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迈向理解布鲁氏菌抗原-抗体特异性的基础

Towards Understanding the Basis of Brucella Antigen-Antibody Specificity.

作者信息

Sood Amika, Bundle David R, Woods Robert J

机构信息

Complex Carbohydrate Research Center, University of Georgia, Athens, GA 30602, USA.

Department of Chemistry, University of Alberta, Edmonton, AB T6G 2R3, Canada.

出版信息

Molecules. 2025 Jul 9;30(14):2906. doi: 10.3390/molecules30142906.

Abstract

Brucellosis continues to be a significant global zoonotic infection, with diagnosis largely relying on the detection of antibodies against the Brucella O-polysaccharide (O-PS) A and M antigens. In this study, computational methods, including homology modeling, molecular docking, and molecular dynamics simulations, were applied to investigate the interaction of the four murine monoclonal antibodies (mAbs) YsT9.1, YsT9.2, Bm10, and Bm28 with hexasaccharide fragments of the A and M epitopes. Through stringent stability criteria, based on interaction energies and mobility of the antigens, high-affinity binding of A antigen with YsT9.1 antibody and M antigen with Bm10 antibody was predicted. In both the complexes hydrophobic interactions dominate the antigen-antibody binding. These findings align well with experimental epitope mapping, indicating YsT9.1's preference for internal sequences of the A epitope and Bm10's preference for internal elements of the M epitope. Interestingly, no stable complexes were identified for YsT9.2 or Bm28 interacting with A or M antigen. This study provides valuable insights into the mechanism of molecular recognition of Brucella O-antigens that can be applied for the development of improved diagnostics, synthetic glycomimetics, and improved vaccine strategies.

摘要

布鲁氏菌病仍然是一种重要的全球人畜共患感染病,其诊断很大程度上依赖于检测针对布鲁氏菌O-多糖(O-PS)A和M抗原的抗体。在本研究中,应用了包括同源建模、分子对接和分子动力学模拟在内的计算方法,来研究四种鼠单克隆抗体(mAb)YsT9.1、YsT9.2、Bm10和Bm28与A和M表位的六糖片段之间的相互作用。通过基于抗原的相互作用能和流动性的严格稳定性标准,预测了A抗原与YsT9.1抗体以及M抗原与Bm10抗体的高亲和力结合。在这两种复合物中,疏水相互作用主导着抗原-抗体结合。这些发现与实验性表位作图结果非常吻合,表明YsT9.1对A表位内部序列的偏好以及Bm10对M表位内部元件的偏好。有趣的是,未发现YsT9.2或Bm28与A或M抗原相互作用形成稳定的复合物。本研究为布鲁氏菌O抗原的分子识别机制提供了有价值的见解,可应用于改进诊断方法、合成糖模拟物以及改进疫苗策略的开发。

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