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胡椒碱对环磷酰胺中毒大鼠海马和肝细胞中 DNA 双链断裂、氧化 DNA 损伤和细胞遗传毒性的改变特征。

Altered hallmarks of DNA double-strand breaks, oxidative DNA damage and cytogenotoxicity by piperlongumine in hippocampus and hepatocytes of rats intoxicated with cyclophosphamide.

机构信息

Neurobehavioral Pharmacology Laboratory, Department of Pharmacology, School of Pharmaceutical Education and Research, Jamia Hamdard, New Delhi 110062, India.

Department of Molecular Medicine, School of Interdisciplinary Science and Technology, Jamia Hamdard, New Delhi 110062, India.

出版信息

Life Sci. 2023 Mar 1;316:121391. doi: 10.1016/j.lfs.2023.121391. Epub 2023 Jan 16.

Abstract

AIM

Cyclophosphamide is an effective anti-tumor agent, however, it induces genomic instability and tissue toxicity in clinical application. This study aims to evaluate the action of piperlongumine against cyclophosphamide-induced toxicity.

MAIN METHODS

The action was investigated in rodent model of genomic instability, where piperlongumine (50 mg/kg) was orally co-administered with cyclophosphamide (5 mg/kg) for 28 days to Wistar albino rats. Further, piperlongumine was also examined for acute and sub-acute toxicity.

KEY FINDINGS

Piperlongumine significantly reversed genotoxicity in high-proliferation tissue (bone marrow: p < 0.05) as well as in vital tissues (hippocampus: p < 0.01 and hepatocytes: p < 0.05), calculated as micronuclei formation and %DNA fragmentation. It also restored the redox homeostasis, counteracted the formation of oxidative DNA damage product and DNA double-strand break in vital tissues, indicated by reduction of 8-OHdG and γH2AX. TUNEL assay revealed that piperlongumine diminished the cyclophosphamide-associated apoptotic cell death in hippocampus as well as in liver tissue and conferred cytoprotection to the host. These findings were finally corroborated with the histopathological findings, where piperlongumine treatment restored the cellular viability of liver and hippocampus. Further, piperlongumine did not produce any toxic effects to rats in systemic toxicity studies.

SIGNIFICANCE

Piperlongumine possesses genome stabilizing effect and reduces cyclophosphamide-associated DNA damage, oxidative stress, hepato-, and neurotoxicity, diminishes the DNA damage response pathway in the rat model, at the same time, conserves the micro-architectural details of liver and hippocampus. The findings are significant in terms of reducing genotoxic impact of chemotherapy-receiving patients.

摘要

目的

环磷酰胺是一种有效的抗肿瘤药物,但在临床应用中会引起基因组不稳定和组织毒性。本研究旨在评估胡椒碱对环磷酰胺诱导毒性的作用。

主要方法

在基因组不稳定的啮齿动物模型中研究了胡椒碱的作用,胡椒碱(50mg/kg)与环磷酰胺(5mg/kg)一起口服给药 28 天,用于 Wistar 白化大鼠。此外,还研究了胡椒碱的急性和亚急性毒性。

主要发现

胡椒碱显著逆转了高增殖组织(骨髓:p<0.05)和重要组织(海马:p<0.01 和肝细胞:p<0.05)中的遗传毒性,表现为微核形成和 DNA 片段化的百分比。它还恢复了氧化还原稳态,抵消了重要组织中氧化 DNA 损伤产物和 DNA 双链断裂的形成,这表现为 8-OHdG 和 γH2AX 的减少。TUNEL 分析表明,胡椒碱减少了海马和肝组织中环磷酰胺相关的细胞凋亡,并为宿主提供了细胞保护作用。这些发现最终与组织病理学发现一致,胡椒碱治疗恢复了肝和海马的细胞活力。此外,胡椒碱在全身毒性研究中对大鼠没有产生任何毒性作用。

意义

胡椒碱具有基因组稳定作用,可降低环磷酰胺相关的 DNA 损伤、氧化应激、肝毒性和神经毒性,减少 DNA 损伤反应途径在大鼠模型中的作用,同时保持肝和海马的微观结构细节。这些发现对于减少接受化疗患者的遗传毒性影响具有重要意义。

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