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Binding Studies on Isolated Porcine Small Intestinal Mucosa and in vitro Toxicity Studies Reveal Lack of Effect of C. perfringens Beta-Toxin on the Porcine Intestinal Epithelium

机译:分离的猪小肠粘膜的结合研究和体外毒性研究表明产气荚膜梭菌β-毒素对猪小肠上皮缺乏影响

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Beta-toxin (CPB) is the essential virulence factor of C. perfringens type C causing necrotizing enteritis (NE) in different hosts. Using a pig infection model, we showed that CPB targets small intestinal endothelial cells. Its effect on the porcine intestinal epithelium, however, could not be adequately investigated by this approach. Using porcine neonatal jejunal explants and cryosections, we performed in situ binding studies with CPB. We confirmed binding of CPB to endothelial but could not detect binding to epithelial cells. In contrast, the intact epithelial layer inhibited CPB penetration into deeper intestinal layers. CPB failed to induce cytopathic effects in cultured polarized porcine intestinal epithelial cells (IPEC-J2) and primary jejunal epithelial cells. C. perfringens type C culture supernatants were toxic for cell cultures. This, however, was not inhibited by CPB neutralization. Our results show that, in the porcine small intestine, CPB primarily targets endothelial cells and does not bind to epithelial cells. An intact intestinal epithelial layer prevents CPB diffusion into underlying tissue and CPB alone does not cause direct damage to intestinal epithelial cells. Additional factors might be involved in the early epithelial damage which is needed for CPB diffusion towards its endothelial targets in the small intestine.
机译:β-毒素(CPB)是C型产气荚膜梭菌的重要毒力因子,可在不同宿主中引起坏死性肠炎(NE)。使用猪感染模型,我们显示CPB靶向小肠内皮细胞。然而,这种方法不能充分研究其对猪肠上皮的作用。使用猪新生儿空肠外植体和冰冻切片,我们用CPB进行了原位结合研究。我们证实了CPB与内皮细胞的结合,但无法检测到与上皮细胞的结合。相反,完整的上皮层抑制了CPB渗透到更深的肠层中。 CPB未能在培养的极化猪肠道上皮细胞(IPEC-J2)和原发性空肠上皮细胞中诱导细胞病变作用。产气荚膜梭菌的C型培养物上清液对细胞培养是有毒的。但是,这不受CPB中和的抑制。我们的结果表明,在猪小肠中,CPB主要靶向内皮细胞,并且不与上皮细胞结合。完整的肠上皮层可防止CPB扩散到下面的组织中,仅CPB不会对肠上皮细胞造成直接损害。 CPB向小肠中的内皮靶标扩散所需的早期上皮损伤可能还涉及其他因素。

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