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新生仔猪小肠对免疫球蛋白G的优先转运。

The preferential transport of immunoglobulin G by the small intestine of the neonatal piglet.

作者信息

Leary H L, Lecce J G

出版信息

J Nutr. 1979 Mar;109(3):458-66. doi: 10.1093/jn/109.3.458.

Abstract

Previous work dealing with the acquisition of passive immunity by the neonatal mammal has shown that the piglet is qualitatively nonselective with regard to the transport of macromolecules from the gut to the blood, whereas rats, mice and hamsters transport only immunoglobulin G (IgG) in detectable quantities. The ability of enterocytes of the proximal and distal small intestine of piglets to internalize fluorescent porcine IgG, bovine albumin or a mixture of these two fluorescent proteins was assessed. At the light microscopic level (macropinocytosis) porcine IgG and bovine albumin were internalized with equal facility by these enterocytes. To determine whether piglets preferentially transported porcine IgG versus bovine albumin, other piglets were gavaged with these proteins or these proteins were injected into ligated segments of the proximal or distal small intestine. Enterocytes in the proximal part of the small intestine transported more of these proteins (P less than 0.10) than did those in the distal part. When either bovine albumin or porcine IgG was presented separately to the piglet's gut, both were transported to about the same low level. However, when mixtures of these proteins were presented, IgG was preferentially transported, i.e., albumin enhanced IgG transport. Porcine albumin or polyvinylpyrrolidone (PVP) also enhanced porcine IgG transport. It was proposed that the preferential transport of IgG occurred by a micropinocytotic mechanism (not visible by light microscopy) and that other macromolecules such as albumin and PVP enhanced IgG transport by nonspecifically stimulating micropinocytosis.

摘要

先前关于新生哺乳动物获得被动免疫的研究表明,仔猪在将大分子从肠道转运到血液方面没有质的选择性,而大鼠、小鼠和仓鼠仅能检测到运输免疫球蛋白G(IgG)。评估了仔猪近端和远端小肠肠细胞内化荧光猪IgG、牛血清白蛋白或这两种荧光蛋白混合物的能力。在光学显微镜水平(巨吞饮作用),这些肠细胞以相同的易化程度内化猪IgG和牛血清白蛋白。为了确定仔猪是否优先转运猪IgG而非牛血清白蛋白,给其他仔猪灌胃这些蛋白质,或将这些蛋白质注射到近端或远端小肠的结扎段。小肠近端的肠细胞比远端的肠细胞转运更多的这些蛋白质(P小于0.10)。当单独给仔猪肠道提供牛血清白蛋白或猪IgG时,两者的转运水平都很低且大致相同。然而,当提供这些蛋白质的混合物时,IgG被优先转运,即白蛋白增强了IgG的转运。猪白蛋白或聚乙烯吡咯烷酮(PVP)也增强了猪IgG的转运。有人提出,IgG的优先转运是通过微吞饮机制发生的(光学显微镜下不可见),而其他大分子如白蛋白和PVP通过非特异性刺激微吞饮作用增强了IgG的转运。

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