Hamad A R, Marrack P, Kappler J W
Department of Medicine, National Jewish Medical and Research Center, Denver, Colorado 80206, USA.
J Exp Med. 1997 Apr 21;185(8):1447-54. doi: 10.1084/jem.185.8.1447.
Staphylococcus aureus produces a set of proteins (e.g., staphylococcal enterotoxin A [SEA], SEB, toxic shock syndrome toxin 1 [TSST-1]) which act both as superantigens (SAgs) and toxins. Although their mode of action as SAgs is well understood, little is known about how they enter the body via the intestine and cause food poisoning. To examine this problem we used an in vitro culture system to study the capacity of class II MHC-negative human intestinal epithelial cells (Caco-2) to transcytose several staphylococcal toxins. We found that Caco-2 cells are capable of dose-dependent, facilitated transcytosis of SEB and TSST-1, but not SEA. We extended these studies in vivo in mice by showing that ingested SEB appears in the blood more efficiently than SEA. Our data suggest that these toxins can cross the epithelium in an immunologically intact form. These results may have important implications for the pathogenesis of food poisoning.
金黄色葡萄球菌产生一组蛋白质(如葡萄球菌肠毒素A [SEA]、SEB、中毒性休克综合征毒素1 [TSST-1]),这些蛋白质既作为超抗原(SAgs)又作为毒素发挥作用。尽管它们作为超抗原的作用模式已被充分了解,但对于它们如何通过肠道进入人体并导致食物中毒却知之甚少。为了研究这个问题,我们使用体外培养系统来研究II类MHC阴性的人肠上皮细胞(Caco-2)转胞吞几种葡萄球菌毒素的能力。我们发现Caco-2细胞能够以剂量依赖的方式促进SEB和TSST-1的转胞吞,但不能促进SEA的转胞吞。我们通过在小鼠体内进行研究扩展了这些发现,结果表明摄入的SEB比SEA更有效地出现在血液中。我们的数据表明,这些毒素能够以免疫完整的形式穿过上皮细胞。这些结果可能对食物中毒的发病机制具有重要意义。
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