首页> 美国卫生研究院文献>PLoS Clinical Trials >Dextran Sodium Sulfate (DSS) Induces Colitis in Mice by Forming Nano-Lipocomplexes with Medium-Chain-Length Fatty Acids in the Colon
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Dextran Sodium Sulfate (DSS) Induces Colitis in Mice by Forming Nano-Lipocomplexes with Medium-Chain-Length Fatty Acids in the Colon

机译:葡聚糖硫酸钠(DSS)通过在结肠中形成具有中等链长脂肪酸的纳米脂质复合物诱导小鼠结肠炎

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摘要

Inflammatory bowel diseases (IBDs), primarily ulcerative colitis and Crohn's disease, are inflammatory disorders caused by multiple factors. Research on IBD has often used the dextran sodium sulfate (DSS)-induced colitis mouse model. DSS induces in vivo but not in vitro intestinal inflammation. In addition, no DSS-associated molecule (free glucose, sodium sulfate solution, free dextran) induces in vitro or in vivo intestinal inflammation. We find that DSS but not dextran associated molecules established linkages with medium-chain-length fatty acids (MCFAs), such as dodecanoate, that are present in the colonic lumen. DSS complexed to MCFAs forms nanometer-sized vesicles ∼200 nm in diameter that can fuse with colonocyte membranes. The arrival of nanometer-sized DSS/MCFA vesicles in the cytoplasm may activate intestinal inflammatory signaling pathways. We also show that the inflammatory activity of DSS is mediated by the dextran moieties. The deleterious effect of DSS is localized principally in the distal colon, therefore it will be important to chemically modify DSS to develop materials beneficial to the colon without affecting colon-targeting specificity.
机译:炎症性肠病(IBD),主要是溃疡性结肠炎和克罗恩氏病,是由多种因素引起的炎症性疾病。 IBD的研究通常使用右旋糖酐硫酸钠(DSS)诱导的结肠炎小鼠模型。 DSS诱导体内而非体外肠道炎症。另外,没有DSS相关分子(游离葡萄糖,硫酸钠溶液,游离右旋糖酐)诱导体外或体内肠道炎症。我们发现,DSS但未与右旋糖酐相关的分子建立了与结肠腔中存在的中链长度脂肪酸(MCFA)(例如十二烷酸酯)的联系。与MCFAs复合的DSS形成直径约200 nm的纳米大小的囊泡,可以与结肠细胞膜融合。纳米级DSS / MCFA囊泡到达细胞质可能会激活肠道炎症信号通路。我们还表明,DSS的炎症活性是由葡聚糖部分介导的。 DSS的有害作用主要位于远端结肠,因此,重要的是化学修饰DSS以开发有益于结肠的物质而不影响结肠靶向特异性。

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