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多种进化机制推动乳头瘤病毒多样化。

Multiple evolutionary mechanisms drive papillomavirus diversification.

作者信息

Gottschling Marc, Stamatakis Alexandros, Nindl Ingo, Stockfleth Eggert, Alonso Angel, Bravo Ignacio G

机构信息

Skin Cancer Center Charité, University Hospital of Berlin, Berlin, Germany.

出版信息

Mol Biol Evol. 2007 May;24(5):1242-58. doi: 10.1093/molbev/msm039. Epub 2007 Mar 6.

DOI:10.1093/molbev/msm039
PMID:17344207
Abstract

The circular, double-stranded 8-kb DNA genome of papillomaviruses (PVes) consists mainly of 4 large genes, E1, E2, L2, and L1. Approximately 150 papillomavirus genomes have been sequenced to date. We analyzed a representative sample of 53 PVes genomes using maximum likelihood, Bayesian inference, maximum parsimony, and distance-based methods both on nucleotide (nt) and on amino acid (aa) alignments. When the 4 genes were analyzed separately, aa-inferred phylogenies contradicted each other less than nt-inferred trees (judged by partition homogeneity tests). In particular, gene combinations including the L2 gene generated significant incongruence (P < 0.001). Combined analyses of the remaining genes E1-E2-L1 produced a well-supported phylogeny including supertaxon beta + gamma + pi + xi-PVes (infecting Artiodactyla, Carnivora, Primates, and Rodentia) and supertaxon kappa + lambda + mu + nu + sigma-PVes (infecting Carnivora, Lagomorpha, Primates, and Rodentia). Based on the tree topology, host-linked evolution appears plausible at shallow, rather than deeper, taxonomic levels. Diversification within PVes may also involve adaptive radiation establishing different niches (within a single-host species) and recombination events (within single-host cells). Heterogeneous groups of closely related PVes infecting, for example, humans and domestic animals such as hamster, dog, and cattle suggest multiple infections across species borders. Additional evolutionary phenomena such as strong codon usage preferences, and computational biases including reconstruction artifacts and insufficient taxon sampling, may contribute to the incomplete resolution of deep phylogenetic nodes. The molecular data globally supports a complex evolutionary scenario for PVes, which is driven by multiple mechanisms but not exclusively by coevolution with corresponding hosts.

摘要

乳头瘤病毒(PV)的环状双链8kb DNA基因组主要由4个大基因E1、E2、L2和L1组成。迄今为止,大约150种乳头瘤病毒基因组已被测序。我们使用最大似然法、贝叶斯推断法、最大简约法以及基于距离的方法,对53种PV基因组的代表性样本进行了核苷酸(nt)和氨基酸(aa)比对分析。当分别分析这4个基因时,氨基酸推断的系统发育树相互矛盾的程度小于核苷酸推断的树(通过分区同质性检验判断)。特别是,包含L2基因的基因组合产生了显著的不一致性(P < 0.001)。对其余基因E1 - E2 - L1的联合分析产生了一个得到充分支持的系统发育树,包括超级分类群β + γ + π + ξ - PV(感染偶蹄目、食肉目、灵长目和啮齿目)和超级分类群κ + λ + μ + ν + σ - PV(感染食肉目、兔形目、灵长目和啮齿目)。基于树的拓扑结构,宿主关联进化在较浅而非较深的分类水平上似乎是合理的。PV内部的多样化也可能涉及建立不同生态位(在单一宿主物种内)的适应性辐射和(在单一宿主细胞内的)重组事件。感染例如人类以及仓鼠、狗和牛等家畜的密切相关PV的异质群体表明存在跨物种边界的多重感染。其他进化现象,如强烈的密码子使用偏好,以及包括重建假象和分类群抽样不足在内的计算偏差,可能导致深层系统发育节点的解析不完整。分子数据总体上支持PV的复杂进化场景,这是由多种机制驱动的,但并非完全由与相应宿主的协同进化驱动。

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