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[疟原虫与吉兰-巴雷综合征抗原之间的分子模拟]

[Molecular mimicry between Plasmodium sp and Guillain-Barre syndrome antigens].

作者信息

Emiliani-Navarro Yuliana Marcela, Vega D, Muzi G, Munera-Gomez Marlon, Sánchez Andrés

机构信息

Facultad de Salud, Grupo de Investigación Nuñista de Medicina (GINUMED), Corporación Universitaria Rafael Núñez, Colombia.

Grupo de Investigación de Infectología Pediátrica (GIINPED), Fundación Hospital Infantil Napoleón Franco Pareja, Universidad de Cartagena, Bolívar, Colombia.

出版信息

Rev Alerg Mex. 2024 Feb 1;71(1):54. doi: 10.29262/ram.v71i1.1374.

Abstract

OBJECTIVE

Analyze the molecular mimicry between Plasmodium spp. and autoantigens associated with GBS, identifying possible antigenic epitopes.

METHODS

PSI-Blast, Praline, Emboss, Protein Data Bank, Swiss Model Server, AlphaFold 2, Ellipro and PyMol 2.3 were used to search for homologies, perform alignments, obtain protein structures, and predict epitopes.

RESULTS

17 autoantigens and seven immunological targets of the peripheral nervous system were included, identifying 72 possible epitopes associated with GBS. From the proteome of Plasmodium spp. (298 proteins), only two showed similarities close to 30% with TRIM21 and BACE1, generating seven possible epitopes.

CONCLUSION

No significant homologies were observed between the proteome of GBS and Plasmodium spp. The exploration of other mechanisms such as immune-mediated capillary damage, Epitope Spreading or Bystander Activation is suggested to explain the mentioned association. These findings underscore the need to clarify the etiology of autoimmune diseases and the role of pathogens. The need for experimental studies to validate these results is emphasized.

摘要

目的

分析疟原虫属与格林-巴利综合征(GBS)相关自身抗原之间的分子模拟,确定可能的抗原表位。

方法

使用PSI-Blast、Praline、Emboss、蛋白质数据库、瑞士模型服务器、AlphaFold 2、Ellipro和PyMol 2.3来搜索同源性、进行比对、获得蛋白质结构并预测表位。

结果

纳入了17种自身抗原和7种外周神经系统免疫靶点,确定了72个与GBS相关的可能表位。在疟原虫属蛋白质组(298种蛋白质)中,只有两种与TRIM21和BACE1显示出接近30%的相似性,产生了7个可能的表位。

结论

在GBS蛋白质组和疟原虫属之间未观察到显著同源性。建议探索其他机制,如免疫介导的毛细血管损伤、表位扩展或旁观者激活,以解释上述关联。这些发现强调了阐明自身免疫性疾病病因和病原体作用的必要性。强调需要进行实验研究来验证这些结果。

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