Discovery, recognized antigenic structures, and evolution of cross-serotype broadly neutralizing antibodies from porcine B-cell repertoires against foot-and-mouth disease virus.

IF 5.5 1区 医学 Q1 MICROBIOLOGY PLoS Pathogens Pub Date : 2024-10-15 eCollection Date: 2024-10-01 DOI:10.1371/journal.ppat.1012623
Fengjuan Li, Shanquan Wu, Lv Lv, Shulun Huang, Zelin Zhang, Zhaxi Zerang, Pinghua Li, Yimei Cao, Huifang Bao, Pu Sun, Xingwen Bai, Yong He, Yuanfang Fu, Hong Yuan, Xueqing Ma, Zhixun Zhao, Jing Zhang, Jian Wang, Tao Wang, Dong Li, Qiang Zhang, Jijun He, Zaixin Liu, Zengjun Lu, Dongsheng Lei, Kun Li
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Abstract

It is a great challenge to isolate the broadly neutralizing antibodies (bnAbs) against foot-and-mouth disease virus (FMDV) due to its existence as seven distinct serotypes without cross-protection. Here, by vaccination of pig with FMDV serotypes O and A whole virus antigens, we obtained 10 bnAbs against serotypes O, A and/or Asia1 by dissecting 216 common clonotypes of two serotypes O and A specific porcine B-cell receptor (BCR) gene repertoires containing total 12720 B cell clones, indicating the induction of cross-serotype bnAbs after sequential vaccination with serotypes O and A antigens. The majority of porcine bnAbs (9/10) were derived from terminally differentiated B cells of different clonal lineages, which convergently targeted the conserved "RGDL" motif on structural protein VP1 of FMDV by mimicking receptor recognition to inhibit viral attachment to cells. Cryo-EM complex structures revealed that the other bnAb pOA-2 specifically targets a novel inter-pentamer antigen structure surrounding the viral three-fold axis, with a highly conserved determinant at residue 68 on VP2. This unique binding pattern enabled cross-serotype neutralization by destabilizing the viral particle. The evolutionary analysis of pOA-2 demonstrated its origin from an intermediate B-cell, emphasizing the crucial role of somatic hypermutations (SHMs) in balancing the breadth and potency of neutralization. However, excessive SHMs may deviate from the trajectory of broad neutralization. This study provides a strategy to uncover bnAbs against highly mutable pathogens and the cross-serotype antigenic structures to explore broadly protective FMDV vaccine.

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猪 B 细胞库中针对口蹄疫病毒的跨血清型广谱中和抗体的发现、识别抗原结构和进化。
由于口蹄疫病毒(FMDV)有七个不同的血清型,且无交叉保护,因此分离针对口蹄疫病毒的广泛中和抗体(bnAbs)是一项巨大的挑战。在此,我们用FMDV血清型O和A全病毒抗原对猪进行免疫接种,通过剖析两个血清型O和A特异性猪B细胞受体(BCR)基因组的216个共同克隆(共包含12720个B细胞克隆),获得了10种针对血清型O、A和/或Asia1的bnAbs,表明在连续接种血清型O和A抗原后可诱导出跨血清型的bnAbs。大多数猪 bnAbs(9/10)来自不同克隆系的终末分化 B 细胞,它们通过模拟受体识别,以 FMDV 结构蛋白 VP1 上保守的 "RGDL "基序为靶点,抑制病毒对细胞的附着。低温电子显微镜复合物结构显示,另一种 bnAb pOA-2 专门针对病毒三折轴周围的新型五聚体间抗原结构,其高度保守的决定簇位于 VP2 上的第 68 个残基。这种独特的结合模式通过破坏病毒颗粒的稳定性实现了跨血清型中和。pOA-2 的进化分析表明它起源于中间 B 细胞,强调了体细胞超突变(SHM)在平衡中和的广度和效力方面的关键作用。然而,过多的SHMs可能会偏离广泛中和的轨迹。这项研究提供了一种策略来发现针对高度变异病原体的 bnAbs 以及跨血清型抗原结构,从而探索具有广泛保护性的 FMDV 疫苗。
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PLoS Pathogens
PLoS Pathogens MICROBIOLOGY-PARASITOLOGY
自引率
3.00%
发文量
598
期刊介绍: Bacteria, fungi, parasites, prions and viruses cause a plethora of diseases that have important medical, agricultural, and economic consequences. Moreover, the study of microbes continues to provide novel insights into such fundamental processes as the molecular basis of cellular and organismal function.
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