Ovchinnikova Leyla A, Eliseev Igor E, Dzhelad Samir S, Simaniv Taras O, Klimina Ksenia M, Ivanova Maria, Ilina Elena N, Zakharova Maria N, Illarioshkin Sergey N, Rubtsov Yury P, Gabibov Alexander G, Lomakin Yakov A
Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, Moscow, Russia.
St. Petersburg School of Physics, Mathematics, and Computer Science, HSE University, Saint Petersburg, Russia.
Front Immunol. 2024 Nov 28;15:1401156. doi: 10.3389/fimmu.2024.1401156. eCollection 2024.
Multiple sclerosis (MS) is a neuroinflammatory disease triggered by a combination of genetic traits and external factors. Autoimmune nature of MS is proven by the identification of pathogenic T cells, but the role of autoantibody-producing B cells is less clear. A comprehensive understanding of the development of neuroinflammation and the identification of targeted autoantigens are crucial for timely diagnosis and appropriate treatment.
An expression library of 44-mer overlapping peptides from a panel of putative autoantigenic human proteins was employed for modified Phage ImmunoPrecipitation Sequencing (PhIP-Seq) to identify B cell peptide epitopes from MS patients. Individual peptides extracted by PhIP-Seq were tested by ELISA to characterize their affinity towards IgG from both MS patients and healthy donors (HD). Three candidate auto-peptides were used for isolating autoreactive antigen-specific IgGs from the serum of MS patients.
Autoantibody screening revealed high heterogeneity of IgG response in MS. The autoantigenic genesis of the PhIP-Seq-identified peptides was further strengthened by clinical ELISA testing of 11 HD and 16 MS donors. Validation experiments on independent cohorts of 22 HD and 28 MS patients confirmed statistically significant elevated titers of IgG specific to spectrin alpha chain (SPTAN1) in the serum of MS patients compared to HD. The levels of anti-SPTAN1 IgG correlated in serum and cerebrospinal fluid (CSF). Isolated autoreactive antigen-specific IgG exhibited increased cross-reactivity to a panel of PhIP-Seq-identified antigenic peptides. Serum IgG from MS patients were reactive to latent membrane protein (LMP1) of Epstein-Barr virus, a potential trigger of MS. Discovered antigenic peptides from SPTAN1, protein-tyrosine kinase 6 (PTK6), periaxin (PRX), and LMP1 were tested as potential biomarker panel for MS diagnostics. We concluded that the combination of particular peptides from SPTAN1, PTK6, PRX and LMP1 could be implemented as a four-peptide biomarker panel for MS diagnosis (area under the curve (AUC) of 0.818 for discriminating between HD and MS).
This study supports the concept that the specificity of autoreactive IgG in MS is highly heterogeneous. Despite that we suggest that the combination of several B-cell epitopes could be employed as reliable and simple test for MS diagnostics.
多发性硬化症(MS)是一种由遗传特征和外部因素共同引发的神经炎症性疾病。致病性T细胞的鉴定证实了MS的自身免疫性质,但产生自身抗体的B细胞的作用尚不清楚。全面了解神经炎症的发展过程并确定靶向自身抗原对于及时诊断和恰当治疗至关重要。
利用一组假定的人类自身抗原蛋白的44聚体重叠肽表达文库进行改良噬菌体免疫沉淀测序(PhIP-Seq),以鉴定MS患者的B细胞肽表位。通过PhIP-Seq提取的单个肽通过酶联免疫吸附测定(ELISA)进行测试,以表征其对MS患者和健康供体(HD)的IgG的亲和力。使用三种候选自身肽从MS患者血清中分离自身反应性抗原特异性IgG。
自身抗体筛查显示MS中IgG反应具有高度异质性。对11名HD和16名MS供体进行的临床ELISA检测进一步强化了PhIP-Seq鉴定的肽的自身抗原起源。对22名HD和28名MS患者的独立队列进行的验证实验证实,与HD相比,MS患者血清中血影蛋白α链(SPTAN1)特异性IgG的滴度在统计学上显著升高。血清和脑脊液(CSF)中抗SPTAN1 IgG的水平相关。分离出的自身反应性抗原特异性IgG对一组PhIP-Seq鉴定的抗原肽表现出增加的交叉反应性。MS患者的血清IgG对爱泼斯坦-巴尔病毒的潜伏膜蛋白(LMP1)有反应,LMP1是MS的潜在触发因素。测试了从SPTAN1、蛋白酪氨酸激酶6(PTK6)、外周蛋白(PRX)和LMP1中发现的抗原肽作为MS诊断的潜在生物标志物组合。我们得出结论,来自SPTAN1、PTK6、PRX和LMP1的特定肽的组合可作为MS诊断的四肽生物标志物组合实施(区分HD和MS的曲线下面积(AUC)为0.818)。
本研究支持MS中自身反应性IgG的特异性高度异质的概念。尽管如此,我们建议几种B细胞表位的组合可作为MS诊断的可靠且简单的检测方法。
