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血清表位谱分析可提高敏感性,以可扩展的多重格式实现莱姆病的早期检测。

Serum Epitope Repertoire Analysis Enables Early Detection of Lyme Disease with Improved Sensitivity in an Expandable Multiplex Format.

机构信息

Serimmune Inc., Goleta, California, USA.

Lyme Disease Biobank, Portland, Oregon, USA.

出版信息

J Clin Microbiol. 2021 Jan 21;59(2). doi: 10.1128/JCM.01836-20.

Abstract

Widely employed diagnostic antibody serology for Lyme disease, known as standard two-tier testing (STTT), exhibits insufficient sensitivity in early Lyme disease, yielding many thousands of false-negative test results each year. Given this problem, we applied serum antibody repertoire analysis (SERA), or next-generation sequencing (NGS)-based serology, to discover IgG and IgM antibody epitope motifs capable of detecting Lyme disease-specific antibodies with high sensitivity and specificity. Iterative motif discovery and bioinformatic analysis of epitope repertoires from subjects with Lyme disease ( = 264) and controls ( = 391) yielded a set of 28 epitope motifs representing 20 distinct IgG antibody epitopes and a set of 38 epitope motifs representing 21 distinct IgM epitopes, which performed equivalently in a large validation cohort of STTT-positive samples. In a second validation set from subjects with clinically defined early Lyme disease ( = 119) and controls ( = 257), the SERA Lyme IgG and IgM assay exhibited significantly improved sensitivity relative to STTT (77% versus 62%; Z-test;  = 0.013) and improved specificity (99% versus 97%). Early Lyme disease subjects exhibited significantly fewer reactive epitopes (Mann-Whitney U test;  < 0.0001) relative to subjects with Lyme arthritis. Thus, SERA Lyme IgG and M panels provided increased accuracy in early Lyme disease in a readily expandable multiplex assay format.

摘要

广泛应用于莱姆病诊断的抗体血清学检测,即标准两阶段检测(STTT),在早期莱姆病中表现出敏感性不足,每年产生数千个假阴性检测结果。鉴于这一问题,我们应用血清抗体谱分析(SERA)或基于下一代测序(NGS)的血清学方法,以发现能够高灵敏度和特异性检测莱姆病特异性抗体的 IgG 和 IgM 抗体表位基序。对莱姆病患者( = 264)和对照组( = 391)的血清抗体谱进行反复的基序发现和生物信息学分析,产生了一组 28 个代表 20 个不同 IgG 抗体表位的表位基序和一组 38 个代表 21 个不同 IgM 表位的表位基序,它们在大量 STTT 阳性样本的验证队列中表现相当。在来自具有临床定义的早期莱姆病患者( = 119)和对照组( = 257)的第二个验证组中,SERA 莱姆 IgG 和 IgM 检测在敏感性方面显著优于 STTT(77%对 62%;Z 检验;  = 0.013),特异性也有所提高(99%对 97%)。与莱姆关节炎患者相比,早期莱姆病患者的反应性表位明显较少(Mann-Whitney U 检验;  < 0.0001)。因此,SERA 莱姆 IgG 和 M 谱在易于扩展的多重检测格式中,为早期莱姆病提供了更高的准确性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7771/8111119/d3d904354830/JCM.01836-20-f0003.jpg

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