A Refined Human Linear B Cell Epitope Map of Outer Surface Protein C (OspC) From the Lyme Disease Spirochete, Borrelia Burgdorferi.

Q1 Medicine
Pathogens and Immunity Pub Date : 2025-02-14 eCollection Date: 2024-01-01 DOI:10.20411/pai.v10i1.756
Grace Freeman-Gallant, Kathleen McCarthy, Jennifer Yates, Karen Kulas, Michael J Rudolph, David J Vance, Nicholas J Mantis
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Abstract

Background: A detailed understanding of the human antibody response to outer surface protein C (OspC) of Borrelia burgdorferi has important implications for Lyme disease diagnostics and vaccines.

Methods: In this report, 13 peptides encompassing 8 reported OspC linear B-cell epitopes from OspC types A, B, and K, including the largely conserved C-terminus (residues 193-210), were evaluated by multiplex immunoassay (MIA) for IgG reactivity with ~700 human serum samples confirmed positive in a 2-tiered Lyme disease diagnostic assay (Bb+) and ~160 post-treatment Lyme disease (PTLD) serum samples. The vmp-like sequence E (VlsE) C6-17 peptide was included as a positive control.

Results: Serum IgG from Bb+ samples were reactive with 10 of the 13 OspC-derived peptides tested, with the C-terminal peptide (residues 193-210) being the most reactive. Spearman's rank correlation matrices and hierarchical clustering revealed a strong correlation between 193-210 and VlsE C6-17 peptide reactivity but little demonstrable association between 193-210 and the other OspC peptides or recombinant OspC. OspC peptide reactivities (excluding 193-210) were strongly correlated with each other and were disproportionately influenced by a subset of pan-reactive samples. In the PTLD sample set, none of the OspC-derived peptides were significantly reactive over baseline, even though VlsE C6-17 peptide reactivity remained.

Conclusions: The asynchronous and potentially short-lived serologic response to OspC-derived peptides reveals the complexity of B-cell responses to B. burgdorferi lipoproteins and confounds interpretation of antibody profiles for Lyme disease diagnostics.

莱姆病螺旋体伯氏疏螺旋体外表面蛋白C (OspC)的精炼人线性B细胞表位图
背景:详细了解人抗体对伯氏疏螺旋体外表面蛋白C (OspC)的反应对莱姆病的诊断和疫苗具有重要意义。方法:在本报告中,采用多重免疫分析法(MIA)对来自A、B和K型OspC的8个已报道的OspC线性B细胞表位(包括大部分保守的c端(残基193-210))的13个多肽进行IgG反应性评估,其中约700份人血清样本在2层莱姆病诊断试验(Bb+)和约160份治疗后莱姆病(PTLD)血清样本中证实为阳性。将vmp样序列E (VlsE) C6-17肽作为阳性对照。结果:Bb+样品的血清IgG与13种ospc衍生肽中的10种具有反应性,其中c端肽(残基193-210)反应性最强。Spearman秩相关矩阵和层次聚类分析显示,193-210与VlsE C6-17肽反应性有较强的相关性,而193-210与其他OspC肽或重组OspC的相关性不明显。OspC肽的反应性(不包括193-210)彼此之间有很强的相关性,并且不成比例地受到一部分泛反应样品的影响。在PTLD样本集中,尽管VlsE C6-17肽的反应性仍然存在,但没有任何ospc衍生肽在基线上具有明显的反应性。结论:对ospc衍生肽的非同步且可能短暂的血清学反应揭示了b细胞对伯氏疏螺旋体脂蛋白反应的复杂性,并混淆了对莱姆病诊断的抗体谱的解释。
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
Pathogens and Immunity
Pathogens and Immunity Medicine-Infectious Diseases
CiteScore
10.60
自引率
0.00%
发文量
16
审稿时长
10 weeks
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