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槲皮素纳米颗粒对吡虫啉诱导的瑞士白化小鼠亚急性遗传毒性和组织病理学改变的改善潜力研究。

Studies on ameliorative potentials of quercetin nanoparticles against imidacloprid induced subacute genotoxicity and histopathological alteration in Swiss albino mice.

作者信息

Bagri Preeti, Bhardwaj Kajal, Kant Vinay, Lather Deepika

机构信息

Department of Veterinary Pharmacology and Toxicology, College of Veterinary Sciences, Lala Lajpat Rai University of Veterinary and Animal Sciences, Hisar, India.

Department of Veterinary Pathology, College of Veterinary Sciences, Lala Lajpat Rai University of Veterinary and Animal Sciences, Hisar, India.

出版信息

Drug Dev Ind Pharm. 2025 Jan;51(1):77-90. doi: 10.1080/03639045.2024.2447872. Epub 2025 Jan 3.

Abstract

OBJECTIVE

Genotoxicity assays include micronucleus test, comet assay, and malformed sperm head used to investigate the protective potential of quercetin (Que) and Que nanoparticles against imidacloprid (IMI)-induced genotoxicity in Swiss albino mice.

METHODS

The ionic gelation procedure was used to synthesize the Que nanoparticles and characterized for their hydrodynamic diameter, zeta potential, scanning electron microscopy (SEM), transmission electron microscopy (TEM), FT-IR, and encapsulation efficiency. A total of 48 mice were taken in eight groups with six animals in each group. Groups 1, 2, 3, and 4 received 3% gum acacia, 22 mg/kg IMI, 25 mg/kg Que and 25 mg/kg Que nanoparticles high dose (QNPs (HD)), respectively. Groups 5, 6, 7, and 8 received 22 mg/kg IMI + 25 mg/kg Que (IMI + Que), 22 mg/kg IMI + 25 mg/kg Que nanoparticles (IMI + QNPs (HD)), 22 mg/kg IMI + 12.5 mg/kg Que nanoparticle medium dose (IMI + QNPs (MD)), and 22 mg/kg IMI + 6.25 mg/kg Que nanoparticles low dose (IMI + QNPs (LD)), respectively.

RESULTS

The IMI causes genotoxicity in bone marrow cells by increasing the frequency of micronuclei and the comet tail length. Additionally, IMI is mutagenic to germ cells, as determined by a test for aberrant sperm heads. Both Que and Que nanoparticles lessen the genotoxicity that IMI induces when administered together or separately. Histopathological findings also revealed degenerative changes in bone marrow and testes in IMI administered group as compared to control.

CONCLUSION

Quercetin and Que nanoparticles showed marked ameliorative effect by restoring the degenerative changes produced by IMI.

摘要

目的

遗传毒性试验包括微核试验、彗星试验和畸形精子头试验,用于研究槲皮素(Que)和槲皮素纳米颗粒对吡虫啉(IMI)诱导的瑞士白化小鼠遗传毒性的保护潜力。

方法

采用离子凝胶法合成槲皮素纳米颗粒,并对其流体动力学直径、zeta电位、扫描电子显微镜(SEM)、透射电子显微镜(TEM)、傅里叶变换红外光谱(FT-IR)和包封率进行表征。总共48只小鼠分为八组,每组6只动物。第1、2、3和4组分别接受3%阿拉伯胶、22毫克/千克IMI、25毫克/千克Que和25毫克/千克槲皮素纳米颗粒高剂量(QNPs(HD))。第5、6、7和8组分别接受22毫克/千克IMI + 25毫克/千克Que(IMI + Que)、22毫克/千克IMI + 25毫克/千克槲皮素纳米颗粒(IMI + QNPs(HD))、22毫克/千克IMI + 12.5毫克/千克槲皮素纳米颗粒中剂量(IMI + QNPs(MD))和22毫克/千克IMI + 6.25毫克/千克槲皮素纳米颗粒低剂量(IMI + QNPs(LD))。

结果

IMI通过增加微核频率和彗星尾长导致骨髓细胞遗传毒性。此外,通过异常精子头试验确定,IMI对生殖细胞具有致突变性。Que和槲皮素纳米颗粒无论是一起给药还是单独给药,都能减轻IMI诱导的遗传毒性。组织病理学结果还显示,与对照组相比,IMI给药组的骨髓和睾丸出现退行性变化。

结论

槲皮素和槲皮素纳米颗粒通过恢复IMI产生 的退行性变化显示出显著的改善作用。

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