三氯蔗糖-6-乙酸酯及其母体三氯蔗糖的毒理学和药代动力学特性:体外筛选试验。

IF 6.4 2区 医学 Q1 ENVIRONMENTAL SCIENCES Journal of Toxicology and Environmental Health-Part B-Critical Reviews Pub Date : 2023-08-18 DOI:10.1080/10937404.2023.2213903
Susan S Schiffman, Elizabeth H Scholl, Terrence S Furey, H Troy Nagle
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引用次数: 2

摘要

本研究的目的是确定三氯蔗糖-6-乙酸酯的毒理学和药代动力学性质,三氯蔗糖是一种结构类似于人工甜味剂三氯蔗糖的物质。三氯蔗糖-6-乙酸是生产三氯蔗糖的中间体和杂质,最近的商业三氯蔗糖样品被发现含有高达0.67%的三氯蔗糖-6-乙酸。在啮齿动物模型中进行的研究发现,粪便样本中也存在三氯蔗糖-6-乙酸酯,其含量高达三氯蔗糖的10%这表明三氯蔗糖在肠道中也会乙酰化。高通量遗传毒性筛选工具MultiFlow®测定和检测细胞遗传损伤的微核(MN)试验均表明三氯蔗糖-6-乙酸酯具有遗传毒性。使用MultiFlow®检测,作用机制被归类为致裂性(产生DNA链断裂)。每日一次含三氯蔗糖饮料中三氯蔗糖-6-乙酸酯的含量可能远远超过基因毒性毒理学关注的阈值(TTCgenotox) 0.15µg/人/天。使用RepliGut®系统将人肠上皮暴露于三氯蔗糖-6-乙酸和三氯蔗糖中,并进行RNA-seq分析以确定这些暴露诱导的基因表达。三氯蔗糖-6-乙酸显著增加炎症、氧化应激和癌症相关基因的表达,其中金属硫蛋白1g基因(MT1G)表达最多。人横结肠上皮经上皮电阻(TEER)和通透性的测量表明,三氯蔗糖-6-醋酸酯和三氯蔗糖都损害了肠屏障的完整性。三氯蔗糖-6-乙酸也抑制细胞色素P450家族的两个成员(CYP1A2和CYP2C19)。总的来说,三氯蔗糖-6-乙酸酯的毒理学和药代动力学研究结果引起了对三氯蔗糖本身安全性和监管地位的重大健康关注。
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Toxicological and pharmacokinetic properties of sucralose-6-acetate and its parent sucralose: in vitro screening assays.

The purpose of this study was to determine the toxicological and pharmacokinetic properties of sucralose-6-acetate, a structural analog of the artificial sweetener sucralose. Sucralose-6-acetate is an intermediate and impurity in the manufacture of sucralose, and recent commercial sucralose samples were found to contain up to 0.67% sucralose-6-acetate. Studies in a rodent model found that sucralose-6-acetate is also present in fecal samples with levels up to 10% relative to sucralose which suggest that sucralose is also acetylated in the intestines. A MultiFlow® assay, a high-throughput genotoxicity screening tool, and a micronucleus (MN) test that detects cytogenetic damage both indicated that sucralose-6-acetate is genotoxic. The mechanism of action was classified as clastogenic (produces DNA strand breaks) using the MultiFlow® assay. The amount of sucralose-6-acetate in a single daily sucralose-sweetened drink might far exceed the threshold of toxicological concern for genotoxicity (TTCgenotox) of 0.15 µg/person/day. The RepliGut® System was employed to expose human intestinal epithelium to sucralose-6-acetate and sucralose, and an RNA-seq analysis was performed to determine gene expression induced by these exposures. Sucralose-6-acetate significantly increased the expression of genes associated with inflammation, oxidative stress, and cancer with greatest expression for the metallothionein 1 G gene (MT1G). Measurements of transepithelial electrical resistance (TEER) and permeability in human transverse colon epithelium indicated that sucralose-6-acetate and sucralose both impaired intestinal barrier integrity. Sucralose-6-acetate also inhibited two members of the cytochrome P450 family (CYP1A2 and CYP2C19). Overall, the toxicological and pharmacokinetic findings for sucralose-6-acetate raise significant health concerns regarding the safety and regulatory status of sucralose itself.

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来源期刊
CiteScore
13.80
自引率
6.90%
发文量
13
审稿时长
>24 weeks
期刊介绍: "Journal of Toxicology and Environmental Health: Part B - Critical Reviews" is an academic journal published by Taylor & Francis, focusing on the critical examination of research in the areas of environmental exposure and population health. With an ISSN identifier of 1093-7404, this journal has established itself as a significant source of scholarly content in the field of toxicology and environmental health. Since its inception, the journal has published over 424 articles that have garnered 35,097 citations, reflecting its impact and relevance in the scientific community. Known for its comprehensive reviews, the journal also goes by the names "Critical Reviews" and "Journal of Toxicology & Environmental Health, Part B, Critical Reviews." The journal's mission is to provide a platform for in-depth analysis and critical discussion of the latest findings in toxicology, environmental health, and related disciplines. By doing so, it contributes to the advancement of knowledge and understanding of the complex interactions between environmental factors and human health, aiding in the development of strategies to protect and improve public health.
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