High-resolution epitope mapping of commercial antibodies to ANCA antigens by yeast surface display

IF 1.6 4区医学 Q4 BIOCHEMICAL RESEARCH METHODS

Journal of immunological methods Pub Date : 2024-03-01 DOI:10.1016/j.jim.2024.113654

John S. Poulton , Sajan Lamba , Meghan Free , Gang Xi , Elizabeth McInnis , Gabrielle Williams , Stephan T. Kudlacek , David Thieker , Brian Kuhlman , Ronald Falk

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引用次数: 0

Abstract

Epitope mapping provides critical insight into antibody-antigen interactions. Epitope mapping of autoantibodies from patients with autoimmune diseases can help elucidate disease immunogenesis and guide the development of antigen-specific therapies. Similarly, epitope mapping of commercial antibodies targeting known autoantigens enables the use of those antibodies to test specific hypotheses. Anti-Neutrophil Cytoplasmic Autoantibody (ANCA) vasculitis results from the formation of autoantibodies to multiple autoantigens, including myeloperoxidase (MPO), proteinase-3 (PR3), plasminogen (PLG), and peroxidasin (PXDN). To perform high-resolution epitope mapping of commercial antibodies to these autoantigens, we developed a novel yeast surface display library based on a series of >5000 overlapping peptides derived from their protein sequences. Using both FACS and magnetic bead isolation of reactive yeast, we screened 19 commercially available antibodies to the ANCA autoantigens. This approach to epitope mapping resulted in highly specific, fine epitope mapping, down to single amino acid resolution in many cases. Our study also identified cross-reactivity between some commercial antibodies to MPO and PXDN, which suggests that patients with apparent autoantibodies to both proteins may be the result of cross-reactivity. Together, our data validate yeast surface display using maximally overlapping peptides as an excellent approach to linear epitope mapping.

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通过酵母表面展示法绘制 ANCA 抗原商用抗体的高分辨率表位图。

表位图谱为了解抗体与抗原之间的相互作用提供了重要依据。绘制自身免疫疾病患者自身抗体的表位图有助于阐明疾病的免疫发生，并指导抗原特异性疗法的开发。同样，针对已知自身抗原的商业抗体的表位图谱也可以用来测试特定的假设。抗中性粒细胞胞浆自身抗体（ANCA）血管炎是由针对多种自身抗原的自身抗体形成的，这些自身抗原包括髓过氧化物酶（MPO）、蛋白酶-3（PR3）、纤溶酶原（PLG）和过氧化物酶原（PXDN）。为了对这些自身抗原的商用抗体进行高分辨率表位图谱绘制，我们开发了一种新型酵母表面展示文库，该文库基于从其蛋白质序列中提取的一系列大于 5000 个重叠肽段。通过使用 FACS 和磁珠分离反应酵母，我们筛选出了 19 种针对 ANCA 自身抗原的市售抗体。这种表位图谱绘制方法可绘制出高度特异、精细的表位图谱，在许多情况下可达到单氨基酸分辨率。我们的研究还发现了一些 MPO 和 PXDN 商用抗体之间的交叉反应，这表明对这两种蛋白都有明显自身抗体的患者可能是交叉反应的结果。总之，我们的数据验证了使用最大重叠肽进行酵母表面展示是线性表位图谱绘制的绝佳方法。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of immunological methods 医学-免疫学

CiteScore

4.10

自引率

0.00%

发文量

120

审稿时长

3 months

期刊介绍： The Journal of Immunological Methods is devoted to covering techniques for: (1) Quantitating and detecting antibodies and/or antigens. (2) Purifying immunoglobulins, lymphokines and other molecules of the immune system. (3) Isolating antigens and other substances important in immunological processes. (4) Labelling antigens and antibodies. (5) Localizing antigens and/or antibodies in tissues and cells. (6) Detecting, and fractionating immunocompetent cells. (7) Assaying for cellular immunity. (8) Documenting cell-cell interactions. (9) Initiating immunity and unresponsiveness. (10) Transplanting tissues. (11) Studying items closely related to immunity such as complement, reticuloendothelial system and others. (12) Molecular techniques for studying immune cells and their receptors. (13) Imaging of the immune system. (14) Methods for production or their fragments in eukaryotic and prokaryotic cells. In addition the journal will publish articles on novel methods for analysing the organization, structure and expression of genes for immunologically important molecules such as immunoglobulins, T cell receptors and accessory molecules involved in antigen recognition, processing and presentation. Submitted full length manuscripts should describe new methods of broad applicability to immunology and not simply the application of an established method to a particular substance - although papers describing such applications may be considered for publication as a short Technical Note. Review articles will also be published by the Journal of Immunological Methods. In general these manuscripts are by solicitation however anyone interested in submitting a review can contact the Reviews Editor and provide an outline of the proposed review.