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通过全基因组分析揭示的新型人类3型嗜T淋巴细胞病毒的古老起源和分子特征

Ancient origin and molecular features of the novel human T-lymphotropic virus type 3 revealed by complete genome analysis.

作者信息

Switzer William M, Qari Shoukat H, Wolfe Nathan D, Burke Donald S, Folks Thomas M, Heneine Walid

机构信息

Laboratory Branch, Division of HIV/AIDS Prevention, National Center for HIV, STD, and TB Prevention, Centers for Disease Control and Prevention, 1600 Clifton Road, MS G-45, Atlanta, GA 30333, USA.

出版信息

J Virol. 2006 Aug;80(15):7427-38. doi: 10.1128/JVI.00690-06.

Abstract

Human T-lymphotropic virus type 3 (HTLV-3) is a new virus recently identified in two primate hunters in Central Africa. Limited sequence analysis shows that HTLV-3 is distinct from HTLV-1 and HTLV-2 but is genetically similar to simian T-lymphotropic virus type 3 (STLV-3). We report here the first complete HTLV-3 sequence obtained by PCR-based genome walking using uncultured peripheral blood lymphocytes from an HTLV-3-infected person. The HTLV-3(2026ND) genome is 8,917 bp long and is genetically equidistant from HTLV-1 and HTLV-2, sharing about 62% identity. Phylogenetic analysis of all gene regions confirms this relationship and shows that HTLV-3 falls within the diversity of STLV-3, suggesting a primate origin. However, HTLV-3(2026ND) is unique, sharing only 87% to 92% sequence identity with STLV-3. SimPlot and phylogenetic analysis did not reveal any evidence of genetic recombination with either HTLV-1, HTLV-2, or STLV-3. Molecular dating estimates that the ancestor of HTLV-3 is as old as HTLV-1 and HTLV-2, with an inferred divergence time of 36,087 to 54,067 years ago. HTLV-3 has a prototypic genomic structure, with all enzymatic, regulatory, and structural proteins preserved. Like STLV-3, HTLV-3 is missing a third 21-bp transcription element found in the long terminal repeats of HTLV-1 and HTLV-2 but instead contains a unique activator protein-1 transcription factor upstream of the 21-bp repeat elements. A PDZ motif, like that in HTLV-1, which is important for cellular signal transduction and transformation, is present in the C terminus of the HTLV-3 Tax protein. A basic leucine zipper region located in the antisense strand of HTLV-1, believed to play a role in viral replication and oncogenesis, was also found in the complementary strand of HTLV-3. The ancient origin of HTLV-3, the broad distribution of STLV-3 in Africa, and the propensity of STLVs to cross species into humans all suggest that HTLV-3 may be prevalent and support the need for expanded surveillance for this virus.

摘要

人类嗜T淋巴细胞病毒3型(HTLV-3)是最近在中非的两名灵长类动物捕猎者身上发现的一种新病毒。有限的序列分析表明,HTLV-3与HTLV-1和HTLV-2不同,但在基因上与猿猴嗜T淋巴细胞病毒3型(STLV-3)相似。我们在此报告通过基于PCR的基因组步移法,利用一名HTLV-3感染者未经培养的外周血淋巴细胞获得的首个完整HTLV-3序列。HTLV-3(2026ND)基因组长度为8917 bp,在基因上与HTLV-1和HTLV-2距离相等,序列一致性约为62%。对所有基因区域的系统发育分析证实了这种关系,并表明HTLV-3属于STLV-3的多样性范围,提示其起源于灵长类动物。然而,HTLV-3(2026ND)是独特的,与STLV-3的序列一致性仅为87%至92%。SimPlot分析和系统发育分析未发现与HTLV-1、HTLV-2或STLV-3发生基因重组的任何证据。分子年代测定估计HTLV-3的祖先与HTLV-1和HTLV-2一样古老,推测其分化时间为36087至54067年前。HTLV-3具有典型的基因组结构,所有酶、调节和结构蛋白均得以保留。与STLV-3一样,HTLV-3在HTLV-1和HTLV-2的长末端重复序列中缺失第三个21 bp的转录元件,但在21 bp重复元件上游含有一个独特的激活蛋白-1转录因子。HTLV-3 Tax蛋白的C末端存在一个与HTLV-1中类似的PDZ基序,该基序对细胞信号转导和转化很重要。在HTLV-1反义链中发现的一个据信在病毒复制和肿瘤发生中起作用的碱性亮氨酸拉链区域,在HTLV-3的互补链中也被发现。HTLV-3的古老起源、STLV-3在非洲的广泛分布以及STLVs跨物种传播给人类的倾向均表明HTLV-3可能很普遍,支持对该病毒扩大监测的必要性。

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