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本文引用的文献

1
Subtle mutational changes in the SU protein of a natural feline leukemia virus subgroup A isolate alter disease spectrum.一株天然的A型猫白血病病毒分离株的SU蛋白中细微的突变变化改变了疾病谱。
J Virol. 2005 Feb;79(3):1351-60. doi: 10.1128/JVI.79.3.1351-1360.2005.
2
Substitution of feline leukemia virus long terminal repeat sequences into murine leukemia virus alters the pattern of insertional activation and identifies new common insertion sites.将猫白血病病毒长末端重复序列替换到鼠白血病病毒中会改变插入激活模式并识别出新的常见插入位点。
J Virol. 2005 Jan;79(1):57-66. doi: 10.1128/JVI.79.1.57-66.2005.
3
Regulation of FeLV-945 by c-Myb binding and CBP recruitment to the LTR.通过c-Myb结合以及CBP募集至长末端重复序列(LTR)对猫白血病病毒945(FeLV-945)进行调控。
Virol J. 2004 Sep 3;1:3. doi: 10.1186/1743-422X-1-3.
4
Feline leukaemia virus LTR variation and disease association in a geographical and temporal cluster.猫白血病病毒长末端重复序列变异与地理和时间集群中的疾病关联
J Gen Virol. 2004 Oct;85(Pt 10):2937-2942. doi: 10.1099/vir.0.80149-0.
5
A point mutation in the binding subunit of a retroviral envelope protein arrests virus entry at hemifusion.逆转录病毒包膜蛋白结合亚基中的一个点突变使病毒进入在半融合阶段停止。
J Virol. 2004 Jan;78(1):473-81. doi: 10.1128/jvi.78.1.473-481.2004.
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Selection forces and constraints on retroviral sequence variation.逆转录病毒序列变异的选择力与限制因素
Science. 2001 May 11;292(5519):1106-9. doi: 10.1126/science.1059128.
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Differential pathogenicity of two feline leukemia virus subgroup A molecular clones, pFRA and pF6A.两种猫白血病病毒A亚群分子克隆pFRA和pF6A的致病性差异
J Virol. 2000 Jul;74(13):5796-801. doi: 10.1128/jvi.74.13.5796-5801.2000.
8
Feline leukemia virus envelope sequences that affect T-cell tropism and syncytium formation are not part of known receptor-binding domains.影响T细胞嗜性和多核体形成的猫白血病病毒包膜序列并非已知受体结合域的一部分。
J Virol. 2000 Jul;74(13):5754-61. doi: 10.1128/jvi.74.13.5754-5761.2000.
9
Identification of a cellular cofactor required for infection by feline leukemia virus.猫白血病病毒感染所需细胞辅助因子的鉴定。
Science. 2000 Mar 10;287(5459):1828-30. doi: 10.1126/science.287.5459.1828.
10
The FeLV-945 LTR confers a replicative advantage dependent on the presence of a tandem triplication.猫白血病病毒945长末端重复序列赋予了一种依赖于串联三联体存在的复制优势。
Virology. 1999 Oct 25;263(2):460-70. doi: 10.1006/viro.1999.9974.

猫白血病病毒独特的长末端重复序列和表面糖蛋白基因序列作为疾病转归的决定因素。

Unique long terminal repeat and surface glycoprotein gene sequences of feline leukemia virus as determinants of disease outcome.

作者信息

Chandhasin Chandtip, Coan Patricia N, Pandrea Ivona, Grant Chris K, Lobelle-Rich Patricia A, Puetter Adriane, Levy Laura S

机构信息

Department of Microbiology and Immunology, Tulane University School of Medicine, 1430 Tulane Ave. SL-38, New Orleans, LA 70112, USA.

出版信息

J Virol. 2005 May;79(9):5278-87. doi: 10.1128/JVI.79.9.5278-5287.2005.

DOI:10.1128/JVI.79.9.5278-5287.2005
PMID:15827142
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1082761/
Abstract

The outcome of feline leukemia virus (FeLV) infection in nature is variable, including malignant, proliferative, and degenerative disorders. The determinants of disease outcome are not well understood but are thought to include viral, host, and environmental factors. In particular, genetic variations in the FeLV long terminal repeat (LTR) and SU gene have been linked to disease outcome. FeLV-945 was previously identified as a natural isolate predominant in non-T-cell neoplastic and nonneoplastic diseases in a geographic cohort. The FeLV-945 LTR was shown to contain unique repeat elements, including a 21-bp triplication downstream of the enhancer. The FeLV-945 SU gene was shown to encode mutational changes in functional domains of the protein. The present study details the outcomes of infection with recombinant FeLVs in which the LTR and envelope (env) gene of FeLV-945, or the LTR only, was substituted for homologous sequences in a horizontally transmissible prototype isolate, FeLV-A/61E. The results showed that the FeLV-945 LTR determined the kinetics of disease. Substitution of the FeLV-945 LTR into FeLV-A/61E resulted in a significantly more rapid disease onset but did not alter the tumorigenic spectrum. In contrast, substitution of both the FeLV-945 LTR and env gene changed the disease outcome entirely. Further, the impact of FeLV-945 env on the disease outcome was dependent on the route of inoculation. Since the TM genes of FeLV-945 and FeLV-A/61E are nearly identical but the SU genes differ significantly, FeLV-945 SU is implicated in the outcome. These findings identify the FeLV-945 LTR and SU gene as determinants of disease.

摘要

猫白血病病毒(FeLV)在自然环境中的感染结果具有多样性,包括恶性、增殖性和退行性疾病。疾病结果的决定因素尚未完全明确,但被认为包括病毒、宿主和环境因素。特别是,FeLV长末端重复序列(LTR)和SU基因的遗传变异与疾病结果有关。FeLV-945先前被鉴定为在一个地理队列中非T细胞肿瘤性和非肿瘤性疾病中占主导的自然分离株。研究表明,FeLV-945的LTR包含独特的重复元件,包括增强子下游一个21碱基对的三联体。研究还表明,FeLV-945的SU基因在该蛋白的功能域编码突变变化。本研究详细阐述了重组FeLV感染的结果,其中用FeLV-945的LTR和包膜(env)基因,或仅LTR,替代水平传播的原型分离株FeLV-A/61E中的同源序列。结果显示,FeLV-945的LTR决定了疾病的进程。将FeLV-945的LTR替换到FeLV-A/61E中导致疾病发作明显更快,但未改变致瘤谱。相反,同时替换FeLV-945的LTR和env基因则完全改变了疾病结果。此外,FeLV-945 env对疾病结果的影响取决于接种途径。由于FeLV-945和FeLV-A/61E的跨膜(TM)基因几乎相同,但SU基因差异显著,因此FeLV-945的SU与疾病结果有关。这些发现确定了FeLV-945的LTR和SU基因是疾病的决定因素。