Berberine-loaded albumin nanoparticles reverse aflatoxin B1-induced liver hyperplasia.

IF 2.8 3区 医学 Q2 PHARMACOLOGY & PHARMACY BMC Pharmacology & Toxicology Pub Date : 2023-08-10 DOI:10.1186/s40360-023-00683-w
Sarah M Khedr, Doaa A Ghareeb, Shadia A Fathy, Germine M Hamdy
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Abstract

Hepatocellular carcinoma (HCC) can be produced from aflatoxin B1 (AFB1) administration. Although berberine (BER) acts as an anticancer agent and can counteract the AFB1 effect, it has low bioavailability. Nanotechnology can overcome this problem. This research aimed to synthesize berberine nanoparticles (NPs) and then estimate their therapeutic effect compared to that of berberine against aflatoxin-induced hepatotoxicity. The desolvation method was used to prepare BER-NPs. Aflatoxicosis was induced by 5 consecutive intraperitoneal injections (IP) of 200 µg/kg/day AFB dissolved in dimethylsulfoxide (DMSO). After the induction period, two treatments were performed: the first with 100 mg/kg BER and the second with 10 mg/kg BER-NPs. Liver, kidney, and diabetic profiles were estimated by using standardized methods. Hepatic oxidative stress, inflammatory, cancer cell proliferation, and invasion markers were used by ELISA and qPCR techniques. The TEM image shows that both BSA NPs and BER-BSA NPs had spherical, regular, and uniform shapes. The BER encapsulation efficiency % was 78.5. The formed-BER-BSA NPs showed a loading capacity % of 7.71 and the synthesis yield % of 92.6. AFB1 increases pro-oxidant markers, decreases antioxidant systems, stimulates inflammatory enzymes, inhibits anti-inflammatory markers, decreases tumor suppressor enzymes, increases oncogenes, increases glycolytic activity, prevents cell death, and promotes cell growth. Most of the biochemical markers and hepatic architecture were normalized in the BER-BSA NP-treated group but not in the BER-treated group. Altogether, the obtained data proved that treatment with BER-NPs was more efficient than treatment with berberine against aflatoxicoses induced in rats.

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黄连素白蛋白纳米粒子逆转黄曲霉毒素B1诱导的肝增生。
肝细胞癌(HCC)可由黄曲霉毒素B1(AFB1)给药产生。尽管黄连素(BER)是一种抗癌剂,可以抵消AFB1的作用,但其生物利用度较低。纳米技术可以克服这个问题。本研究旨在合成黄连素纳米颗粒(NPs),并与黄连素对黄曲霉毒素诱导的肝毒性的治疗效果进行比较。采用去溶剂化方法制备了BER NPs。通过连续5次腹膜内注射(IP)溶于二甲基亚砜(DMSO)的200µg/kg/天AFB来诱导黄曲霉毒素中毒。诱导期后,进行两次处理:第一次用100mg/kg BER,第二次用10mg/kg BER NPs。肝、肾和糖尿病的情况是通过使用标准化方法进行评估的。通过ELISA和qPCR技术检测肝氧化应激、炎症、癌症细胞增殖和侵袭标志物。TEM图像显示BSA NPs和BER-BSA NPs都具有球形、规则和均匀的形状。BER封装效率%为78.5。所形成的BER-BSA NP显示出7.71的负载能力%和92.6的合成产率%。AFB1增加促氧化标记物,减少抗氧化系统,刺激炎症酶,抑制抗炎标记物,降低肿瘤抑制酶,增加致癌基因,增加糖酵解活性,防止细胞死亡,促进细胞生长。BER-BSA NP治疗组的大多数生化标志物和肝脏结构正常化,但BER治疗组没有。总之,所获得的数据证明,用BER NPs治疗对大鼠诱发的aflatoxides比用黄连素治疗更有效。
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来源期刊
BMC Pharmacology & Toxicology
BMC Pharmacology & Toxicology PHARMACOLOGY & PHARMACYTOXICOLOGY&nb-TOXICOLOGY
CiteScore
4.80
自引率
0.00%
发文量
87
审稿时长
12 weeks
期刊介绍: BMC Pharmacology and Toxicology is an open access, peer-reviewed journal that considers articles on all aspects of chemically defined therapeutic and toxic agents. The journal welcomes submissions from all fields of experimental and clinical pharmacology including clinical trials and toxicology.
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