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首页> 外文期刊>Journal of Translational Medicine >A large-scale investigation into the role of classical HLA loci in multiple types of severe infections, with a focus on overlaps with autoimmune and mental disorders
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A large-scale investigation into the role of classical HLA loci in multiple types of severe infections, with a focus on overlaps with autoimmune and mental disorders

机译:大规模调查古典HLA基因座在多种严重感染中的作用,重点关注自身免疫和精神障碍的重叠

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Infections are a major disease burden worldwide. While they are caused by external pathogens, host genetics also plays a part in susceptibility to infections. Past studies have reported diverse associations between human leukocyte antigen (HLA) alleles and infections, but many were limited by small sample sizes and/or focused on only one infection. We performed an immunogenetic association study examining 13 categories of severe infection (bacterial, viral, central nervous system, gastrointestinal, genital, hepatitis, otitis, pregnancy-related, respiratory, sepsis, skin infection, urological and other infections), as well as a phenotype for having?any infection, and seven classical HLA loci (HLA-A, B, C, DPB1, DQA1, DQB1 and DRB1). Additionally, we examined associations between infections and specific alleles highlighted in our previous studies of psychiatric disorders and autoimmune disease, as these conditions are known to be linked to infections. Associations between HLA loci and infections were generally not strong. Highlighted associations included associations between DQB1*0302 and DQB1*0604 and viral infections (P?=?0.002835 and P?=?0.014332, respectively), DQB1*0503 and sepsis (P?=?0.006053), and DQA1*0301 with “other” infections (a category which includes infections not included in our main categories e.g. protozoan infections) (P?=?0.000369). Some HLA alleles implicated in autoimmune diseases showed association with susceptibility to infections, but the latter associations were generally weaker, or with opposite trends (in the case of HLA-C alleles, but not with alleles of HLA class II genes). HLA alleles associated with psychiatric disorders did not show association with susceptibility to infections. Our results suggest that classical HLA alleles do not play a large role in the etiology of severe infections. The discordant association trends with autoimmune disease for some alleles could contribute to mechanistic theories of disease etiology.
机译:感染是全世界的主要疾病负担。虽然它们是由外部病原体引起的,但宿主遗传学也涉及感染的易感性。过去的研究报告了人白细胞抗原(HLA)等位基因和感染之间的多种关联,但许多人受到小样本尺寸的限制和/或仅在一种感染上。我们进行了免疫原性关联研究检查检查13类严重感染类别(细菌,病毒,中枢神经系统,胃肠道,生殖器,肝炎,中耳炎,妊娠相关,呼吸,脓毒症,皮肤感染,泌尿外科和其他感染),以及一个具有α的表型,任何感染和七种古典HLA基因座(HLA-A,B,C,DPB1,DQA1,DQB1和DRB1)。此外,我们检查了在我们以前的精神疾病和自身免疫疾病研究中突出的感染和特定等位基因之间的关联,因为已知这些条件与感染有关。 HLA基因座和感染之间的关联通常不强。突出显示的关联包括DQB1 * 0302和DQB1 * 0604和病毒感染之间的关联(P?= 0.002835和P?= 0.014332),DQB1 * 0503和SEPSIS(P?= 0.006053),DQA1 * 0301与“其他“感染(包括未包含在我们的主要类别中的感染,例如原生动物感染)(p?= 0.000369)。一些HLA等位基因涉及自身免疫性疾病,表现出与感染的易感性相关,但后一种关联通常较弱,或者具有相反的趋势(在HLA-C等位基因的情况下,但不具有HLA II类基因的等位基因)。与精神病疾病相关的HLA等位基因没有表现出与感染易感性的关联。我们的研究结果表明,古典HLA等位基因在严重感染的病因中没有发挥着重要作用。某些等位基因具有自身免疫性疾病的不安全的关联趋势可能有助于疾病病因的机制理论。

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