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胎儿和新生小鼠获取母体IgG对β2-微球蛋白相关Fc受体的需求。

Requirement for a beta 2-microglobulin-associated Fc receptor for acquisition of maternal IgG by fetal and neonatal mice.

作者信息

Israel E J, Patel V K, Taylor S F, Marshak-Rothstein A, Simister N E

机构信息

Combined Program in Pediatric Gastroenterology and Nutrition, Harvard Medical School, Massachusetts General Hospital, Boston 02114, USA.

出版信息

J Immunol. 1995 Jun 15;154(12):6246-51.

PMID:7759862
Abstract

There is considerable evidence to suggest that an FcR similar in structure to class I MHC Ags, neonatal Fc receptor (FcRn), transports IgG across the intestinal epithelium of suckling mice. However, this has not previously been shown definitively, nor has it been shown whether FcRn is the only, or even the major, IgG transporter in the neonatal mouse gut. We report here that neonatal mice homozygous for a targeted disruption of the beta 2microglobulin (beta 2m) gene, which encodes one subunit of FcRn, had reduced FcRn alpha-chain at the lumenal plasma membrane of intestinal cells. These mice had strikingly lower serum IgG levels during the first month after birth than littermates that possessed functional FcRn. Furthermore, we found by fostering mice on mothers with a different IgG allotype that all of the IgG in sera of beta 2m-/- mice was endogenous, and that none was obtained from milk. We conclude that FcRn is the only transporter of IgG from mother to young in the mouse. The onset of IgG synthesis in mice that received no milk IgG lagged behind that in siblings with normal IgG transport, suggesting that maternal IgG stimulates Ab production in the neonate. We noted no difference between the IgG concentrations in the milk of beta 2m-/- and beta 2m+/- mice, indicating that FcRn is not involved in the secretion of IgG into milk.

摘要

有大量证据表明,一种结构与I类MHC抗原相似的FcR,即新生儿Fc受体(FcRn),可将IgG转运过哺乳期小鼠的肠上皮。然而,此前尚未明确证实这一点,也未表明FcRn是否是新生小鼠肠道中唯一的,甚至是主要的IgG转运蛋白。我们在此报告,β2微球蛋白(β2m)基因靶向破坏的纯合新生小鼠,该基因编码FcRn的一个亚基,其肠道细胞腔面膜上的FcRnα链减少。这些小鼠在出生后的第一个月血清IgG水平明显低于具有功能性FcRn的同窝小鼠。此外,我们通过将小鼠寄养在具有不同IgG同种异型的母亲身上发现,β2m-/-小鼠血清中的所有IgG都是内源性的,没有从乳汁中获得。我们得出结论,FcRn是小鼠中IgG从母体到幼体的唯一转运蛋白。未接受乳汁IgG的小鼠中IgG合成的开始时间落后于具有正常IgG转运的同窝小鼠,这表明母体IgG刺激新生儿抗体产生。我们注意到β2m-/-和β2m+/-小鼠乳汁中的IgG浓度没有差异,表明FcRn不参与IgG分泌到乳汁中。

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