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应用生理动力学模型预测脱氧雪腐镰刀菌烯醇的代谢及其在人类肠道炎症和胆汁酸动力学中的作用。

Use of Physiologically Based Kinetic Modeling to Predict Deoxynivalenol Metabolism and Its Role in Intestinal Inflammation and Bile Acid Kinetics in Humans.

机构信息

Division of Toxicology, Wageningen University and Research, Stippeneng 4, 6708 WE, Wageningen, Netherlands.

出版信息

J Agric Food Chem. 2024 Jan 10;72(1):761-772. doi: 10.1021/acs.jafc.3c07137. Epub 2023 Dec 22.

Abstract

Current points of departure used to derive health-based guidance values for deoxynivalenol (DON) are based on studies in laboratory animals. Here, an animal-free testing approach was adopted in which a reverse dosimetry physiologically based kinetic (PBK) modeling is used to predict in vivo dose response curves for DON's effects on intestinal pro-inflammatory cytokine secretion and intestinal bile acid reabsorption in humans from concentration-effect relationships for DON in vitro. The calculated doses for inducing a 5% added effect above the background level (ED) of DON for increasing IL-1β secretion in intestinal tissue and for increasing the amounts in the colon lumen of glycochenodeoxycholic acid (GCDCA) were 246 and 36 μg/kg bw/day, respectively. These in vitro-in silico-derived ED values were compared to human dietary DON exposure levels, indicating that the risk of DON's effects on these end points occurring in various human populations cannot be excluded. This in vitro-in silico approach provides a novel testing strategy for hazard and risk assessment without using laboratory animals.

摘要

目前用于推导脱氧雪腐镰刀菌烯醇 (DON) 的基于健康的指导值的出发点是基于实验室动物的研究。在这里,采用了一种无动物测试方法,该方法使用反向剂量学基于生理学的动力学 (PBK) 建模来预测 DON 对肠道促炎细胞因子分泌的体内剂量反应曲线,以及从 DON 在体外对肠道胆汁酸重吸收的浓度-效应关系中,预测 DON 对人类肠道促炎细胞因子分泌和肠道胆汁酸重吸收的体内剂量反应曲线。计算得出,使肠道组织中 IL-1β 分泌增加 5%的 DON 诱导剂量(ED)和使结肠腔中甘氨胆酸 (GCDCA) 量增加的 DON 诱导剂量分别为 246 和 36 μg/kg bw/day。将这些体外-计算得出的 ED 值与人类膳食 DON 暴露水平进行比较,表明不能排除 DON 对这些终点的影响在不同人群中发生的风险。这种体外-计算方法为危害和风险评估提供了一种新颖的测试策略,而无需使用实验室动物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/acbc/10786035/973e9b8b7043/jf3c07137_0001.jpg

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