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研究恒河猴巨细胞病毒(RhCMV)在食蟹猴中的种属特异性。

Examining the species-specificity of rhesus macaque cytomegalovirus (RhCMV) in cynomolgus macaques.

作者信息

Marsh Angie K, Ambagala Aruna P, Perciani Catia T, Russell Justen N Hoffman, Chan Jacqueline K, Janes Michelle, Antony Joseph M, Pilon Richard, Sandstrom Paul, Willer David O, MacDonald Kelly S

机构信息

Department of Immunology, University of Toronto, Toronto, ON, Canada.

Department of Microbiology, Mount Sinai Hospital, Toronto, ON, Canada; Department of Medicine, University of Toronto, Toronto, ON, Canada.

出版信息

PLoS One. 2015 Mar 30;10(3):e0121339. doi: 10.1371/journal.pone.0121339. eCollection 2015.

Abstract

Cytomegalovirus (CMV) is a highly species-specific virus that has co-evolved with its host over millions of years and thus restricting cross-species infection. To examine the extent to which host restriction may prevent cross-species research between closely related non-human primates, we evaluated experimental infection of cynomolgus macaques with a recombinant rhesus macaque-derived CMV (RhCMV-eGFP). Twelve cynomolgus macaques were randomly allocated to three groups: one experimental group (RhCMV-eGFP) and two control groups (UV-inactivated RhCMV-eGFP or media alone). The animals were given two subcutaneous inoculations at week 0 and week 8, and a subset of animals received an intravenous inoculation at week 23. No overt clinical or haematological changes were observed and PBMCs isolated from RhCMV-eGFP inoculated animals had comparable eGFP- and IE-1-specific cellular responses to the control animals. Following inoculation with RhCMV-eGFP, we were unable to detect evidence of infection in any blood or tissue samples up to 4 years post-inoculation, using sensitive viral co-culture, qPCR, and Western blot assays. Co-culture of urine and saliva samples demonstrated the presence of endogenous cynomolgus CMV (CyCMV) cytopathic effect, however no concomitant eGFP expression was observed. The absence of detectable RhCMV-eGFP suggests that the CyCMV-seropositive cynomolgus macaques were not productively infected with RhCMV-eGFP under these inoculation conditions. In a continued effort to develop CMV as a viral vector for an HIV/SIV vaccine, these studies demonstrate that CMV is highly restricted to its host species and can be highly affected by laboratory cell culture. Consideration of the differences between lab-adapted and primary viruses with respect to species range and cell tropism should be a priority in evaluating CMV as vaccine vector for HIV or other pathogens at the preclinical development stage.

摘要

巨细胞病毒(CMV)是一种高度物种特异性的病毒,它与宿主共同进化了数百万年,因此限制了跨物种感染。为了研究宿主限制在多大程度上可能阻碍密切相关的非人灵长类动物之间的跨物种研究,我们评估了食蟹猴经重组恒河猴源CMV(RhCMV-eGFP)进行的实验性感染。12只食蟹猴被随机分为三组:一组实验组(RhCMV-eGFP)和两组对照组(紫外线灭活的RhCMV-eGFP或仅用培养基)。动物在第0周和第8周接受两次皮下接种,一部分动物在第23周接受静脉接种。未观察到明显的临床或血液学变化,从接种RhCMV-eGFP的动物中分离的外周血单核细胞(PBMC)对对照动物具有相当的eGFP和IE-1特异性细胞反应。接种RhCMV-eGFP后,在接种后长达4年的时间里,我们使用灵敏的病毒共培养、定量聚合酶链反应(qPCR)和蛋白质印迹分析,在任何血液或组织样本中均未检测到感染证据。尿液和唾液样本的共培养显示存在内源性食蟹猴CMV(CyCMV)细胞病变效应,但未观察到相应的eGFP表达。未检测到可检测到的RhCMV-eGFP表明,在这些接种条件下,CyCMV血清阳性的食蟹猴未被RhCMV-eGFP有效感染。为了继续努力将CMV开发为HIV/SIV疫苗的病毒载体,这些研究表明CMV对其宿主物种具有高度限制,并且可能受到实验室细胞培养的高度影响。在临床前开发阶段评估CMV作为HIV或其他病原体的疫苗载体时,应优先考虑实验室适应病毒和原始病毒在物种范围和细胞嗜性方面的差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a82/4378995/f86901089b02/pone.0121339.g001.jpg

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