Lyme disease serodiagnosis has limited early sensitivity and cannot distinguish active from past infections. To address this, we screen a Borrelia afzelii whole-proteome microarray (1,296 proteins) using human (n = 149) and murine (n = 32) sera. We evaluate three early-stage antigens-BafPKo_A0001, BafPKo_D0016, and BafPKo_A0029. ELISA cutoffs are established using discovery cohort sera (n = 99) and validated with the validation (n = 242) and the prospective (n = 223) cohorts. A0001 demonstrates 87.8% sensitivity, outperforming C6 (69.4%) and STTT (22.5%) in the discovery cohort. In the validation cohort, A0001 reaches 90.5% sensitivity, surpassing C6 by 11.6% and STTT by 50%. In hyper-acute erythema migrans sera (from the prospective cohort), A0001 achieves 55.1% sensitivity, exceeding C6 and STTT by 14.6% and 33.3%, respectively. COMBO-3 and COMBO-2 yield the highest sensitivity of 92.9% and 66.1% in the validation and prospective cohort, respectively. A0001 and D0016 show enhanced and robust seroreversion after antibiotic treatment suggesting their potential as test of cure biomarkers in early Lyme disease.
Diagnostic validation of novel Borrelia antigens discovered by whole-proteome microarray: Advancing early detection and test of cure for Lyme disease.
利用全蛋白质组微阵列技术对新发现的伯氏疏螺旋体抗原进行诊断验证:推进莱姆病的早期检测和治愈试验
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作者:Nayak Abhijeet, Baarsma M E, van Eck Jacqueline A, Randall Arlo Z, Ursinus Jeanine, Teng Andy A, Pablo Jozelyn V, Hung Chris, Wopereis Doris U M, van de Schoor Freek, Popa Calin D, van den Wijngaard Cees C, Kullberg Bart-Jan, Joosten Leo A B, Kuiper Herman, Campo Joseph J, Liang Xiaouw, Hovius Joppe W
| 期刊: | Cell Reports Medicine | 影响因子: | 10.600 |
| 时间: | 2025 | 起止号: | 2025 May 20; 6(5):102097 |
| doi: | 10.1016/j.xcrm.2025.102097 | 研究方向: | 免疫/内分泌 |
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