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桔霉素的食品毒性及其通过计算机辅助多维数据分析预测的相关靶点产生潜在毒性作用的分子机制

Food Toxicity of Mycotoxin Citrinin and Molecular Mechanisms of Its Potential Toxicity Effects through the Implicated Targets Predicted by Computer-Aided Multidimensional Data Analysis.

作者信息

Zargar Seema, Wani Tanveer A

机构信息

Department of Biochemistry, College of Science, King Saud University, Riyadh 11495, Saudi Arabia.

Department of Pharmaceutical Chemistry, College of Pharmacy, King Saud University, Riyadh 11451, Saudi Arabia.

出版信息

Life (Basel). 2023 Mar 26;13(4):880. doi: 10.3390/life13040880.

Abstract

The mycotoxin citrinin, which can contaminate food, is a major global concern. Citrinin is regarded as an inevitable pollutant in foods and feed since fungi are widely present in the environment. To identify contentious toxicity and lessen its severity by understanding the targets of citrinin in the human body and the impacted biosynthetic pathways, we analyzed the production of citrinin from and and used a thorough bioinformatics analysis to characterize the toxicity and predict genes and protein targets for it. The predicted median fatal dosage (LD) for citrinin was 105 mg/kg weight, and it belonged to toxicity class 3 (toxic if swallowed). Citrinin was found to be well absorbed by human intestinal epithelium and was a Pgp nonsubstrate (permeability glycoprotein), which means that once it is absorbed, it cannot be pumped out, hence leading to bioconcentration or biomagnification in the human body. The main targets of toxicity were casp3, TNF, IL10, IL1B, BAG3, CCNB1, CCNE1, and CDC25A, and the biological pathways implicated were signal transduction involved in DNA damage checkpoints, cellular and chemical responses to oxidative stress, DNA damage response signal transduction by P53, stress-activated protein kinase signaling cascade, netrin-UNC5B signaling, PTEN gene regulation, and immune response. Citrinin was linked to neutrophilia, squamous cell carcinoma, Fanconi anemia, leukemia, hepatoblastoma, and fatty liver diseases. The transcription factors E2F1, HSF1, SIRT1, RELA, NFKB, JUN, and MYC were found to be responsible. When data mining was performed on citrinin targets, the top five functional descriptions were a cell's response to an organic cyclic compound, the netrin-UNC5B signaling pathway, lipids and atherosclerosis, thyroid cancer, and controlling the transcription of the PTEN gene.

摘要

可污染食物的霉菌毒素桔霉素是全球主要关注的问题。由于真菌在环境中广泛存在,桔霉素被视为食品和饲料中不可避免的污染物。为了通过了解桔霉素在人体中的作用靶点和受影响的生物合成途径来确定其有争议的毒性并减轻其严重程度,我们分析了桔霉素的产生情况,并进行了全面的生物信息学分析以表征其毒性并预测其基因和蛋白质靶点。桔霉素的预测半数致死剂量(LD)为105毫克/千克体重,属于3类毒性(吞咽有毒)。研究发现,桔霉素能被人肠上皮细胞很好地吸收,且不是Pgp底物(通透性糖蛋白),这意味着它一旦被吸收就无法被泵出,从而导致在人体中生物浓缩或生物放大。毒性的主要靶点是casp3、TNF、IL10、IL1B、BAG3、CCNB1、CCNE1和CDC25A,涉及的生物途径包括DNA损伤检查点中的信号转导、对氧化应激的细胞和化学反应、P53介导的DNA损伤反应信号转导、应激激活蛋白激酶信号级联、netrin-UNC5B信号传导、PTEN基因调控和免疫反应。桔霉素与嗜中性粒细胞增多、鳞状细胞癌、范可尼贫血、白血病、肝母细胞瘤和脂肪肝疾病有关。发现转录因子E2F1、HSF1、SIRT1、RELA、NFKB、JUN和MYC对此负责。对桔霉素靶点进行数据挖掘时,排名前五的功能描述是细胞对有机环状化合物的反应、netrin-UNC5B信号通路、脂质与动脉粥样硬化、甲状腺癌以及控制PTEN基因的转录。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a6af/10142723/12744465180c/life-13-00880-g001.jpg

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