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通过纳米封装伊马替尼和橙皮苷靶向 MDR-1 基因表达、BAX/BCL2、caspase-3 和 Ki-67,以增强抗癌活性并减轻心脏毒性。

Targeting MDR-1 gene expression, BAX/BCL2, caspase-3, and Ki-67 by nanoencapsulated imatinib and hesperidin to enhance anticancer activity and ameliorate cardiotoxicity.

机构信息

Pharmacology and Toxicology department, College of Pharmacy, University of Tanta, Tanta, Egypt.

Department of Pathology, College of Veterinary Medicine, University of El-Mansoura, Mansoura, Egypt.

出版信息

Fundam Clin Pharmacol. 2020 Aug;34(4):458-475. doi: 10.1111/fcp.12549. Epub 2020 Mar 12.

DOI:10.1111/fcp.12549
PMID:32080901
Abstract

There is a great demand to introduce new approaches into cancer treatment field due to incidence of increased breast cancer all over the world. The current study was designed to evaluate the role of imatinib mesylate (IM) and/or hesperidin (HES) nanoparticles alone or in combination in enhancing the anticancer activity and to investigate the ability of nanoencapsulation to reduce cardiotoxicity of IM in solid Ehrlich carcinoma (SEC)-bearing mice. IM and HES were loaded into PLGA (poly(lactic-co-glycolic acid) polymer. SEC was induced in female albino mice as a model for experimentally induced breast cancer. Mice were randomly divided into eight groups (n = 10). On day 28 from tumor inoculation, mice were sacrificed and blood samples were collected in heparinized tubes for hematological studies, biochemical determination of lactate dehydrogenase (LDH), and glutamic oxaloacetic transaminase (SGOT) levels. In addition, tumor and cardiac tissues were utilized for histopathological examination as well as determination of MDR-1 gene expression. Immunohistochemical staining of BAX and BCL-2 was done. Nano IM- and/or Nano HES-treated groups showed a significant reduction in tumor volume, weight, hematological, cardiac markers, and tumor MDR-1 gene downregulation compared to free conventional treated groups. In conclusion, the use of HES as an adjuvant therapy with IM could improve its cytotoxic effects and limit its cardiac toxicity. Furthermore, nanoencapsulation of IM and/or HES with PLGA polymer showed a remarkable anticancer activity.

摘要

由于全球乳腺癌发病率的增加,人们迫切需要引入新的方法来治疗癌症。本研究旨在评估甲磺酸伊马替尼(IM)和/或橙皮苷(HES)纳米粒单独或联合应用在增强抗癌活性方面的作用,并研究纳米包封对降低 IM 在固着型艾氏腹水癌(SEC)荷瘤小鼠中心脏毒性的能力。IM 和 HES 被载入 PLGA(聚(乳酸-共-乙醇酸)聚合物中。将雌性白化小鼠诱导为实验性诱导乳腺癌的模型。将小鼠随机分为 8 组(n=10)。在肿瘤接种后第 28 天,处死小鼠并收集肝素化管中的血液样本,用于血液学研究、乳酸脱氢酶(LDH)和谷氨酸草酰乙酸转氨酶(SGOT)水平的生化测定。此外,还利用肿瘤和心脏组织进行组织病理学检查以及多药耐药基因-1(MDR-1)基因表达的测定。进行了 BAX 和 BCL-2 的免疫组织化学染色。与游离常规治疗组相比,纳米 IM-和/或纳米 HES 治疗组的肿瘤体积、重量、血液学、心脏标志物和肿瘤 MDR-1 基因下调均显著降低。总之,将 HES 作为 IM 的辅助治疗药物可以提高其细胞毒性作用并限制其心脏毒性。此外,用 PLGA 聚合物对 IM 和/或 HES 进行纳米包封显示出显著的抗癌活性。

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