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新生儿Fc受体对人IgG在小鼠体内生物分布的影响。

The effect of the neonatal Fc receptor on human IgG biodistribution in mice.

作者信息

Chen Nancy, Wang Weirong, Fauty Scott, Fang Yulin, Hamuro Lora, Hussain Azher, Prueksaritanont Thomayant

机构信息

Department of Pharmacokinetics, Pharmacodynamics, and Drug Metabolism; Merck Research Laboratories; West Point, PA USA.

Department of Laboratory Animal Resources; Merck Research Laboratories; West Point, PA USA.

出版信息

MAbs. 2014 Mar-Apr;6(2):502-8. doi: 10.4161/mabs.27765. Epub 2014 Jan 9.

Abstract

The neonatal Fc receptor (FcRn) plays a pivotal role in IgG homeostasis, i.e., it salvages IgG antibodies from lysosomal degradation following fluid-phase pinocytosis, thus preventing rapid systemic elimination of IgG. Recombinant therapeutic antibodies are typically composed of human or humanized sequences, and their biodistribution, or tissue distribution, is often studied in murine models, although, the effect of FcRn on tissue distribution of human IgG in rodents has not been investigated. In this report, an (125)I-labeled human IgG1 antibody was studied in both wild type C57BL/6 (WT) and FcRn knockout (KO) mice. Total radioactivity in both plasma and tissues (0-96hr post-dose) was measured by gamma-counting. Plasma exposure of human IgG1 were significantly lower in FcRn KO mice, which is consistent with the primary function of FcRn. Differences in biodistribution of human IgG to selected tissues were also observed. Among the tissue examined, the fat, skin and muscle showed a decrease in tissue-to-blood (T/B) exposure ratio of human IgG1 in FcRn KO mice comparing to the WT mice, while the liver, spleen, kidney, and lung showed an increase in the T/B exposure ratio in FcRn KO mice. A time-dependent change in the T/B ratios of human IgG1 was also observed for many tissues in FcRn KO mice. These results suggest that, in addition to its role in IgG elimination, FcRn may also play a role in antibody biodistribution.

摘要

新生儿Fc受体(FcRn)在IgG稳态中起关键作用,即它能从液相胞饮作用后的溶酶体降解中挽救IgG抗体,从而防止IgG在体内快速清除。重组治疗性抗体通常由人源或人源化序列组成,其生物分布或组织分布常通过小鼠模型进行研究,然而,FcRn对啮齿动物体内人IgG组织分布的影响尚未得到研究。在本报告中,研究人员使用了(125)I标记的人IgG1抗体在野生型C57BL/6(WT)小鼠和FcRn基因敲除(KO)小鼠体内进行实验。通过γ计数测量给药后0至96小时血浆和组织中的总放射性。FcRn基因敲除小鼠中,人IgG1的血浆暴露量显著降低,这与FcRn的主要功能一致。同时还观察到了人IgG在选定组织中的生物分布差异。在检测的组织中,与野生型小鼠相比,FcRn基因敲除小鼠的脂肪、皮肤和肌肉中,人IgG1的组织与血液(T/B)暴露比降低,而肝脏、脾脏、肾脏和肺中,FcRn基因敲除小鼠的T/B暴露比增加。在FcRn基因敲除小鼠的许多组织中,还观察到了人IgG1的T/B比值随时间的变化。这些结果表明,FcRn除了在IgG清除中发挥作用外,可能还在抗体生物分布中起作用。

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