MODULATOR IMPACTS OF PROPOLIS EXTRACT AGAINST DOXORUBICIN MEDIATED CARCINOGENESIS ON HEPATOCELLULAR CARCINOMA AND Drosophila SOMATIC CELLS

Egyptian Journal of Genetics and Cytology Pub Date : 2018-01-12 DOI:10.21608/EJGC.2018.9211

Naglaa M. Ebeed, Sawsan M. Abdelmegeed

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引用次数: 1

Abstract

The antitumor action of propolis is of clinical interest because of the need for new anticancer treatment agents. The present investigation intended to extract and assess the chemical content, cytotoxic action, the growth inhibitory activity and anticancer capability of Egyptian propolis versus Chinese propolis. This was carried out using water extract (WE) and ethanolic extract (EE) on the human hepatocellular carcinoma (HEp-2) cell line and the loss of heterozygosity (LOH) assay of Drosophila melanogaster somatic cells against the direct genotoxicity of doxorubicin. EPWE, EPEE, CPWE and CPEE extracts analyzed by HPLC showed that there were sensible and various concentrations of phenolic compounds in both. Total phenolics were determined to be 18.83, 34.87, 39.29 and 180.89 g-1 by using EPWE, CPWE, EPEE and CPEE extracts, respectively. Chinese propolis ethanol extract (CPEE) have major concentrations of total phenolics and phenolic acids and contained high concentrations of rutin (188.90 g/mL). The study of the antiproliferative capacity of propolis extractors against HEp-2 cancer cell lines showed that all the studied propolis extracts induce suppression of cell growth except CPWE extract; it gave 100% cell viability. The great majority of the propolis are strongly cytotoxic against HEp-2 cell line with 500 μg/ml CPEE. Also, PEE is the most effective in inhibition of HEp-2 cell proliferation compared to PWE. In Drosophila assay, treatment with propolis extract and DOX carcinogenic agent led to a reduction in the frequency of recombination compared to the treatment with DOX alone either in the post- and pre-treatments. In general, PEE exhibited powerful anti-proliferative effects than PWE. The ethanol extract provided the highest protection against Doxorubicin (DOR) induced genotoxicity, a fact that supports their anti-cancer activity. The results demonstrate that PEE is a good source of a natural antitumor operator able to inhibit cancer cell proliferation.

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紫杉醇提取物对阿霉素介导的肝癌和果蝇体细胞癌变的调节作用

由于需要新的抗癌治疗剂，蜂胶的抗肿瘤作用引起了临床的兴趣。本研究旨在提取和评价埃及蜂胶与中国蜂胶的化学成分、细胞毒性、生长抑制活性和抗癌能力。这是使用水提取物（WE）和乙醇提取物（EE）对人肝细胞癌（HEp-2）细胞系和果蝇体细胞针对阿霉素的直接遗传毒性的杂合性损失（LOH）测定进行的。EPWE、EPEE、CPWE和CPEE提取物的HPLC分析表明，两者中都存在明显的不同浓度的酚类化合物。用EPWE、CPWE、EPEE和CPEE提取物测定的总酚含量分别为18.83、34.87、39.29和180.89g-1。蜂胶乙醇提取物中总酚类物质和酚酸含量较高，芦丁含量较高（188.90g/mL）。蜂胶提取物对HEp-2癌症细胞系的抗增殖能力研究表明，除CPWE提取物外，所有研究的蜂胶提取物均诱导细胞生长抑制；它提供了100%的细胞活力。绝大多数蜂胶对500μg/ml CPEE的HEp-2细胞系具有强烈的细胞毒性。此外，与PWE相比，PEE在抑制HEp-2细胞增殖方面最有效。在果蝇试验中，与单独使用DOX处理相比，在处理后和处理前，使用蜂胶提取物和DOX致癌剂处理可降低重组频率。一般来说，PEE比PWE表现出强大的抗增殖作用。乙醇提取物对阿霉素（DOR）诱导的遗传毒性提供了最高的保护，这一事实支持了它们的抗癌活性。结果表明，PEE是一种能够抑制癌症细胞增殖的天然抗肿瘤算子的良好来源。

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来源期刊

Egyptian Journal of Genetics and Cytology

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审稿时长

12 weeks