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靶向人新生儿 Fc 受体的纳米抗体的筛选。

Selection of nanobodies that target human neonatal Fc receptor.

机构信息

Centre for Immune Regulation (CIR) and Department of Molecular Biosciences, University of Oslo, Oslo, Norway.

出版信息

Sci Rep. 2013;3:1118. doi: 10.1038/srep01118. Epub 2013 Jan 23.

Abstract

FcRn is a key player in several immunological and non-immunological processes, as it mediates maternal-fetal transfer of IgG, regulates the serum persistence of IgG and albumin, and transports both ligands between different cellular compartments. In addition, FcRn enhances antigen presentation. Thus, there is an intense interest in studies of how FcRn binds and transports its cargo within and across several types of cells, and FcRn detection reagents are in high demand. Here we report on phage display-selected Nanobodies that target human FcRn. The Nanobodies were obtained from a variable-domain repertoire library isolated from a llama immunized with recombinant human FcRn. One candidate, Nb218-H4, was shown to bind FcRn with high affinity at both acidic and neutral pH, without competing ligand binding and interfering with FcRn functions, such as transcytosis of IgG. Thus, Nb218-H4 can be used as a detection probe and as a tracker for visualization of FcRn-mediated cellular transport.

摘要

FcRn 是几个免疫和非免疫过程中的关键参与者,因为它介导 IgG 的母婴转移,调节 IgG 和白蛋白的血清半衰期,并在不同的细胞区室之间运输这两种配体。此外,FcRn 增强抗原呈递。因此,人们对 FcRn 如何在多种类型的细胞内和细胞间结合和运输其货物的研究产生了浓厚的兴趣,并且对 FcRn 检测试剂的需求也很高。在这里,我们报告了通过噬菌体展示筛选出的针对人 FcRn 的 Nanobodies。这些 Nanobodies 是从用重组人 FcRn 免疫的骆驼的可变结构域库中分离出来的。一个候选物 Nb218-H4 被证明在酸性和中性 pH 下都能与 FcRn 高亲和力结合,而不与配体竞争结合并干扰 FcRn 的功能,如 IgG 的转胞吞作用。因此,Nb218-H4 可用作检测探针,并可用于可视化 FcRn 介导的细胞运输。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ec3/3552320/1c12cbf75123/srep01118-f1.jpg

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