T-SOD), glutathione peroxidase (GSH-Px), total antioxidant capacity (T-AOC), and malondialdehyde (MDA) content were measured. The mitochondrial function was also examined. Furthermore, the Pkm2/Nrf2 signaling pathway was evaluated.

Results: Overexpression of Pkm2 dramatically ameliorated the CS-induced mitochondrial oxidative damage. Further studies indicated that ECC-BYF III significantly improved mitochondrial function and inhibited oxidative stress in the lung tissues of COPD rats. Moreover, it can upregulate mitochondrial respiratory chain enzyme activity. ECC-BYF III also decreased the MDA content and increased T-SOD, GSH-Px, and T-AOC expression to facilitate oxidative homeostasis. Finally, our results indicated that the Pkm2/Nrf2 pathway is regulated by ECC-BYF III in A549 cells and lung tissue.

Conclusion: These results indicate that ECC-BYF III exerts a strong effective therapeutic effect against cigarette smoke combined with bacteria-induced COPD in rats by activating the Pkm2/Nrf2 signaling pathway and restoring mitochondrial oxidative stress. Although more in vivo animal model research is needed to confirm these findings, this study contributes new data to support the conventional usage of ECC-BYF III.

有效成分复方布非益生方Ⅲ通过Pkm2/Nrf2途径抑制慢性阻塞性肺病线粒体氧化损伤
目的:本研究的主要目的是探讨布非益生方Ⅲ(ECC-BYFⅢ)在慢性阻塞性肺疾病(COPD)大鼠模型中抑制线粒体氧化应激的有效成分相容性机制:方法:用暴露于香烟烟雾提取物(CSE)的 A549 细胞建立线粒体氧化损伤模型。用编码 Pkm2 的质粒处理细胞,测量参与氧化应激和线粒体功能的酶和蛋白质。利用 CS 和细菌建立了慢性阻塞性肺病大鼠模型。建立了两种不同的治疗方法:ECC-BYF III(5.5 毫克/千克/天)和 N-乙酰半胱氨酸(54 毫克/千克/天)。治疗八周后,对动物进行肺功能测试(Vt、PEF、FVC、FEV0.1s 和 Cdyn)并将其处死。进行肺部 H&E 染色,并测量总超氧化物歧化酶(T-SOD)、谷胱甘肽过氧化物酶(GSH-Px)、总抗氧化能力(T-AOC)和丙二醛(MDA)含量。还对线粒体功能进行了检测。此外,还评估了 Pkm2/Nrf2 信号通路:结果:过表达 Pkm2 能显著改善 CS 诱导的线粒体氧化损伤。进一步的研究表明,ECC-BYF III 能显著改善 COPD 大鼠肺组织的线粒体功能,抑制氧化应激。此外,它还能提高线粒体呼吸链酶的活性。ECC-BYF III 还能降低 MDA 含量,增加 T-SOD、GSH-Px 和 T-AOC 的表达,从而促进氧化平衡。最后,我们的研究结果表明,在 A549 细胞和肺组织中,Pkm2/Nrf2 通路受到 ECC-BYF III 的调控:这些结果表明,ECC-BYF III 通过激活 Pkm2/Nrf2 信号通路和恢复线粒体氧化应激,对香烟烟雾和细菌诱导的大鼠慢性阻塞性肺病有很强的治疗效果。尽管还需要更多的体内动物模型研究来证实这些发现,但本研究为支持 ECC-BYF III 的常规用法提供了新的数据。
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
CiteScore
4.80
自引率
10.70%
发文量
372
审稿时长
16 weeks
期刊介绍: An international, peer-reviewed journal of therapeutics and pharmacology focusing on concise rapid reporting of clinical studies and reviews in COPD. Special focus will be given to the pathophysiological processes underlying the disease, intervention programs, patient focused education, and self management protocols. This journal is directed at specialists and healthcare professionals
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