Center for Experimental and Molecular Medicine, Academic Medical Center, University of Amsterdam, Amsterdam, The Netherlands.
Central Research Institute of Epidemiology, Moscow, Russia.
Clin Microbiol Infect. 2018 Dec;24(12):1338.e1-1338.e7. doi: 10.1016/j.cmi.2018.03.009. Epub 2018 Mar 14.
Borrelia miyamotoi disease (BMD) is an emerging tick-borne disease in the Northern hemisphere. Serodiagnosis by measuring antibodies against glycerophosphodiester-phosphodiesterase (GlpQ) has been performed experimentally but has not been extensively clinically validated. Because we had previously shown the differential expression of antigenic variable major proteins (Vmps) in B. miyamotoi, our aim was to study antibody responses against GlpQ and Vmps in PCR-proven BMD patients and controls.
We assessed seroreactivity against GlpQ and four Vmps in a well-described, longitudinal cohort of sera from BMD patients (n=182), healthy blood donors (n=136) and controls (n=68). All samples were tested by ELISA and positive sera were tested by western blot, and antibody dynamics and diagnostic value were assessed.
IgM antibodies against GlpQ and Vmps peaked between 11 and 20 days, and IgG between 21 and 50 days, after disease onset. Various combinations of GlpQ and Vmps increased sensitivity and/or specificity compared to single antigens. Notably, the GlpQ or variable large protein (Vlp)-15/16 combination yielded a sensitivity of 94.7% (95% CI: 75.4-99.7) 11-20 days after disease onset and a specificity of 96.6% (92.7-98.4) for IgM. A specificity of 100% (97.8-100) for IgM, and 98.3% for IgG (95.2-100), was found when positivity was defined as reactivity to GlpQ and any Vmp, with maximum sensitivities of 79% (56.7-91.5) for IgM and 86.7% (62.1-97.6) for IgG.
We clearly demonstrate here the diagnostic potential of these seromarkers. Our findings will facilitate future epidemiological and clinical studies on BMD and lead to the development of a serologic test to be used in clinical practice.
伯氏疏螺旋体病(BMD)是一种在北半球新兴的蜱传疾病。通过测量针对甘油磷酸二酯-磷酸二酯酶(GlpQ)的抗体进行血清学诊断已在实验中进行,但尚未广泛进行临床验证。因为我们之前已经显示出抗原可变主要蛋白(Vmps)在伯氏疏螺旋体中的差异表达,所以我们的目的是研究 PCR 证实的 BMD 患者和对照者中针对 GlpQ 和 Vmps 的抗体反应。
我们评估了来自 BMD 患者(n=182)、健康献血者(n=136)和对照者(n=68)的纵向队列中经描述良好的血清中针对 GlpQ 和四个 Vmps 的血清反应性。所有样品均通过 ELISA 进行检测,阳性血清通过 Western blot 进行检测,并评估了抗体动力学和诊断价值。
IgM 抗体针对 GlpQ 和 Vmps 的峰值分别出现在疾病发作后 11 至 20 天和 21 至 50 天,而 IgG 则在 21 至 50 天之间出现。与单个抗原相比,GlpQ 和 Vmps 的各种组合增加了敏感性和/或特异性。值得注意的是,GlpQ 或可变大蛋白(Vlp)-15/16 组合在疾病发作后 11-20 天的敏感性为 94.7%(95%CI:75.4-99.7),特异性为 96.6%(92.7-98.4)为 IgM。当将阳性定义为对 GlpQ 和任何 Vmp 的反应性时,IgM 的特异性为 100%(97.8-100),IgG 的特异性为 98.3%(95.2-100),IgM 的最大敏感性为 79%(56.7-91.5),IgG 的最大敏感性为 86.7%(62.1-97.6)。
我们在这里清楚地证明了这些血清标志物的诊断潜力。我们的发现将促进未来对 BMD 的流行病学和临床研究,并导致开发用于临床实践的血清学检测方法。
