首页> 美国卫生研究院文献>Journal of Virology >Worldwide Genomic Diversity of the High-Risk Human Papillomavirus Types 31, 35, 52, and 58, Four Close Relatives of Human Papillomavirus Type 16
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Worldwide Genomic Diversity of the High-Risk Human Papillomavirus Types 31, 35, 52, and 58, Four Close Relatives of Human Papillomavirus Type 16

机译:31、35、52和58型高危人类乳头瘤病毒的全球基因组多样性16种人类乳头瘤病毒的四个近亲

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摘要

Among the more than one hundred formally described human papillomavirus (HPV) types, 18 are referred to as high-risk HPV types due to their association with anogenital cancer. Despite pathogenic similarities, these types form three remotely related taxonomic groups. One of these groups is called HPV species 9 and is formed by HPV-16, the most common and best-studied type, together with HPV-31, -33, -35, -52, -58, and -67. Previous worldwide comparisons of HPV-16 samples showed about 2% nucleotide diversity between isolates, which were subsequently termed variants. The distribution of divergent variants has been found to correlate frequently with the geographic origin and the ethnicity of the infected patients and led to the concept of unique African, European, Asian, and Native American HPV-16 variants. In the current study, we address the question of whether geography and ethnicity also correlate with sequence variations found for HPV-31, -35, -52, and -58. This was done by sequencing the long control region in samples derived from Europe, Asia, and Africa, and from immigrant populations in North and South America. We observed maximal divergence between any two variants within each of these four HPV types ranging from 1.8 to 3.6% based on nucleotide exchanges and, occasionally, on insertions and deletions. Similar to the case with HPV-16, these mutations are not random but indicate a relationship between the variants in form of phylogenetic trees. An interesting example is presented by a 16-bp insert in select variants of HPV-35, which appears to have given rise to additional variants by nucleotide exchanges within the insert. All trees showed distinct phylogenetic topologies, ranging from dichotomic branching in the case of HPV-31 to star phylogenies of the other three types. No clear similarities between these types or between these types and HPV-16 exist. While variant branches in some types were specific for Europe, Africa, or East Asia, none of the four trees reflected human evolution and spread to the extent illustrated by HPV-16. One possible explanation is that the rare HPV types that we studied spread and thereby diversified more slowly than the more abundant HPV-16 and may have established much of today's variant diversity already before the worldwide spread of humans 100,000 years ago. Most variants had prototypic amino acid sequences within the E6 oncoprotein and a segment of the L1 capsid protein. Some had one, two, or three amino acid substitutions in these regions, which might indicate biological and pathogenic diversity between the variants of each HPV type.
机译:在一百多种正式描述的人类乳头瘤病毒(HPV)类型中,有18种因与生殖器癌相关而被称为高危HPV类型。尽管在病原学上有相似之处,但这些类型形成了三个远程相关的生物分类群。其中一组称为HPV物种9,由HPV-16(最常见和研究最好的类型)以及HPV-31,-33,-35,-52,-58和-67组成。以前在全球对HPV-16样品进行的比较显示,分离株之间的核苷酸多样性约为2%,随后将其称为变体。已经发现不同变异体的分布经常与受感染患者的地理起源和种族相关,并导致了独特的非洲,欧洲,亚洲和美洲原住民HPV-16变异体的概念。在当前的研究中,我们解决了地理和种族是否也与HPV-31,-35,-52和-58的序列变异相关的问题。通过对来自欧洲,亚洲和非洲以及北美和南美移民人口的样本中的长对照区域进行测序来完成。我们观察到这四种HPV类型中每一种的两个变异之间的最大差异为1.8%至3.6%(基于核苷酸交换,偶尔基于插入和缺失)。与HPV-16的情况类似,这些突变不是随机的,而是以系统发育树的形式指示了变体之间的关系。一个有趣的例子是在HPV-35的选定变体中插入一个16 bp的插入片段,该插入片段中的核苷酸交换似乎引起了其他变体的出现。所有树木均显示出独特的系统发育拓扑,范围从HPV-31的二分枝到其他三种类型的星系。这些类型之间或这些类型与HPV-16之间没有明显的相似之处。尽管某些类型的变异树枝专门针对欧洲,非洲或东亚,但四棵树都没有反映出人类的进化并传播到HPV-16所说明的程度。一种可能的解释是,我们研究的稀有HPV类型比更丰富的HPV-16传播并因此分散的速度更慢,并且可能在100,000年前人类在世界范围内传播之前就已经建立了当今的许多变异。大多数变体在E6癌蛋白和L1衣壳蛋白的一部分中具有原型氨基酸序列。一些在这些区域具有一个,两个或三个氨基酸取代,这可能表明每种HPV类型变异之间的生物学和致病性多样性。

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