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Human Papillomavirus Epitope Mimicry and Autoimmunity: The Molecular Truth of Peptide Sharing

机译:人乳头瘤病毒表位模仿和自身免疫:肽共享的分子真实

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Objective: To define the cross-reactivity potential and the consequent autoimmunity intrinsic to viral versus human peptide sharing. Methods: Using human papillomavirus (HPV) infection/active immunization as a research model, the experimentally validated HPV L1 epitopes catalogued at the Immune Epitope DataBase were analyzed for peptide sharing with the human proteome. Results: The final data show that the totality of the immunoreactive HPV L1 epi-topes is mostly composed by peptides present in human proteins. Conclusions: Immunologically, the high extent of peptide sharing between the HPV L1 epitopes and human proteins invites to revise the concept of the negative selection of self-reactive lymphocytes. Pathologically, the data highlight a cross-reactive potential for a spectrum of autoimmune diseases that includes ovarian failure, systemic lupus erythematosus (SLE), breast cancer and sudden death, among others. Therapeutically, analyzing already validated immunoreactive epitopes filters out the peptide sharing possibly exempt of self-reactivity, defines the effective potential for pathologic autoimmunity, and allows singling out peptide epitopes for safe immunotherapeutic protocols.
机译:目的:定义交叉反应性潜力和随后的自身免疫固有对病毒与人肽共享。方法:使用人乳头瘤病毒(HPV)感染/主动免疫作为研究模型,分析了在免疫表位数据库中目录的实验验证的HPV L1表位,用于与人蛋白质组共享。结果:最终数据表明,免疫反应性HPV L1外圈的全部主要由存在于人蛋白中存在的肽组成。结论:免疫,HPV L1表位和人蛋白之间的肽共享的高度邀请修改自活性淋巴细胞的负面选择的概念。病理学上,数据突出了一种具有卵巢衰竭,全身狼疮红斑(SLE),乳腺癌和猝死等卵巢衰竭的横向反应性潜力。治疗性地,分析已经验证的免疫反应表位过滤出肽共享可能豁免自我反应性,定义病理自身免疫的有效潜力,并允许单肽表位用于安全免疫治疗方案。

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