Epigenetic Control of Cytomegalovirus Latency and Reactivation

Liu, Xue Feng; Wang, Xueqiong; Yan, Shi; Zhang, Zheng; Abecassis, Michael; Hummel, Mary

doi:10.3390/v5051325

Cited by 46 publications

(57 citation statements)

References 111 publications

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“…IE-3 is the MCMV functional homologue of HCMV IE-2, which is the major transactivator of early gene expression (Angulo et al, 2000;Keil et al, 1987aKeil et al, , 1987bMartínez et al, 2010;Messerle et al, 1992). We previously showed that allogeneic transplantation induced reactivation of IE gene expression 48 h after transplant, and that RNA polymerase phosphorylated at Ser2 (Pol II pS2) was recruited to both the MIEP and the IE-3 coding region (Hummel et al, 2001;Liu et al, 2013). Here, we show that IE-3 RNA expression was detectable by reverse transcriptase-qPCR at 48 h, but not at 3 or 24 h post-transplant ( Fig.…”

Section: Nf-k B and Ap-1 Family Members Are Differentially Regulated supporting

confidence: 49%

“…CMV genomes are heterochromatinized and the IE genes, which are required for lytic replication, are transcriptionally silent in latent infection (Grzimek et al, 2001;Hummel et al, 2001;Kurz et al, 1997Kurz et al, , 1999Liu et al, 2008Liu et al, , 2010Seckert et al, 2013;Simon et al, 2005). Activation of IE gene expression, through recruitment of transcription factors that control MIEP activity and remodelling of viral chromatin, is therefore likely required for reactivation of the virus.…”

Section: Discussionmentioning

confidence: 99%

“…Chromatin remodelling complexes are recruited to the MIEP upon reactivation of IE gene expression MCMV genomes are highly enriched in histones in latently infected mice, suggesting that the nucleosomes are in a compacted configuration, which is closed to transcription (Liu et al, 2008). Many inducible genes require remodelling of the chromatin by the SWI/SNF complex in order to activate gene expression (Ramirez-Carrozzi et al,…”

Section: Mechanisms Of Transplant-induced MCMV Reactivationmentioning

confidence: 99%

“…However, due to the species specificity of HCMV, it has not been possible to test this hypothesis in the context of organ transplantation. Murine cytomegalovirus (MCMV) is very similar to HCMV in many important ways, including: (i) ability to establish latency and to reactivate; (ii) hierarchical regulation of viral gene expression; (iii) structure, function and organization of the major immediate early (IE) genes (Keil et al, 1987a, b;Meier & Stinski, 2013;Stenberg et al, 1984); (iv) repression of IE gene expression during latency by heterochromatinization of viral genomes (Grzimek et al, 2001;Hummel & Abecassis, 2002;Hummel et al, 2001;Kurz et al, 1999;Liu et al, 2008;Reeves & Sinclair, 2013;Reeves et al, 2005;Seckert et al, 2013); (v) the presence of similar regulatory elements (e.g. NF-k B, AP-1, Sp1 and CREB/ATF binding sites) in the viral IE enhancers Meier & Stinski, 2013); and (vi) (re)activation of the MIEP and/or IE transcription in response to inflammatory mediators or allogeneic stimulation (Döcke et al, 1994;Fietze et al, 1994;Huang et al, 2012;Hummel & Abecassis, 2002;Hummel et al, 2001;Kew et al, 2014;Lee et al, 2004;Liu et al, 2013;O'Connor & Murphy, 2012;Prösch et al, 1995;Reeves & Compton, 2011;Simon et al, 2005;Stein et al, 1993).…”

Section: Introductionmentioning

confidence: 99%

“…We previously developed a renal transplant model for reactivation of MCMV IE gene expression (Hummel et al, 2001). In this model, transplantation of latently infected kidneys into allogeneic recipients induced IE gene expression and epigenetic reprogramming of the MIEP within 48 h (Hummel et al, 2001;Liu et al, 2013). In addition, allogeneic transplantation induced expression of a lacZ reporter transgene under the control of the HCMV MIEP (MIEP-lacZ) (Hummel et al, 2001).…”

Section: Introductionmentioning

confidence: 99%

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Transplant-induced reactivation of murine cytomegalovirus immediate early gene expression is associated with recruitment of NF-κB and AP-1 to the major immediate early promoter

Liu

Jie

Zhang

et al. 2016

Journal of General Virology

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Reactivation of latent human cytomegalovirus is a significant infectious complication of organ transplantation and current therapies target viral replication once reactivation of latent virus has already occurred. The specific molecular pathways that activate viral gene expression in response to transplantation are not well understood. Our studies aim to identify these factors, with the goal of developing novel therapies that prevent transcriptional reactivation in transplant recipients. Murine cytomegalovirus (MCMV) is a valuable model for studying latency and reactivation of CMV in vivo. We previously demonstrated that transplantation of MCMV-latently infected kidneys into allogeneic recipients induces reactivation of immediate early (IE) gene expression and epigenetic reprogramming of the major immediate early promoter (MIEP) within 48 h. We hypothesize that these events are mediated by activation of signalling pathways that lead to binding of transcription factors to the MIEP, including AP-1 and NF-k B. Here we show that transplantation induces rapid activation of several members of the AP-1 and NF-k B transcription factor family and we demonstrate that canonical NF-k B (p65/p50), the junD component of AP-1, and nucleosome remodelling complexes are recruited to the MIEP following transplantation. Proteomic analysis of recipient plasma and transcriptome analysis of kidney RNA identified five extracellular ligands, including TNF, IL-1b, IL-18, CD40L and IL-6, and three intracellular signalling pathways associated with reactivation of IE gene expression. Identification of the factors that mediate activation of these signalling pathways may eventually lead to new therapies to prevent reactivation of CMV and its sequelae.

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Section: Nf-k B and Ap-1 Family Members Are Differentially Regulated supporting

confidence: 49%

Section: Discussionmentioning

confidence: 99%

Section: Mechanisms Of Transplant-induced MCMV Reactivationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Transplant-induced reactivation of murine cytomegalovirus immediate early gene expression is associated with recruitment of NF-κB and AP-1 to the major immediate early promoter

Liu

Jie

Zhang

et al. 2016

Journal of General Virology

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Cytomegalovirus (CMV) in cervical cancer screening tests: A series of 8 cases and review of the literature

Elgert

Yee‐Chang

Simsir

2018

Diagnostic Cytopathology

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Role of codon usage and tRNA changes in rat cytomegalovirus latency and (re)activation

Kanduc

2016

J. Basic Microbiol.

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Herpesviruses can remain in their hosts by establishing a latent infection with a low pattern of viral gene expression. Passage from latency to reactivation may occur under particular conditions such as immunosuppressive treatments or during fetal development, and often is accompanied by heavy pathologic sequelae. To investigate the molecular basis underlying herpesvirus latency and (re)activation, codon usage of rat cytomegalovirus was comparatively analyzed with respect to the rat codon usage. Two major points stand out as follows: (i) six codons - GCG (Ala), CCG (Pro), CGG (Arg), CGC (Arg), TCG (Ser), and ACG (Thr) - are rare in rat genes and intensively used in rat cytomegalovirus coding sequences; (ii) in many instances, the codons seldom used by the host are clustered along viral sequences coding for single amino acid repeats such as poly-Ala and poly-Thr stretches. The results indicate that rare host codons and their iteration along viral sequences might represent major constraints that lock rat cytomegalovirus translation in its host during the viral latent phase. Consequently, the data also suggest a link between rat cytomegalovirus quiescence/activation and the functional tRNA coadaptation phenomenon. Indeed, increases in minor tRNA species corresponding to rare rat codons mark rat cell proliferation and might rescue difficult viral translational contexts. Ala isoaccepting-tRNA (CGC) is reported as an example. On the whole, the present findings may contribute to explain how the molecular mechanisms that normally control host gene expression can silence/(re)activate viral gene expression, and might address research toward new approaches in anti-viral therapeutics.

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Epigenetic Control of Cytomegalovirus Latency and Reactivation

Cited by 46 publications

References 111 publications

Transplant-induced reactivation of murine cytomegalovirus immediate early gene expression is associated with recruitment of NF-κB and AP-1 to the major immediate early promoter

Transplant-induced reactivation of murine cytomegalovirus immediate early gene expression is associated with recruitment of NF-κB and AP-1 to the major immediate early promoter

Cytomegalovirus (CMV) in cervical cancer screening tests: A series of 8 cases and review of the literature

Role of codon usage and tRNA changes in rat cytomegalovirus latency and (re)activation

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