Hepatoprotective effect of flavonoid rich fraction of Sesbania grandiflora: Results of In vivo, in vitro, and molecular docking studies

IF 1.7 Q3 INTEGRATIVE & COMPLEMENTARY MEDICINE
Anitha Kuttiappan , Santenna Chenchula , Murugesan Vanangamudi , Shvetank Bhatt , Radhika Chikatipalli , P Shaila Bhanu , Nagaraju Bandaru
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引用次数: 0

Abstract

Background

Phytochemicals and their derivatives are promising target drugs for various ailments and have served as therapeutic agents for several decades. Using in vivo and in vitro models and molecular docking, this study investigated the pharmacological potential of a flavonoid-rich fraction of the ethanolic extract of Sesbania grandiflora (SG).

Objectives

This research aimed to determine whether flavonoid-rich whole-plant extracts of SGs have any cytoprotective or in vivo hepatoprotective effects. Additionally, the study was intended to elucidate the molecular connections between the discovered flavonoid flavonols and PPARα target proteins linked to liver problems, for which an in silico molecular docking investigation was performed.

Materials and methods

To separate the flavonoid components, the entire Sesbania grandiflora plant was first extracted using ethanol as a solvent by soxhlet extraction. The resulting ethanolic extract was then fractionated. The cytoprotective and hepatoprotective properties were evaluated via in vitro and in vivo experiments. SGOT, SGPT, triglyceride, bilirubin, and total protein levels were used to evaluate hepatotoxicity in animal models. In vitro studies on Hepatocellular Carcinoma G2 (HepG2) cell lines have examined their cytotoxic effects and antioxidant activity. The most promising flavonoid-flavanol compounds were identified by conducting molecular docking studies against PPARα target protein (PDB ID: 3VI8) using MOE software.

Results

In vivo, the serum levels of SGOT, SGPT, total triglyceride and total bilirubin were measured in experimental animals treated with the flavonoid-rich ethanolic extract of SG. Significant reductions in the levels of these hepatic injury markers were observed, indicating the hepatoprotective potential of the extract. Elevated levels of liver biomarkers in the untreated group indicated liver injury or dysfunction. The treated groups showed significant restoration of these biomarkers, suggesting the hepatoprotective potential of SG. The IC50 value for the total flavonoid content of SG was 190.28 μg/ml, indicating its safety in inhibiting HepG2 cell growth. Flavonoid treatment decreased cell viability but did not affect antioxidant parameters in hepatocytes. In addition, SG restored the damaged hepatocyte architecture. Molecular docking studies revealed the binding affinities of flavonoids for PPARα. These findings suggest that a promising lead candidate for the development of therapeutic medicines against anti-TB drug-induced hepatotoxicity has been identified.

Conclusion

Our findings demonstrate the hepatoprotective potential of the flavonoid-rich fraction of Sesbania grandiflora both in vivo and in vitro. This study provides valuable insights into its mechanism of action, highlighting its promising therapeutic application in the management of liver disorders. This study highlights the hepatoprotective and cytoprotective potential of the total flavonoid-rich fraction of SG.

大叶芝麻富含黄酮类成分的肝保护作用:体内、体外和分子对接研究的结果。
背景:几十年来,植物化学物质及其衍生物一直是治疗各种疾病的有前途的靶向药物。本研究利用体内和体外模型以及分子对接,研究了大叶芝麻(SG)乙醇提取物中富含黄酮类成分的药理潜力:本研究旨在确定富含黄酮类化合物的 SG 全植物提取物是否具有细胞保护或体内肝脏保护作用。此外,该研究还旨在阐明已发现的类黄酮黄酮醇与与肝脏问题有关的 PPARα 靶蛋白之间的分子联系,并为此进行了硅学分子对接调查:为了分离黄酮类成分,首先使用乙醇作为溶剂,通过索氏提取法提取整株大叶芝麻。然后对得到的乙醇提取物进行分馏。通过体外和体内实验对其细胞保护和肝脏保护特性进行了评估。采用 SGOT、SGPT、甘油三酯、胆红素和总蛋白水平来评估动物模型的肝毒性。对肝细胞癌 G2(HepG2)细胞系进行的体外研究检验了它们的细胞毒性作用和抗氧化活性。通过使用 MOE 软件对 PPARα 靶蛋白(PDB ID:3VI8)进行分子对接研究,确定了最有前景的黄酮-黄烷醇化合物:用富含黄酮的 SG 乙醇提取物对实验动物进行体内血清 SGOT、SGPT、总甘油三酯和总胆红素水平的测定。结果表明,这些肝损伤标志物的水平明显降低,表明萃取物具有保护肝脏的潜力。未处理组的肝脏生物标志物水平升高表明肝脏损伤或功能障碍。治疗组的这些生物标志物水平明显恢复,表明 SG 具有保护肝脏的潜力。SG 总黄酮含量的 IC50 值为 190.28 μg/ml,表明其在抑制 HepG2 细胞生长方面具有安全性。类黄酮处理可降低细胞活力,但不会影响肝细胞的抗氧化参数。此外,SG 还能恢复受损的肝细胞结构。分子对接研究揭示了类黄酮与 PPARα 的结合亲和力。这些研究结果表明,我们已经找到了一种很有希望的候选药物,可用于开发抗结核药物引起的肝毒性的治疗药物:我们的研究结果表明,富含黄酮类成分的大叶芝麻在体内和体外都具有保肝潜力。这项研究对其作用机制提供了宝贵的见解,突出了其在治疗肝脏疾病方面的应用前景。本研究强调了五加科植物总黄酮富集部分的保肝和细胞保护潜力。
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
Journal of Ayurveda and Integrative Medicine
Journal of Ayurveda and Integrative Medicine INTEGRATIVE & COMPLEMENTARY MEDICINE-
CiteScore
4.70
自引率
12.50%
发文量
136
审稿时长
30 weeks
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