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炭疽疫苗接种、海湾战争综合征与人类白细胞抗原(HLA)

Anthrax Vaccination, Gulf War Illness, and Human Leukocyte Antigen (HLA).

作者信息

James Lisa M, Carpenter Adam F, Engdahl Brian E, Johnson Rachel A, Lewis Scott M, Georgopoulos Apostolos P

机构信息

The GWI and HLA Research Groups, Brain Sciences Center, Department of Veterans Affairs Health Care System, Minneapolis, MN 55417, USA.

Department of Neuroscience, University of Minnesota Medical School, Minneapolis, MN 55455, USA.

出版信息

Vaccines (Basel). 2024 Jun 4;12(6):613. doi: 10.3390/vaccines12060613.

Abstract

We report on a highly significant, positive association between anthrax vaccination and occurrence of Gulf War Illness (GWI) in 111 Gulf War veterans (42 with GWI and 69 controls). GWI was diagnosed in 47.1% of vaccinated veterans but only in 17.2% of non-vaccinated veterans (Pearson = 7.08, = 0.008; odds ratio = 3.947; relative risk = 2.617), with 1.6x higher GWI symptom severity in vaccinated veterans ( = 0.007, F-test in analysis of covariance). Next, we tested the hypothesis that the susceptibility to GWI following anthrax vaccination could be due to inability to make antibodies against the anthrax protective antigen (PA), the key protein contained in the vaccine. Since the first step in initiating antibody production would be the binding of PA peptide fragments (typically 15-amino acid long [15-mer]) to peptide-binding motifs of human leukocyte antigen (HLA) Class II molecules, we assessed the binding-motif affinities of such HLA specific molecules to all linear 15-mer peptide fragments of the anthrax PA. We identified a total of 58 HLA Class II alleles carried by the veterans in our sample and found that, of those, 18 (31%) were present in the vaccinated group that did not develop GWI but were absent from the vaccinated group who developed GWI. Remarkably, in silico analyses revealed very high binding affinities of peptide-binding motifs of those 18 HLA alleles with fragments of anthrax vaccine PA, leading to the successful production of anti-PA antibodies. Conversely, the absence of these protective HLA alleles points to a reduced ability to develop antibodies against PA, thus resulting in harmful PA persistence and development of GWI.

摘要

我们报告了111名海湾战争退伍军人(42名患有海湾战争综合征[GWI],69名作为对照)中炭疽疫苗接种与GWI发生之间存在高度显著的正相关。47.1%接种疫苗的退伍军人被诊断患有GWI,而未接种疫苗的退伍军人中这一比例仅为17.2%(Pearson检验=7.08,P=0.008;优势比=3.947;相对风险=2.617),接种疫苗的退伍军人GWI症状严重程度高1.6倍(P=0.007,协方差分析中的F检验)。接下来,我们检验了一个假设,即接种炭疽疫苗后对GWI的易感性可能是由于无法产生针对炭疽保护性抗原(PA)的抗体,PA是疫苗中的关键蛋白质。由于启动抗体产生的第一步是PA肽片段(通常为15个氨基酸长[15聚体])与人白细胞抗原(HLA)II类分子的肽结合基序结合,我们评估了此类HLA特异性分子与炭疽PA所有线性15聚体肽片段的结合基序亲和力。我们在样本中总共鉴定出退伍军人携带的58个HLA II类等位基因,发现其中18个(31%)存在于未患GWI的接种疫苗组中,但在患GWI的接种疫苗组中不存在。值得注意的是,计算机分析显示这18个HLA等位基因的肽结合基序与炭疽疫苗PA片段具有非常高的结合亲和力,从而成功产生了抗PA抗体。相反,这些保护性HLA等位基因的缺失表明产生抗PA抗体的能力降低,从而导致有害的PA持续存在并引发GWI。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c750/11209475/30e90a4458da/vaccines-12-00613-g001.jpg

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