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生成、多样性测定及人源天然 Fab 库在抗体选择中的应用。

Generation, Diversity Determination, and Application to Antibody Selection of a Human Naïve Fab Library.

机构信息

Department of Systems Immunology, College of Biomedical Science, Kangwon National University, Chuncheon 24341, Korea.

Therapeutic Antibody Research Center, Korea Research Institute of Bioscience and Biotechnology, Daejeon 34141, Korea.

出版信息

Mol Cells. 2017 Sep 30;40(9):655-666. doi: 10.14348/molcells.2017.0106. Epub 2017 Sep 20.

Abstract

We constructed a large naïve human Fab library (3 × 10 colonies) from the lymphocytes of 809 human donors, assessed available diversities of the heavy-chain variable (VH) and κ light-chain variable (VK) domain repertoires, and validated the library by selecting Fabs against 10 therapeutically relevant antigens by phage display. We obtained a database of unique 7,373 VH and 41,804 VK sequences by 454 pyrosequencing, and analyzed the repertoires. The distribution of VH and VK subfamilies and germline genes in our antibody repertoires slightly differed from those in earlier published natural antibody libraries. The frequency of somatic hypermutations (SHMs) in heavy-chain complementarity determining region (HCDR)1 and HCDR2 are higher compared with the natural IgM repertoire. Analysis of position-specific SHMs in CDRs indicates that asparagine, threonine, arginine, aspartate and phenylalanine are the most frequent non-germline residues on the antibody-antigen interface and are converted mostly from the germline residues, which are highly represented in germline SHM hotspots. The amino acid composition and length-dependent changes in amino acid frequencies of HCDR3 are similar to those in previous reports, except that frequencies of aspartate and phenylalanine are a little higher in our repertoire. Taken together, the results show that this antibody library shares common features of natural antibody repertoires and also has unique features. The antibody library will be useful in the generation of human antibodies against diverse antigens, and the information about the diversity of natural antibody repertoires will be valuable in the future design of synthetic human antibody libraries with high functional diversity.

摘要

我们构建了一个来自 809 位人类供体淋巴细胞的大型初始人类 Fab 文库(3×10 个克隆),评估了重链可变区(VH)和κ轻链可变区(VK)的可用多样性,并用噬菌体展示筛选针对 10 种治疗相关抗原的 Fab 对文库进行了验证。我们通过 454 焦磷酸测序获得了一个由 7373 个 VH 和 41804 个 VK 序列组成的独特数据库,并对这些序列进行了分析。我们抗体库中 VH 和 VK 亚家族和胚系基因的分布与早期发表的天然抗体文库略有不同。与天然 IgM 库相比,重链互补决定区(HCDR)1 和 HCDR2 中的体细胞高频突变(SHM)频率更高。CDR 中位置特异性 SHM 的分析表明,天冬酰胺、苏氨酸、精氨酸、天冬氨酸和苯丙氨酸是抗体-抗原界面上最常见的非胚系残基,并且主要由高度代表胚系 SHM 热点的胚系残基转换而来。HCDR3 的氨基酸组成和长度依赖性氨基酸频率变化与以前的报告相似,但在我们的文库中,天冬氨酸和苯丙氨酸的频率略高。总之,这些结果表明,该抗体文库具有天然抗体库的共同特征,也具有独特的特征。该抗体文库将有助于针对多种抗原产生人类抗体,并且关于天然抗体库多样性的信息对于未来设计具有高功能多样性的合成人类抗体库将是有价值的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5af0/5638773/c1389f7909df/molce-40-9-655f1.jpg

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