A type-specific B-cell epitope at the apex of outer surface protein C (OspC) of the Lyme disease spirochete, Borreliella burgdorferi.

IF 3.7 2区生物学 Q2 MICROBIOLOGY

Microbiology spectrum Pub Date : 2025-04-01 Epub Date: 2025-02-14 DOI:10.1128/spectrum.02883-24

David J Vance, Grace Freeman-Gallant, Kathleen McCarthy, Carol Lyn Piazza, Yang Chen, Clint Vorauer, Beatrice Muriuki, Michael J Rudolph, Lisa Cavacini, Miklos Guttman, Nicholas J Mantis

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Abstract

Broadly protective immunity to the Lyme disease spirochete, Borreliella burgdorferi, is constrained by antibodies against type-specific epitopes on outer surface protein C (OspC), a homodimeric helix-rich lipoprotein essential for early stages of spirochete dissemination in vertebrate hosts. However, the molecular basis for type-specific immunity has not been fully elucidated. In this report, we produced and characterized an OspC mouse monoclonal antibody, 8C1, that recognizes native and recombinant OspC type A (OspC_A) but not OspC type B or K. Epitope mapping by hydrogen-deuterium exchange mass spectrometry (HDX-MS) localized 8C1's epitope to a protruding ridge on the apex of OspC_Aα-helix 3 (residues 130-150) previously known to be an immunodominant region of the molecule. Alanine scanning pinpointed 8C1's core binding motif to a solvent exposed patch consisting of residues K₁₄₁, H₁₄₂, T₁₄₃, and D₁₄₄. Analysis of 26 Lyme disease-positive serum samples confirmed human antibody reactivity with this region of OspC_A, with residues E₁₄₀ and D₁₄₄ as being the most consequential. Our results underscore the importance of α-helix 3 as a target of type-specific epitopes on OspC_A that should be taken into consideration in Lyme disease vaccine design.IMPORTANCEA central challenge in the development of vaccines against Lyme disease, the most common vector-borne infection in the United States, is the antigenically variable nature of the lipoproteins displayed on the surface of the disease-causing spirochete, Borreliella burgdorferi. For example, antibodies against one type of outer surface protein C (OspC), a lipoprotein involved in B. burgdorferi transmission and early stages of infection, may have little or no cross reactivity with another seemingly closely related variant of OspC, thereby hampering the use of a single OspC type as a vaccine antigen. For the sake of vaccine design, it is critical to identify the specific epitopes on OspC that both restrict and enable cross-reactivity.

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莱姆病螺旋体伯氏疏螺旋体外表面蛋白C （OspC）顶端的一种类型特异性b细胞表位。

针对莱姆病螺旋体伯氏疏螺旋体的广泛保护性免疫受到针对外表面蛋白C （OspC）上类型特异性表位的抗体的限制，OspC是一种同源二聚体富含螺旋的脂蛋白，在脊椎动物宿主中螺旋体传播的早期阶段至关重要。然而，类型特异性免疫的分子基础尚未完全阐明。在这篇报道中，我们制作并鉴定了一种OspC小鼠单克隆抗体8C1，它可以识别原生和重组OspCA型（OspCA），但不能识别OspC B型或k型。通过氢-氢交换质谱（HDX-MS）的表位定位，8C1的表位定位在OspCAα-螺旋3（残基130-150）顶端的突出脊上，这是先前已知的OspCA分子的免疫优势区。丙氨酸扫描将8C1的核心结合基序定位到由残基K141， H142， T143和D144组成的溶剂暴露补丁上。对26份莱姆病阳性血清样本的分析证实了人抗体与OspCA该区域的反应性，残基E140和D144是最重要的。我们的结果强调α-螺旋3作为OspCA上类型特异性表位靶标的重要性，在莱姆病疫苗设计中应加以考虑。莱姆病是美国最常见的媒介传播感染，在开发针对莱姆病疫苗方面的一个核心挑战是，在致病性螺旋体伯氏疏螺旋体表面显示的脂蛋白具有抗原性可变的性质。例如，针对一种外表面蛋白C （OspC）的抗体（OspC是一种参与伯氏疏螺旋体传播和感染早期阶段的脂蛋白）可能与另一种看似密切相关的OspC变体很少或没有交叉反应性，从而阻碍了单一OspC类型作为疫苗抗原的使用。为了疫苗设计的目的，确定OspC上既限制又允许交叉反应的特异性表位是至关重要的。

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

Microbiology spectrum Biochemistry, Genetics and Molecular Biology-Genetics

CiteScore

3.20

自引率

5.40%

发文量

1800

期刊介绍： Microbiology Spectrum publishes commissioned review articles on topics in microbiology representing ten content areas: Archaea; Food Microbiology; Bacterial Genetics, Cell Biology, and Physiology; Clinical Microbiology; Environmental Microbiology and Ecology; Eukaryotic Microbes; Genomics, Computational, and Synthetic Microbiology; Immunology; Pathogenesis; and Virology. Reviews are interrelated, with each review linking to other related content. A large board of Microbiology Spectrum editors aids in the development of topics for potential reviews and in the identification of an editor, or editors, who shepherd each collection.