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Bioinformatic Analysis of Chlamydia trachomatis Polymorphic Membrane Proteins PmpE PmpF PmpG and PmpH as Potential Vaccine Antigens

机译:沙眼衣原体多态性膜蛋白PmpEPmpFPmpG和PmpH作为潜在的疫苗抗原的生物信息学分析

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摘要

Chlamydia trachomatis is the most important infectious cause of infertility in women with important implications in public health and for which a vaccine is urgently needed. Recent immunoproteomic vaccine studies found that four polymorphic membrane proteins (PmpE, PmpF, PmpG and PmpH) are immunodominant, recognized by various MHC class II haplotypes and protective in mouse models. In the present study, we aimed to evaluate genetic and protein features of Pmps (focusing on the N-terminal 600 amino acids where MHC class II epitopes were mapped) in order to understand antigen variation that may emerge following vaccine induced immune selection. We used several bioinformatics platforms to study: i) Pmps’ phylogeny and genetic polymorphism; ii) the location and distribution of protein features (GGA(I, L)/FxxN motifs and cysteine residues) that may impact pathogen-host interactions and protein conformation; and iii) the existence of phase variation mechanisms that may impact Pmps’ expression. We used a well-characterized collection of 53 fully-sequenced strains that represent the C. trachomatis serovars associated with the three disease groups: ocular (N=8), epithelial-genital (N=25) and lymphogranuloma venereum (LGV) (N=20). We observed that PmpF and PmpE are highly polymorphic between LGV and epithelial-genital strains, and also within populations of the latter. We also found heterogeneous representation among strains for GGA(I, L)/FxxN motifs and cysteine residues, suggesting possible alterations in adhesion properties, tissue specificity and immunogenicity. PmpG and, to a lesser extent, PmpH revealed low polymorphism and high conservation of protein features among the genital strains (including the LGV group). Uniquely among the four Pmps, pmpG has regulatory sequences suggestive of phase variation. In aggregate, the results suggest that PmpG may be the lead vaccine candidate because of sequence conservation but may need to be paired with another protective antigen (like PmpH) in order to prevent immune selection of phase variants.
机译:沙眼衣原体是妇女不育的最重要的传染原因,对公共卫生具有重要影响,因此迫切需要疫苗。最近的免疫蛋白质组疫苗研究发现,四种多态性膜蛋白(PmpE,PmpF,PmpG和PmpH)具有免疫优势,可以被多种MHC II类单倍型识别并在小鼠模型中具有保护作用。在本研究中,我们旨在评估Pmps的遗传和蛋白质特征(着眼于定位MHC II类表位的N末端600个氨基酸),以了解疫苗诱导的免疫选择后可能出现的抗原变异。我们使用了几种生物信息学平台来研究:i)Pmp的系统发育和遗传多态性; ii)可能影响病原体-宿主相互作用和蛋白质构象的蛋白质特征(GGA(I,L)/ FxxN基序和半胱氨酸残基)的位置和分布; iii)存在可能影响Pmps表达的相位变化机制。我们使用了表征良好的53个全序列菌株的集合,这些菌株代表与以下三个疾病组相关的沙眼衣原体血清:眼病(N = 8),上皮生殖器(N = 25)和淋巴肉芽肿性病(LGV)(N = 20)。我们观察到PmpF和PmpE在LGV和上皮生殖器之间以及在后者的人群中高度多态。我们还发现菌株之间的GGA(I,L)/ FxxN基序和半胱氨酸残基的异质表示,表明粘附特性,组织特异性和免疫原性可能发生改变。在生殖器菌株(包括LGV组)中,PmpG和较小程度的PmpH显示出低多态性和高蛋白保守性。在这四个Pmp中,pmpG具有独特的调节序列,暗示了相位变化。总体而言,结果表明PmpG可能是序列保守的候选候选疫苗,但可能需要与其他保护性抗原(如PmpH)配对,以防止对相变体进行免疫选择。

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