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银纳米颗粒在乳腺癌小鼠模型中诱导DNA甲基化和组蛋白H3甲基化的变化。

Silver Nanoparticles Induced Changes in DNA Methylation and Histone H3 Methylation in a Mouse Model of Breast Cancer.

作者信息

Brzóska Kamil, Sochanowicz Barbara, Szczygieł Małgorzata, Drzał Agnieszka, Śniegocka Martyna, Michalczyk-Wetula Dominika, Elas Martyna, Kapka-Skrzypczak Lucyna, Kruszewski Marcin

机构信息

Centre for Radiobiology and Biological Dosimetry, Institute of Nuclear Chemistry and Technology, Dorodna 16, 03-195 Warsaw, Poland.

Department of Biophysics and Cancer Biology, Faculty of Biochemistry, Biophysics and Biotechnology, Jagiellonian University, Gronostajowa 7, 30-387 Cracow, Poland.

出版信息

Materials (Basel). 2023 Jun 2;16(11):4163. doi: 10.3390/ma16114163.

Abstract

The importance of epigenetic changes as a measurable endpoint in nanotoxicological studies is getting more and more appreciated. In the present work, we analyzed the epigenetic effects induced by citrate- and PEG-coated 20 nm silver nanoparticles (AgNPs) in a model consisting of 4T1 breast cancer tumors in mice. Animals were administered with AgNPs intragastrically (1 mg/kg b.w. daily-total dose 14 mg/kg b.w.) or intravenously (administration twice with 1 mg/kg b.w.-total dose 2 mg/kg b.w.). We observed a significant decrease in 5-methylcytosine (5-mC) level in tumors from mice treated with citrate-coated AgNPs regardless of the route of administration. For PEG-coated AgNPs, a significant decrease in DNA methylation was observed only after intravenous administration. Moreover, treatment of 4T1 tumor-bearing mice with AgNPs decreased histone H3 methylation in tumor tissue. This effect was the most pronounced for PEG-coated AgNPs administered intravenously. No changes in histone H3 Lys9 acetylation were observed. The decrease in methylation of DNA and histone H3 was accompanied by changes in expression of genes encoding chromatin-modifying enzymes (Setd4, Setdb1, Smyd3, Suv39h1, Suv420h1, Whsc1, Kdm1a, Kdm5b, Esco2, Hat1, Myst3, Hdac5, Dnmt1, Ube2b, and Usp22) and genes related to carcinogenesis (Akt1, Brca1, Brca2, Mlh1, Myb, Ccnd1, and Src). The significance of the observed changes and the mechanisms responsible for their development are unclear, and more research in this area is warranted. Nevertheless, the present work points to the epigenetic effects as an important level of interaction between nanomaterials and biological systems, which should always be taken into consideration during analysis of the biological activity of nanomaterials and development of nanopharmaceuticals.

摘要

表观遗传变化作为纳米毒理学研究中一个可测量的终点的重要性正越来越受到重视。在本研究中,我们分析了柠檬酸盐和聚乙二醇包覆的20纳米银纳米颗粒(AgNPs)在小鼠4T1乳腺癌肿瘤模型中诱导的表观遗传效应。动物通过胃内给予AgNPs(1毫克/千克体重,每日 - 总剂量14毫克/千克体重)或静脉内给予(分两次给予,每次1毫克/千克体重 - 总剂量2毫克/千克体重)。我们观察到,无论给药途径如何,用柠檬酸盐包覆的AgNPs处理的小鼠肿瘤中5 - 甲基胞嘧啶(5 - mC)水平显著降低。对于聚乙二醇包覆的AgNPs,仅在静脉内给药后观察到DNA甲基化显著降低。此外,用AgNPs处理4T1荷瘤小鼠可降低肿瘤组织中的组蛋白H3甲基化。这种效应在静脉内给予聚乙二醇包覆的AgNPs时最为明显。未观察到组蛋白H3赖氨酸9乙酰化的变化。DNA和组蛋白H3甲基化的降低伴随着编码染色质修饰酶(Setd4、Setdb1、Smyd3、Suv39h1、Suv420h1、Whsc1、Kdm1a、Kdm5b、Esco2、Hat1、Myst3、Hdac5、Dnmt1、Ube2b和Usp22)的基因以及与致癌作用相关的基因(Akt1、Brca1、Brca2、Mlh1、Myb、Ccnd1和Src)表达的变化。观察到的变化的意义及其发生机制尚不清楚,该领域需要更多研究。然而,本研究指出表观遗传效应是纳米材料与生物系统之间相互作用的一个重要层面,在分析纳米材料的生物活性和纳米药物开发过程中应始终予以考虑。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/011e/10254218/b5f4e8ee08dd/materials-16-04163-g001.jpg

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