MMP-1 and MMP-7 Expression is Influenced by Ginsenosides in Mice Exposed to Aflatoxin B1: in vivo Study

Q3 Pharmacology, Toxicology and Pharmaceutics

Jordan Journal of Pharmaceutical Sciences Pub Date : 2024-03-19 DOI:10.35516/jjps.v17i2.1989

Safa M Abdulateef, S. Ibraheem, Humam S Hussein, B. Dheeb, B. M. Khashman, Dunya Muayed Ahmed, Khaled H Abu-Elteen, L. Abu-Qatouseh

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Abstract

Panax ginseng (PG), one of the most widely used herbal medicines, has demonstrated various beneficial effects such as anti-inflammatory, antioxidant, and anticancer impacts. Naturally occurring ginsenosides in the ginseng plant inhibit cell proliferation and significantly reduce liver damage induced by certain chemicals. Aflatoxin B1 (AFB1) is a primary mycotoxin due to its hepatotoxic, immunotoxic, and oncogenic effects in animal models and humans. In this study, we examined the effects of assorted doses of PG aqueous crude extract on the expression of matrix metalloproteinase 1 and 7 (MMP-1 and MMP-7) in the kidney, spleen, and liver of experimental AFB1-exposed mice, using immunohistochemistry (IHC). Mice were orally administered 6 mg/kg body weight (bw) of refined AFB1 (isolated and extracted from Aspergillus flavus, conc. 0.05 ppm) twice weekly for two weeks. We then compared the effects of three different doses (50, 100, and 150 mg/kg bw) of crude ginseng. We estimated the expression of MMP-1 and 7 in organs using IHC. We used the 6 mg/kg of purified AFB1, representing a 60% concentration, as a control group. IHC analysis showed that MMP (1 and 7) expression in the spleen, liver, and kidney of mice decreased after treatment with ginseng crude extract. MMP-1 expression was reduced in the liver by approximately 2.6 times, while the effectiveness in the MMP-1 reduction reached 9 and 8 times, respectively, in the spleen and kidney when treated with a higher dose of PG compared to the control. MMP-7 expression was reduced in the liver by approximately 13 times, while the reduction effectiveness fell to 2.3 and 5.6 times in the spleen and kidney when treated with a higher dose of PG compared to the control. The reduction in MMPs expression due to the effect of PG aqueous crude extract was observed to act against the effect of AFB1 on various living organs involved in AFB1 metabolism. IHC analysis indicated a more significant reduction efficiency observed in the expression of MMP-7 compared to both studied markers in the mice's liver.

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人参皂苷影响暴露于黄曲霉毒素 B1 的小鼠体内 MMP-1 和 MMP-7 的表达：体内研究

人参（PG）是应用最广泛的草药之一，具有抗炎、抗氧化和抗癌等多种有益作用。人参植物中天然存在的人参皂苷能够抑制细胞增殖，并显著减轻某些化学物质对肝脏造成的损伤。黄曲霉毒素 B1（AFB1）是一种主要的霉菌毒素，在动物模型和人体中具有肝毒性、免疫毒性和致癌作用。在这项研究中，我们采用免疫组织化学方法（IHC），研究了各种剂量的 PG 水提取物对基质金属蛋白酶 1 和 7（MMP-1 和 MMP-7）在暴露于 AFB1 的小鼠肾脏、脾脏和肝脏中表达的影响。给小鼠口服 6 毫克/千克体重（bw）的精制 AFB1（从黄曲霉中分离提取，浓度为 0.05 ppm），每周两次，连续两周。然后，我们比较了三种不同剂量（50、100 和 150 毫克/千克体重）粗人参的效果。我们使用 IHC 评估了器官中 MMP-1 和 7 的表达。我们使用 6 毫克/千克纯化的 AFB1（浓度为 60%）作为对照组。IHC 分析表明，使用人参粗提取物治疗后，小鼠脾脏、肝脏和肾脏中的 MMP（1 和 7）表达量减少。肝脏中的 MMP-1 表达量减少了约 2.6 倍，而与对照组相比，用较高剂量的 PG 处理脾脏和肾脏时，MMP-1 的减少效果分别达到了 9 倍和 8 倍。与对照组相比，当使用较高剂量的 PG 时，肝脏中 MMP-7 的表达量减少了约 13 倍，而脾脏和肾脏中 MMP-7 的减少效果则分别下降到 2.3 倍和 5.6 倍。据观察，PG 水提取物可减少 MMPs 的表达，从而抵消 AFB1 对参与 AFB1 代谢的各种活体器官的影响。IHC 分析表明，与所研究的两种标记物相比，小鼠肝脏中 MMP-7 的表达明显减少。

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来源期刊

Jordan Journal of Pharmaceutical Sciences Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science

CiteScore

1.70

自引率

0.00%

发文量

期刊介绍： The Jordan Journal of Pharmaceutical Sciences (JJPS) is a scientific, bi-annual, peer-reviewed publication that will focus on current topics of interest to the pharmaceutical community at large. Although the JJPS is intended to be of interest to pharmaceutical scientists, other healthy workers, and manufacturing processors will also find it most interesting and informative. Papers will cover basic pharmaceutical and applied research, scientific commentaries, as well as views, reviews. Topics on products will include manufacturing process, quality control, pharmaceutical engineering, pharmaceutical technology, and philosophies on all aspects of pharmaceutical sciences. The editorial advisory board would like to place an emphasis on new and innovative methods, technologies, and techniques for the pharmaceutical industry. The reader will find a broad range of important topics in this first issue.