FcRn 介导的 IgG 抗 IgE/IgE 免疫复合物在小鼠肠道中的吸收。
FcRn-mediated intestinal absorption of IgG anti-IgE/IgE immune complexes in mice.
机构信息
Department of Immunology, University of Connecticut Health Center, Farmington, CT, USA.
出版信息
Clin Exp Allergy. 2012 Dec;42(12):1791-800. doi: 10.1111/j.1365-2222.2012.04043.x.
BACKGROUND
The mechanism(s) responsible for the acquisition of maternal antibody isotypes other than IgG are not fully understood.
OBJECTIVE
To define the ability of the neonatal Fc receptor for IgG uptake (FcRn) to mediate intestinal absorption of IgG(1) anti-IgE/IgE immune complexes.
METHODS
C57BL/6 allergic ovalbumin (OVA)-immune foster mothers were generated to nurse naïve FcRn(+/-) or FcRn(-/-) progeny. At the time of weaning, serum levels of OVA-specific antibodies and IgG(1) anti-IgE/IgE immune complexes were determined in allergic foster mothers and FcRn(+/+), FcRn(+/-), or FcRn(-/-) breastfed offspring. In separate experiments, FcRn(+/-) or FcRn(-/-) neonatal mice were gavage fed TNP-specific IgE as IgG(1) anti-IgE/IgE immune complexes, IgG(1) isotype control and IgE, or IgE alone. Mice were killed 2 h after feeding to determine serum levels and biological activity of absorbed TNP-specific IgE.
RESULTS
As expected, the absorption of maternal OVA-specific IgG(1) in FcRn(-/-) offspring was at levels 10(3) -10(4) less than observed in FcRn(+/+) or FcRn(+/-) offspring. Surprisingly, FcRn expression also influenced the absorption of maternal IgE. OVA-specific IgE was detected in FcRn(+/+) and FcRn(+/-) offspring, but not in FcRn(-/-) offspring. IgG(1) anti-IgE/IgE immune complexes were detected in allergic foster mothers and correlated strongly with levels in FcRn(+/+) and FcRn(+/-) offspring (ρ = 0.88, P < 0.0001). Furthermore, FcRn expression was required for neonatal mice to absorb TNP-specific IgE when fed as IgG(1) anti-IgE/IgE immune complexes. When immune complexes were generated with IgG(1) anti-IgE directed against the Cε4 domain, the absorbed IgE was able to function in antigen-dependent basophil degranulation.
CONCLUSIONS AND CLINICAL RELEVANCE
These data demonstrate a novel mechanism by which FcRn may facilitate absorption of maternal antibodies other than IgG. These findings are clinically relevant because FcRn mediates the transplacental passage of maternal IgG to the fetus. This raises the possibility that FcRn could mediate the transplacental passage of maternal IgE as IgG anti-IgE/IgE immune complexes.
背景
负责获得 IgG 以外的母体抗体同种型的机制尚未完全阐明。
目的
定义新生儿 Fc 受体 IgG 摄取(FcRn)介导 IgG(1)抗 IgE/IgE 免疫复合物肠道吸收的能力。
方法
生成 C57BL/6 过敏卵清蛋白(OVA)免疫的寄养母亲,以养育新生 FcRn(+/-)或 FcRn(-/-)后代。在断奶时,测定过敏寄养母亲和 FcRn(+/+)、FcRn(+/-)或 FcRn(-/-)母乳喂养后代的 OVA 特异性抗体和 IgG(1)抗 IgE/IgE 免疫复合物血清水平。在单独的实验中,用 TNP 特异性 IgE 作为 IgG(1)抗 IgE/IgE 免疫复合物、IgG(1)同种型对照和 IgE 或 IgE 单独灌胃喂养 FcRn(+/-)或 FcRn(-/-)新生小鼠。喂食后 2 小时处死小鼠,以确定吸收的 TNP 特异性 IgE 的血清水平和生物学活性。
结果
正如预期的那样,FcRn(-/-)后代中母体 OVA 特异性 IgG(1)的吸收水平比 FcRn(+/+)或 FcRn(+/-)后代低 10(3)-10(4)倍。令人惊讶的是,FcRn 表达也影响母体 IgE 的吸收。在 FcRn(+/+)和 FcRn(+/-)后代中检测到 OVA 特异性 IgE,但在 FcRn(-/-)后代中未检测到。在过敏寄养母亲中检测到 IgG(1)抗 IgE/IgE 免疫复合物,并且与 FcRn(+/+)和 FcRn(+/-)后代中的水平密切相关(ρ=0.88,P<0.0001)。此外,当用 IgG(1)抗 IgE 作为 IgG(1)抗 IgE/IgE 免疫复合物喂养时,FcRn 表达是新生小鼠吸收 TNP 特异性 IgE 所必需的。当用针对 Cε4 结构域的 IgG(1)抗 IgE 生成免疫复合物时,吸收的 IgE 能够在抗原依赖性嗜碱性粒细胞脱颗粒中发挥作用。
结论和临床相关性
这些数据表明 FcRn 可能通过一种新的机制促进 IgG 以外的母体抗体的吸收。这些发现具有临床相关性,因为 FcRn 介导母体 IgG 向胎儿的胎盘转运。这就提出了 FcRn 可能介导母体 IgE 作为 IgG 抗 IgE/IgE 免疫复合物向胎盘转运的可能性。
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