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分析海洋生物毒素 okadaic 酸通过体外人体肠道屏障的过程。

Analysis of the passage of the marine biotoxin okadaic acid through an in vitro human gut barrier.

机构信息

Federal Institute for Risk Assessment, Department of Food Safety, Thielallee 88-92, D-14195 Berlin, Germany.

出版信息

Toxicology. 2011 Jan 11;279(1-3):196-202. doi: 10.1016/j.tox.2010.11.001. Epub 2010 Nov 17.

Abstract

The marine biotoxin okadaic acid (OA), produced by dinoflagellates, can accumulate in various bivalve molluscs. In humans, oral consumption of shellfish contaminated with OA induces acute toxic effects like diarrhea, nausea, vomiting and abdominal pain. However, tumorigenic and embryotoxic effects of OA have been also described. Current toxicokinetic studies with mice were performed with high cytotoxic oral doses leading presumably to a paracellular passage of OA through the gastrointestinal barrier. There are no studies available analyzing the absorption at low concentrations, which represent a realistic dietary exposure, making a reliable risk assessment difficult. Therefore, we performed a low-dose study using the human intestinal Caco-2 cell model to simulate the intestinal barrier. Low level exposure of 20-200 nM OA to the cell monolayer allows an only limited passage from the "luminal" to the "blood side". Furthermore, we could detect a significant efflux of OA, which led to the suggestion that active transport mechanisms are involved in the elimination process of OA. In conclusion, our results indicate that besides the well known defense mechanisms of humans against this marine biotoxin--vomiting and diarrhea--further detoxification mechanisms are available to limit the absorption of toxic OA.

摘要

海洋生物毒素 okadaic 酸(OA)由双鞭毛藻类产生,可在各种双壳贝类中积累。人类食用受 OA 污染的贝类会引起急性毒性作用,如腹泻、恶心、呕吐和腹痛。然而,OA 也具有致瘤和胚胎毒性作用。目前对小鼠进行的毒代动力学研究采用高细胞毒性口服剂量,推测 OA 通过胃肠道屏障的细胞旁途径。目前尚无分析低浓度吸收的研究,而低浓度吸收代表了实际的饮食暴露,这使得可靠的风险评估变得困难。因此,我们使用人肠 Caco-2 细胞模型进行了一项低剂量研究,以模拟肠道屏障。细胞单层中 20-200 nM OA 的低水平暴露仅允许 OA 从“腔侧”有限地穿过到“血侧”。此外,我们可以检测到 OA 的显著外排,这表明主动转运机制参与了 OA 的消除过程。总之,我们的结果表明,除了人类已知的针对这种海洋生物毒素的防御机制——呕吐和腹泻——之外,还有其他解毒机制可用于限制有毒 OA 的吸收。

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