Cortese Marianna, Leng Yumei, Bjornevik Kjetil, Mitchell Moriah, Healy Brian C, Mina Michael J, Mancuso James D, Niebuhr David W, Munger Kassandra L, Elledge Stephen J, Ascherio Alberto
Department of Nutrition, Harvard T. H. Chan School of Public Health, Boston, Massachusetts.
Division of Genetics, Department of Medicine, Howard Hughes Medical Institute, Brigham and Women's Hospital, Boston, Massachusetts.
JAMA Neurol. 2024 May 1;81(5):515-524. doi: 10.1001/jamaneurol.2024.0272.
It remains unclear why only a small proportion of individuals infected with the Epstein-Barr virus (EBV) develop multiple sclerosis (MS) and what the underlying mechanisms are.
To assess the serologic response to all EBV peptides before the first symptoms of MS occur, determine whether the disease is associated with a distinct immune response to EBV, and evaluate whether specific EBV epitopes drive this response.
DESIGN, SETTING, AND PARTICIPANTS: In this prospective, nested case-control study, individuals were selected among US military personnel with serum samples stored in the US Department of Defense Serum Repository. Individuals with MS had serum collected at a median 1 year before onset (reported to the military in 2000-2011) and were matched to controls for age, sex, race and ethnicity, blood collection, and military branch. No individuals were excluded. The data were analyzed between September 1, 2022, and August 31, 2023.
Antibodies (enrichment z scores) to the human virome measured using VirScan (phage-displayed immunoprecipitation and sequencing).
Rate ratios (RRs) for MS for antibodies to 2263 EBV peptides (the EBV peptidome) were estimated using conditional logistic regression, adjusting for total anti-EBV nuclear antigen 1 (EBNA-1) antibodies, which have consistently been associated with a higher MS risk. The role of antibodies against other viral peptides was also explored.
A total of 30 individuals with MS were matched with 30 controls. Mean (SD) age at sample collection was 27.8 (6.5) years; 46 of 60 participants (76.7%) were male. The antibody response to the EBV peptidome was stronger in individuals with MS, but without a discernible pattern. The antibody responses to 66 EBV peptides, the majority mapping to EBNA antigens, were significantly higher in preonset sera from individuals with MS (RR of highest vs lowest tertile of antibody enrichment, 33.4; 95% CI, 2.5-448.4; P for trend = .008). Higher total anti-EBNA-1 antibodies were also associated with an elevated MS risk (top vs bottom tertile: RR, 27.6; 95% CI, 2.3-327.6; P for trend = .008). After adjusting for total anti-EBNA-1 antibodies, risk estimates from most EBV peptides analyses were attenuated, with 4 remaining significantly associated with MS, the strongest within EBNA-6/EBNA-3C, while the association between total anti-EBNA-1 antibodies and MS persisted.
These findings suggest that antibody response to EBNA-1 may be the strongest serologic risk factor for MS. No single EBV peptide stood out as being selectively targeted in individuals with MS but not controls. Larger investigations are needed to explore possible heterogeneity of anti-EBV humoral immunity in MS.
目前尚不清楚为何只有一小部分感染爱泼斯坦-巴尔病毒(EBV)的个体发展为多发性硬化症(MS),其潜在机制是什么。
评估在MS首次出现症状之前对所有EBV肽段的血清学反应,确定该疾病是否与对EBV的独特免疫反应相关,并评估特定的EBV表位是否驱动这种反应。
设计、背景和参与者:在这项前瞻性巢式病例对照研究中,从美国国防部血清库中存储有血清样本的美国军事人员中选取个体。MS患者在发病前中位数1年(2000 - 2011年向军队报告)采集血清,并与对照组在年龄、性别、种族和民族、采血时间以及军种方面进行匹配。没有个体被排除。数据在2022年9月1日至2023年8月31日期间进行分析。
使用VirScan(噬菌体展示免疫沉淀和测序)测量针对人类病毒组的抗体(富集z分数)。
使用条件逻辑回归估计针对2263种EBV肽段(EBV肽组)的抗体的MS发病率比(RRs),并对总抗EBV核抗原1(EBNA - 1)抗体进行校正,该抗体一直与较高的MS风险相关。还探讨了针对其他病毒肽段的抗体的作用。
共有30例MS患者与30例对照匹配。样本采集时的平均(标准差)年龄为27.8(6.5)岁;60名参与者中有46名(76.7%)为男性。MS患者对EBV肽组的抗体反应更强,但无明显模式。对66种EBV肽段的抗体反应,其中大多数映射到EBNA抗原,在MS患者发病前血清中显著更高(抗体富集最高三分位数与最低三分位数的RR为33.4;95%CI,2.5 - 448.4;趋势P值 = 0.008)。较高的总抗EBNA - 1抗体也与MS风险升高相关(最高三分位数与最低三分位数:RR,27.6;95%CI,2.3 - 327.6;趋势P值 = 0.008)。在对总抗EBNA - 1抗体进行校正后,大多数EBV肽段分析的风险估计值减弱,仍有4种与MS显著相关,最强的在EBNA - 6/EBNA - 3C内,而总抗EBNA - 1抗体与MS之间的关联仍然存在。
这些发现表明,对EBNA - 1的抗体反应可能是MS最强的血清学风险因素。没有单一的EBV肽段在MS患者而非对照组中表现出被选择性靶向。需要进行更大规模的研究来探索MS中抗EBV体液免疫可能存在的异质性。
