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狒狒猿猴嗜T淋巴细胞病毒1感染:序列异质性与T细胞识别

Simian T Lymphotropic Virus 1 Infection of Papio anubis: Sequence Heterogeneity and T Cell Recognition.

作者信息

Termini James M, Magnani Diogo M, Maxwell Helen S, Lauer William, Castro Iris, Pecotte Jerilyn, Barber Glen N, Watkins David I, Desrosiers Ronald C

机构信息

Department of Pathology, University of Miami Miller School of Medicine, Miami, Florida, USA.

Southwest National Primate Research Center, Texas Biomedical Research Institute, San Antonio, Texas, USA.

出版信息

J Virol. 2017 Sep 27;91(20). doi: 10.1128/JVI.00950-17. Print 2017 Oct 15.

Abstract

Baboons naturally infected with simian T lymphotropic virus (STLV) are a potentially useful model system for the study of vaccination against human T lymphotropic virus (HTLV). Here we expanded the number of available full-length baboon STLV-1 sequences from one to three and related the T cell responses that recognize the immunodominant Tax protein to the sequences present in two individual baboons. Continuously growing T cell lines were established from two baboons, animals 12141 and 12752. Next-generation sequencing (NGS) of complete STLV genome sequences from these T cell lines revealed them to be closely related but distinct from each other and from the baboon STLV-1 sequence in the NCBI sequence database. Overlapping peptides corresponding to each unique Tax sequence and to the reference baboon Tax sequence were used to analyze recognition by T cells from each baboon using intracellular cytokine staining (ICS). Individual baboons expressed more gamma interferon and tumor necrosis factor alpha in response to Tax peptides corresponding to their own STLV-1 sequence than in response to Tax peptides corresponding to the reference baboon STLV-1 sequence. Thus, our analyses revealed distinct but closely related STLV-1 genome sequences in two baboons, extremely low heterogeneity of STLV sequences within each baboon, no evidence for superinfection within each baboon, and a ready ability of T cells in each baboon to recognize circulating Tax sequences. While amino acid substitutions that result in escape from CD8 T cell recognition were not observed, premature stop codons were observed in 7% and 56% of sequences from peripheral blood mononuclear cells from animals 12141 and 12752, respectively. It has been estimated that approximately 100,000 people suffer serious morbidity and 10,000 people die each year from the consequences associated with human T lymphotropic virus (HTLV) infection. There are no antiviral drugs and no preventive vaccine. A preventive vaccine would significantly impact the global burden associated with HTLV infections. Here we provide fundamental information on the simian T lymphotropic virus (STLV) naturally transmitted in a colony of captive baboons. The limited viral sequence heterogeneity in individual baboons, the identity of the viral gene product that is the major target of cellular immune responses, the persistence of viral amino acid sequences that are the major targets of cellular immune responses, and the emergence of truncated variants in the major target of cellular immune responses all parallel what are seen with HTLV infection of humans. These results justify the use of STLV-infected baboons as a model system for vaccine development efforts.

摘要

自然感染猿猴嗜T淋巴细胞病毒(STLV)的狒狒是研究针对人类嗜T淋巴细胞病毒(HTLV)疫苗接种的一个潜在有用的模型系统。在此,我们将可用的全长狒狒STLV - 1序列数量从1个增加到3个,并将识别免疫显性Tax蛋白的T细胞反应与两只个体狒狒中存在的序列相关联。从两只狒狒(动物12141和12752)建立了持续生长的T细胞系。对这些T细胞系的完整STLV基因组序列进行的下一代测序(NGS)显示,它们彼此密切相关,但又彼此不同,且与NCBI序列数据库中的狒狒STLV - 1序列不同。对应于每个独特Tax序列和参考狒狒Tax序列的重叠肽被用于通过细胞内细胞因子染色(ICS)分析来自每只狒狒的T细胞的识别情况。与对应于参考狒狒STLV - 1序列的Tax肽相比,个体狒狒对与其自身STLV - 1序列对应的Tax肽产生更多的γ干扰素和肿瘤坏死因子α。因此,我们的分析揭示了两只狒狒中不同但密切相关的STLV - 1基因组序列,每只狒狒内STLV序列的异质性极低,没有证据表明每只狒狒内存在双重感染,并且每只狒狒中的T细胞能够轻易识别循环中的Tax序列。虽然未观察到导致逃避CD8 T细胞识别的氨基酸替代,但在动物12141和12752外周血单个核细胞的序列中,分别有7%和56%观察到了提前终止密码子。据估计,每年约有10万人因人类嗜T淋巴细胞病毒(HTLV)感染的相关后果而遭受严重发病,1万人死亡。目前没有抗病毒药物,也没有预防性疫苗。预防性疫苗将对与HTLV感染相关的全球负担产生重大影响。在此,我们提供了关于在一群圈养狒狒中自然传播的猿猴嗜T淋巴细胞病毒(STLV)的基础信息。个体狒狒中有限的病毒序列异质性、作为细胞免疫反应主要靶点的病毒基因产物的特性、作为细胞免疫反应主要靶点的病毒氨基酸序列的持续性以及在细胞免疫反应主要靶点中截短变体的出现,都与人类HTLV感染中所见的情况相似。这些结果证明将感染STLV的狒狒用作疫苗开发研究的模型系统是合理的。

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