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Neonatal Fc Receptor-Mediated IgG Transport Across Porcine Intestinal Epithelial Cells: Potentially Provide the Mucosal Protection

机译:跨猪肠道上皮细胞的新生Fc受体介导的IgG运输:潜在地提供粘膜保护。

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It has been well characterized that piglets can absorb colostrum IgG across the intestine to neonatal bloodstream and a certain level of IgG has been found in the mucosal secretions of the porcine intestinal tract. However, little is known about how the maternal IgG transport across the intestinal barrier and how IgG enter the lumen of intestinal tract. In this study, we demonstrated that the porcine neonatal Fc receptor (pFcRn) was expressed in a model of normal porcine intestinal epithelial cells (IPEC-J2) as well as in kidney cells (PK-15), and pFcRn was mainly distributed in the apical side of the polarized IPEC-J2 cells. Analyzing the phylogenetic relatedness of this gene we found that swine and human neonatal Fc receptor (FcRn) amino acid sequence are closer than rodents. We also showed that pFcRn mediated bidirectional IgG transport across polarized IPEC-J2 cells and bound to IgG in a pH-dependent manner. Furthermore, pFcRn-transcytosed viral-specific IgG reduced the transmissible gastroenteritis virus (TGEV) yield from the luminal direction by a 50% tissue culture infective dose (TCID50) assay. Our results indicate that pFcRn-dependent bidirectional IgG transport across the intestinal epithelium plays critical role in the acquisition of humoral immunity in early life and in host defense at mucosal surfaces.
机译:众所周知,仔猪可以从肠道吸收初乳IgG进入新生儿血流,并且在猪肠道粘膜分泌物中发现了一定水平的IgG。然而,关于母体IgG如何跨肠屏障运输以及IgG如何进入肠腔的了解甚少。在这项研究中,我们证明了猪新生Fc受体(pFcRn)在正常猪肠上皮细胞(IPEC-J2)和肾细胞(PK-15)的模型中表达,而pFcRn主要分布在极化的IPEC-J2细胞的顶侧。分析该基因的系统发育相关性,我们发现猪和人类新生儿Fc受体(FcRn)氨基酸序列比啮齿动物更近。我们还显示,pFcRn介导的双​​向IgG跨极化IPEC-J2细胞转运,并以pH依赖性方式与IgG结合。此外,通过50%组织培养物感染剂量(TCID50)分析,pFcRn转导的病毒特异性IgG从腔方向降低了可传播的胃肠炎病毒(TGEV)的产量。我们的结果表明,pFcRn依赖的双向IgG跨肠上皮运输在生命早期获得体液免疫和黏膜表面宿主防御中起关键作用。

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