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首页> 外文期刊>Virology Journal >Phylogenetic comparison of exonic US4, US7 and UL44 regions of clinical herpes simplex virus type 1 isolates showed lack of association between their anatomic sites of infection and genotypic/sub genotypic classification
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Phylogenetic comparison of exonic US4, US7 and UL44 regions of clinical herpes simplex virus type 1 isolates showed lack of association between their anatomic sites of infection and genotypic/sub genotypic classification

机译:临床单纯疱疹病毒1型分离株的外显子US4,US7和UL44区的系统发育比较显示,感染的解剖部位与基因型/亚基因型分类之间缺乏关联

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摘要

Background HSV-1 genome is a mosaic of recombinants. Clinical Herpes simplex virus -1 (HSV1) isolates were already genotyped as A, B and C types based on nucleotide variations at Unique Short (US) 4 (gG) and US 7 (gI) regions through phylogeny. Analysis of Glycoprotein C (gC) exon present on the Unique Long (UL) region had also revealed the existence of different genotypes. Glycoprotein C is mainly involved in initial viral attachment to heparan sulphate on host cell surface facilitating the virus's binding and penetration into cell. As the amount of heparan sulphate on the host cell surface varies according to the cell type, it is plausible that different genotypes bind differentially to cell types. Hence, this study was framed to determine the existence of novel genotypes/sub genotypes in the US or UL regions which could associate with clinical entities. Results All the twenty five isolates analyzed in this study were of genotype A as per their gG gene sequences. In case of gI gene, 16 out of 25 were found to be type A and the remaining nine were type B putative intergenic recombinants. Intragenic recombinations were also encountered in both the US genes, with gG possessing novel subgenotypes, arbitrarily designated A1 and A2. The 9 type B isolates of gI genes also branched out into 2 clades due to genetic variations. Glycoprotein C of UL region had two distinct genotypic clades α and β, whose topological distribution was significantly different from that of the US region. Neither the US nor UL regions, however, showed any preference among the genotypes to a specific anatomic site of infection. Even the non synonymous variations identified in the functional domain of gC, were not confined to a particular genotype/clinical entity. Conclusion The analyses of the US and UL regions of the HSV-1 genome showed the existence of variegated genotypes in these two regions. In contrary to the documented literature, in which Asian strains were concluded as more conserved than European ones, our study showed the existence of a higher degree of variability among Indian strains. However, the identified novel genotypes and subgenotypes were not found associated with clinical entities.
机译:背景HSV-1基因组是重组体的镶嵌体。临床单纯疱疹病毒-1(HSV1)分离株已经通过系统发育在独特短(US)4(gG)和US 7(gI)区域的核苷酸变异进行了基因分型,分别为A,B和C型。分析存在于独特长(UL)区域的糖蛋白C(gC)外显子也揭示了不同基因型的存在。糖蛋白C主要参与病毒在宿主细胞表面上与硫酸乙酰肝素的初始附着,从而促进病毒的结合和渗透进入细胞。由于宿主细胞表面上硫酸乙酰肝素的量根据细胞类型而变化,因此不同基因型与细胞类型的差异结合是合理的。因此,本研究旨在确定在美国或UL地区可能与临床实体相关的新型基因型/亚基因型的存在。结果本研究中分析的全部25个分离株,根据其gG基因序列均属于基因型A。对于gI基因,发现25个基因中有16个是A型,其余9个是B型推定的基因间重组子。在两个美国基因中也都遇到了基因内重组,其中gG具有新的亚基因型,任意指定为A1和A2。由于遗传变异,gI基因的9种B型分离株也分支为2个进化枝。 UL地区的糖蛋白C有两个明显的基因型进化枝α和β,其拓扑分布与美国地区的拓扑分布显着不同。但是,美国地区和UL地区均未显示出基因型对特定感染部位的偏爱。即使在gC的功能域中识别出的非同义变异也不限于特定的基因型/临床实体。结论对HSV-1基因组的US和UL区域的分析表明在这两个区域中存在多样化的基因型。与有文献记载的亚洲菌株被认为比欧洲菌株更为保守的文献相反,我们的研究表明印度菌株之间存在较高程度的变异性。但是,未发现已鉴定的新基因型和亚基因型与临床实体相关。

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