Your search keyword '"Muromegalovirus"' showing total 761 results

1. Inconsistent reversal of HIV-1 latency ex vivo by antigens of HIV-1, CMV, and other infectious agents

Author

Vollbrecht, Thomas, Angerstein, Aaron O, Menke, Bryson, Kumar, Nikesh M, de Oliveira, Michelli Faria, Richman, Douglas D, and Guatelli, John C

Subjects

Microbiology, Biological Sciences, HIV/AIDS, Clinical Research, Infectious Diseases, 2.2 Factors relating to the physical environment, Aetiology, Infection, Good Health and Well Being, Adult, Aged, Antigen Presentation, Antigens, CD4-Positive T-Lymphocytes, Dendritic Cells, Female, HIV Infections, HIV-1, Humans, Immunologic Memory, Interferon-gamma, Male, Middle Aged, Muromegalovirus, RNA, Messenger, RNA, Viral, Virion, Virus Activation, Virus Latency, Latency, Antigen, CD4 T cell, Clinical Sciences, Virology

Abstract

BackgroundA reservoir of replication-competent but latent virus is the main obstacle to a cure for HIV-1 infection. Much of this reservoir resides in memory CD4 T cells. We hypothesized that these cells can be reactivated with antigens from HIV-1 and other common pathogens to reverse latency.ResultsWe obtained mononuclear cells from the peripheral blood of antiretroviral-treated patients with suppressed viremia. We tested pools of peptides and proteins derived from HIV-1 and from other pathogens including CMV for their ability to reverse latency ex vivo by activation of memory responses. We assessed activation of the CD4 T cells by measuring the up-regulation of cell-surface CD69. We assessed HIV-1 expression using two assays: a real-time PCR assay for virion-associated viral RNA and a droplet digital PCR assay for cell-associated, multiply spliced viral mRNA. Reversal of latency occurred in a minority of cells from some participants, but no single antigen induced HIV-1 expression ex vivo consistently. When reversal of latency was induced by a specific peptide pool or protein, the extent was proportionally greater than that of T cell activation.ConclusionsIn this group of patients in whom antiretroviral therapy was started during chronic infection, the latent reservoir does not appear to consistently reside in CD4 T cells of a predominant antigen-specificity. Peptide-antigens reversed HIV-1 latency ex vivo with modest and variable activity. When latency was reversed by specific peptides or proteins, it was proportionally greater than the extent of T cell activation, suggesting partial enrichment of the latent reservoir in cells of specific antigen-reactivity.

Published

2020

2. Atomic structures and deletion mutant reveal different capsid-binding patterns and functional significance of tegument protein pp150 in murine and human cytomegaloviruses with implications for therapeutic development.

Author

Liu, Wei, Dai, Xinghong, Jih, Jonathan, Chan, Karen, Trang, Phong, Yu, Xuekui, Balogun, Rilwan, Mei, Ye, Liu, Fenyong, and Zhou, Z Hong

Subjects

Animals, Humans, Mice, Cytomegalovirus, Muromegalovirus, Virion, Capsid, Cytomegalovirus Infections, Phosphoproteins, Capsid Proteins, Viral Matrix Proteins, Cryoelectron Microscopy, Virus Assembly, Sequence Deletion, Genome, Viral, Vaccine Related, Immunization, Infectious Diseases, Infection, Virology, Microbiology, Immunology, Medical Microbiology

Abstract

Cytomegalovirus (CMV) infection causes birth defects and life-threatening complications in immunosuppressed patients. Lack of vaccine and need for more effective drugs have driven widespread ongoing therapeutic development efforts against human CMV (HCMV), mostly using murine CMV (MCMV) as the model system for preclinical animal tests. The recent publication (Yu et al., 2017, DOI: 10.1126/science.aam6892) of an atomic model for HCMV capsid with associated tegument protein pp150 has infused impetus for rational design of novel vaccines and drugs, but the absence of high-resolution structural data on MCMV remains a significant knowledge gap in such development efforts. Here, by cryoEM with sub-particle reconstruction method, we have obtained the first atomic structure of MCMV capsid with associated pp150. Surprisingly, the capsid-binding patterns of pp150 differ between HCMV and MCMV despite their highly similar capsid structures. In MCMV, pp150 is absent on triplex Tc and exists as a "Λ"-shaped dimer on other triplexes, leading to only 260 groups of two pp150 subunits per capsid in contrast to 320 groups of three pp150 subunits each in a "Δ"-shaped fortifying configuration. Many more amino acids contribute to pp150-pp150 interactions in MCMV than in HCMV, making MCMV pp150 dimer inflexible thus incompatible to instigate triplex Tc-binding as observed in HCMV. While pp150 is essential in HCMV, our pp150-deletion mutant of MCMV remained viable though with attenuated infectivity and exhibiting defects in retaining viral genome. These results thus invalidate targeting pp150, but lend support to targeting capsid proteins, when using MCMV as a model for HCMV pathogenesis and therapeutic studies.

Published

2019

3. Rapid and sequential quantitation of salivary gland-associated mouse cytomegalovirus in oral lavage

Author

Kamimura, Yosuke and Lanier, Lewis L

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Digestive Diseases, Infectious Diseases, Dental/Oral and Craniofacial Disease, Aetiology, 2.1 Biological and endogenous factors, Infection, Inflammatory and immune system, Animals, Cytomegalovirus Infections, Disease Models, Animal, Killer Cells, Natural, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Muromegalovirus, Saliva, Salivary Glands, T-Lymphocytes, Therapeutic Irrigation, Time Factors, Viral Load, Cytomegalovirus, Protocols, PCR, Microbiology, Virology, Medical microbiology

Abstract

Cytomegalovirus (CMV) establishes a persistent infection in the salivary glands and transmits to other hosts. Mouse cytomegalovirus (MCMV) is a well-characterized model for studying the mechanisms of host responses against CMV. The viral load in salivary glands has been measured traditionally because it has been considered to reflect the consequence of anti-virus responses by T cells and natural killer (NK) cells. However, the standard plaque assay is cumbersome and it is impossible to monitor sequentially the viral load in same host. Hence, the goal of this study was to develop a real-time quantitative PCR (qPCR)-based procedure to measure the viral load in oral lavage. This report demonstrates that the viral load in oral lavage correlates well with viral titers in the salivary glands. This method allows sequential quantitation of viral loads without sacrificing mice and provides a technique that will facilitate kinetic studies of anti-viral immunity mediated by the innate and adaptive immune systems.

Published

2014

4. Expression of the RAE-1 family of stimulatory NK-cell ligands requires activation of the PI3K pathway during viral infection and transformation.

Author

Tokuyama, Maria, Lorin, Clarisse, Delebecque, Frederic, Jung, Heiyoun, Raulet, David H, and Coscoy, Laurent

Subjects

Killer Cells, Natural, Cell Line, Tumor, Fibroblasts, Animals, Mice, Muromegalovirus, Cytomegalovirus Infections, Cell Transformation, Viral, Nucleocytoplasmic Transport Proteins, Nuclear Matrix-Associated Proteins, Ligands, Catalytic Domain, Receptors, Natural Killer Cell, NK Cell Lectin-Like Receptor Subfamily K, Phosphatidylinositol 3-Kinases, Class I Phosphatidylinositol 3-Kinases, Phosphatidylinositol 3-Kinase, Infectious Diseases, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Inflammatory and immune system, Infection, Virology, Microbiology, Immunology, Medical Microbiology

Abstract

Natural killer (NK) cells are lymphocytes that play a major role in the elimination of virally-infected cells and tumor cells. NK cells recognize and target abnormal cells through activation of stimulatory receptors such as NKG2D. NKG2D ligands are self-proteins, which are absent or expressed at low levels on healthy cells but are induced upon cellular stress, transformation, or viral infection. The exact molecular mechanisms driving expression of these ligands remain poorly understood. Here we show that murine cytomegalovirus (MCMV) infection activates the phosphatidylinositol-3-kinase (PI3K) pathway and that this activation is required for the induction of the RAE-1 family of mouse NKG2D ligands. Among the multiple PI3K catalytic subunits, inhibition of the p110α catalytic subunit blocks this induction. Similarly, inhibition of p110α PI3K reduces cell surface expression of RAE-1 on transformed cells. Many viruses manipulate the PI3K pathway, and tumors frequently mutate the p110α oncogene. Thus, our findings suggest that dysregulation of the PI3K pathway is an important signal to induce expression of RAE-1, and this may represent a commonality among various types of cellular stresses that result in the induction of NKG2D ligands.

Published

2011

5. Evolutionarily conserved herpesviral protein interaction networks.

Author

Fossum, Even, Friedel, Caroline C, Rajagopala, Seesandra V, Titz, Björn, Baiker, Armin, Schmidt, Tina, Kraus, Theo, Stellberger, Thorsten, Rutenberg, Christiane, Suthram, Silpa, Bandyopadhyay, Sourav, Rose, Dietlind, von Brunn, Albrecht, Uhlmann, Mareike, Zeretzke, Christine, Dong, Yu-An, Boulet, Hélène, Koegl, Manfred, Bailer, Susanne M, Koszinowski, Ulrich, Ideker, Trey, Uetz, Peter, Zimmer, Ralf, and Haas, Jürgen

Subjects

Hela Cells, Humans, Herpesviridae, Herpesvirus 1, Human, Herpesvirus 3, Human, Muromegalovirus, Herpesvirus 4, Human, Herpesvirus 8, Human, Virion, Viral Proteins, Viral Core Proteins, Immunohistochemistry, Cluster Analysis, Protein Interaction Mapping, Evolution, Molecular, Phylogeny, Signal Transduction, HeLa Cells, Evolution, Molecular, Herpesvirus 1, Human, Herpesvirus 3, Herpesvirus 4, Herpesvirus 8, Virology, Microbiology, Immunology, Medical Microbiology

Abstract

Herpesviruses constitute a family of large DNA viruses widely spread in vertebrates and causing a variety of different diseases. They possess dsDNA genomes ranging from 120 to 240 kbp encoding between 70 to 170 open reading frames. We previously reported the protein interaction networks of two herpesviruses, varicella-zoster virus (VZV) and Kaposi's sarcoma-associated herpesvirus (KSHV). In this study, we systematically tested three additional herpesvirus species, herpes simplex virus 1 (HSV-1), murine cytomegalovirus and Epstein-Barr virus, for protein interactions in order to be able to perform a comparative analysis of all three herpesvirus subfamilies. We identified 735 interactions by genome-wide yeast-two-hybrid screens (Y2H), and, together with the interactomes of VZV and KSHV, included a total of 1,007 intraviral protein interactions in the analysis. Whereas a large number of interactions have not been reported previously, we were able to identify a core set of highly conserved protein interactions, like the interaction between HSV-1 UL33 with the nuclear egress proteins UL31/UL34. Interactions were conserved between orthologous proteins despite generally low sequence similarity, suggesting that function may be more conserved than sequence. By combining interactomes of different species we were able to systematically address the low coverage of the Y2H system and to extract biologically relevant interactions which were not evident from single species.

Published

2009

6. Two murine cytomegalovirus microRNAs target the major viral immediate early 3 gene

Author

Stefanie Herb, Jelena Zeleznjak, Thomas Hennig, Anne L'Hernault, Manivel Lodha, Christopher Jürges, Tihana Trsan, Vanda Juranic Lisnic, Stipan Jonjic, Florian Erhard, Astrid Krmpotic, and Lars Dölken

Subjects

Muromegalovirus, immediate early genes, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, CD8-Positive T-Lymphocytes, miRNA, Mice, MicroRNAs, Virology, Humans, Animals, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti, Genes, Immediate-Early, 3' Untranslated Regions, cytomegalovirus

Abstract

Human cytomegalovirus is responsible for morbidity and mortality in immune compromised patients and is the leading viral cause of congenital infection. Virus-encoded microRNAs (miRNAs) represent interesting targets for novel antiviral agents. While many cellular targets that augment productive infection have been identified in recent years, regulation of viral genes such as the major viral immediate early protein 72 (IE72) by hcmv-miR-UL112-1 may contribute to both the establishment and the maintenance of latent infection. We employed photoactivated ribonucleotide-enhanced individual nucleotide resolution crosslinking (PAR-iCLIP) to identify murine cytomegalovirus (MCMV) miRNA targets during lytic infection. While the PAR-iCLIP data were of insufficient quality to obtain a comprehensive list of cellular and viral miRNA targets, the most prominent PAR-iCLIP peak in the MCMV genome mapped to the 3′ untranslated region of the major viral immediate early 3 ( ) transcript. We show that this results from two closely positioned binding sites for the abundant MCMV miRNAs miR-M23-2-3p and miR-m01-2-3p. Their pre-expression significantly impaired viral plaque formation. However, mutation of the respective binding sites did not alter viral fitness during acute or subacute infection . Furthermore, no differences in the induction of virus-specific CD8 T cells were observed. Future studies will probably need to go beyond studying immunocompetent laboratory mice housed in pathogen-free conditions to reveal the functional relevance of viral miRNA-mediated regulation of key viral immediate early genes.

Published

2022

7. Mouse Models for Cytomegalovirus Infections in Newborns and Adults

Author

Ilija Brizić, Berislav Lisnić, Fran Krstanović, Wolfram Brune, Hartmut Hengel, and Stipan Jonjić

Subjects

Medical Laboratory Technology, Disease Models, Animal, Mice, Muromegalovirus, General Immunology and Microbiology, cytomegalovirus infections, disease models, fibroblasts, herpesviridae infections, MCMV, mice, mouse cytomegalovirus, salivary gland, viral load, viral plaque assay, virology, virus replication, General Neuroscience, Cytomegalovirus Infections, Animals, Health Informatics, General Pharmacology, Toxicology and Pharmaceutics, General Biochemistry, Genetics and Molecular Biology, Salivary Glands

Abstract

This article describes procedures for infecting adult mice with murine cytomegalovirus (MCMV) and for infecting newborn mice to model congenital CMV infection. Methods are included for propagating MCMV in cell cultures and preparing a more virulent form of MCMV from the salivary glands of infected mice. A plaque assay is provided for determining MCMV titers of infected tissues or virus stocks. Also, methods are described for preparing the murine embryonic fibroblasts used for propagating MCMV, and for the plaque assay. © 2022 Wiley Periodicals LLC.

Published

2022

8. Recent Advancements in Understanding Primary Cytomegalovirus Infection in a Mouse Model

Author

Kimberley Bruce, Jiawei Ma, Clara Lawler, Wanxiaojie Xie, Philip G. Stevenson, and Helen E. Farrell

Subjects

Disease Models, Animal, Mice, Muromegalovirus, Infectious Diseases, Virology, Cytomegalovirus Infections, Animals, Cytomegalovirus, Humans, Herpesviridae Infections, Antiviral Agents

Abstract

Animal models that mimic human infections provide insights in virus–host interplay; knowledge that in vitro approaches cannot readily predict, nor easily reproduce. Human cytomegalovirus (HCMV) infections are acquired asymptomatically, and primary infections are difficult to capture. The gap in our knowledge of the early events of HCMV colonization and spread limits rational design of HCMV antivirals and vaccines. Studies of natural infection with mouse cytomegalovirus (MCMV) have demonstrated the olfactory epithelium as the site of natural colonization. Systemic spread from the olfactory epithelium is facilitated by infected dendritic cells (DC); tracking dissemination uncovered previously unappreciated DC trafficking pathways. The olfactory epithelium also provides a unique niche that supports efficient MCMV superinfection and virus recombination. In this review, we summarize recent advances to our understanding of MCMV infection and spread and the tissue-specific mechanisms utilized by MCMV to modulate DC trafficking. As these mechanisms are likely conserved with HCMV, they may inform new approaches for preventing HCMV infections in humans.

Published

2022

9. The Role of Autophagy in Murine Cytomegalovirus Hepatitis

Author

Xing-lou Liu, Lin-Lin Zhang, Yidan Bi, Yuanyuan Lu, Feng Fang, and Xinyan Zhang

Subjects

0301 basic medicine, Human cytomegalovirus, Muromegalovirus, viruses, Immunology, Cytomegalovirus, Inflammation, Biology, Hepatitis, Pathogenesis, Mice, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, Western blot, Virology, Autophagy, medicine, Animals, Protein kinase B, PI3K/AKT/mTOR pathway, Mice, Inbred BALB C, medicine.diagnostic_test, virus diseases, medicine.disease, 030104 developmental biology, Cytomegalovirus Infections, Molecular Medicine, 030211 gastroenterology & hepatology, medicine.symptom

Abstract

Autophagy is involved in the pathogenesis of multiple pathogen infection. Previous studies have reported that human cytomegalovirus (CMV) activates autophagy in the early stage of infection and then inhibits autophagy. Little is known about the role of autophagy in murine CMV (MCMV) infection, especially in MCMV-induced hepatitis. The purpose of this study is to investigate the role of autophagy in MCMV hepatitis. BALB/c mice were infected with MCMV and a series of experiments involving western blot, immunofluorescence, immunohistochemistry, HE (Hematoxylin and Eosin) staining and quantitative real-time polymerase chain reaction were performed in this study. The expression of SQSTM1/p62, PI3K, the ratio of phosphorylated Akt to total Akt, and the ratio of phosphorylated mammalian target of rapamycin (mTOR) to total mTOR were increased, and the expression of light-chain 3 (LC3)-II were decreased in the livers of infected mice on days 3 and 7 postinfection (p.i.). Compared with the untreated infected group, increased transcription level of MCMV glycoprotein B (gB), increased expression levels of interleukin1-β (IL-1β), aspartate aminotransferase (AST) and alanine aminotransferase (ALT), decreased expression level of type I interferon α (IFN-α), as well as aggravated liver pathological injury were detected in starvation-treated infected group on days 3 and 7 p.i.; whereas decreased transcription level of MCMV gB, decreased expression levels of IL-1β, AST and ALT, increased expression level of type I IFN-α, as well as alleviated liver pathological injury were detected in chloroquine (CQ)-treated infected group on day 3 p.i. In conclusion, autophagy is inhibited through activating the PI3K/Akt/mTOR pathway in the liver of BALB/c mice during MCMV infection, and autophagy may promote MCMV replication and aggravate liver pathological damage and inflammation. Further understanding of the interactions between autophagy and MCMV infection and its potential mechanism may bring new important cues to the control of MCMV infection and antiviral therapy.

Published

2021

10. Decoding murine cytomegalovirus

Author

Manivel Lodha, Ihsan Muchsin, Christopher Jürges, Vanda Juranic Lisnic, Anne L’hernault, Andrzej J. Rutkowski, Bhupesh Prusty, Arnhild Grothey, Andrea Milic, Thomas Hennig, Stipan Jonjic, Caroline C. Friedel, Florian Erhard, Lars Dölken, Dölken, Lars [0000-0002-4651-3544], and Apollo - University of Cambridge Repository

Subjects

Muromegalovirus, Base Sequence, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, Immunology, Cytomegalovirus, Microbiology, Mice, Viral Proteins, Open Reading Frames, Virology, Genetics, Animals, Humans, Parasitology, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti, Molecular Biology

Abstract

The genomes of both human cytomegalovirus (HCMV) and murine cytomegalovirus (MCMV) were first sequenced over 20 years ago. Similar to HCMV, the MCMV genome had initially been proposed to harbor ≈170 open reading frames (ORFs). More recently, omics approaches revealed HCMV gene expression to be substantially more complex comprising several hundreds of translated ORFs. Here, we provide a state-of-the art reannotation of lytic MCMV gene expression based on integrative analysis of a large set of omics data. Our data reveal 363 viral transcription start sites (TiSS) that give rise to 380 and 454 viral transcripts and ORFs, respectively. The latter include >200 small ORFs, some of which represented the most highly expressed viral gene products. By combining TiSS profiling with metabolic RNA labelling and chemical nucleotide conversion sequencing (dSLAM-seq), we provide a detailed picture of the expression kinetics of viral transcription. This not only resulted in the identification of a novel MCMV immediate early transcript encoding the m166.5 ORF, which we termedie4, but also revealed a group of well-expressed viral transcripts that are induced later than canonical true late genes and contain an initiator element (Inr) but no TATA- or TATT-box in their core promoters. We show that viral uORFs tune gene expression of longer viral ORFs expressed incisat translational level. Finally, we identify a truncated isoform of the viral NK-cell immune evasin m145 arising from a viral TiSS downstream of the canonical m145 mRNA. Despite being ≈5-fold more abundantly expressed than the canonical m145 protein it was not required for downregulating the NK cell ligand, MULT-I. In summary, our work will pave the way for future mechanistic studies on previously unknown cytomegalovirus gene products in an important virus animal model.Author summaryWe conducted a comprehensive characterization and reannotation of murine cytomegalovirus (MCMV) gene expression during lytic infection in murine fibroblasts using an integrative multi-omics approach. This unveiled hundreds of novel transcripts that explained the expression of close to 300 so far unknown viral open reading frames (ORFs). Interestingly, small viral ORFs (sORFs) were amongst the most highly expressed viral gene products and thus presumably encode for important viral microproteins of unknown function. However, we also show that sORFs located upstream of larger ORFs tune the expression of the downstream ORFs at the level of translation. We classified viral transcription start sites (TiSS) based on their expression kinetics obtained by a new combination of metabolic RNA labelling with transcription start sites profiling. This not only identified a so far unknown viral immediate-early transcript (ie4, m166.5 RNA) but also revealed a novel class of viral late transcripts that are expressed later than canonical true late genes and lack TATA box-like motifs. We exemplify for the m145 locus how so far unknown TiSS give rise to abundantly expressed truncated viral proteins. In summary, we provide a state-of-the-art annotation of an important model virus, which will be instrumental for future studies on CMV biology, immunology and pathogenesis.

Published

2023

11. CD4 + T Cells Control Murine Cytomegalovirus Infection Indirectly

Author

Wanxiaojie Xie, Byungchul Lee, Kimberley Bruce, Clara Lawler, Helen E. Farrell, and Philip G. Stevenson

Subjects

CD4-Positive T-Lymphocytes, Interferon-gamma, Mice, Muromegalovirus, Virology, Insect Science, Cytomegalovirus Infections, Immunology, Pathogenesis and Immunity, Animals, Humans, Antiviral Agents, Microbiology

Abstract

CD4(+) T cells are key to controlling cytomegalovirus infections. Salivary gland infection by murine cytomegalovirus (MCMV) provides a way to identify mechanisms. CD11c(+) dendritic cells (DC) disseminate MCMV to the salivary glands, where they transfer infection to acinar cells. Antiviral CD4(+) T cells are often considered to be directly cytotoxic for cells expressing major histocompatibility complex class II (MHCII). However, persistently infected salivary gland acinar cells are MHCII(−) and are presumably inaccessible to direct CD4 T cell recognition. Here, we show that CD4(+) T cell depletion amplified infection of MHCII(−) acinar cells but not MHCII(+) cells. MCMV-infected mice with disrupted MHCII on CD11c(+) cells showed increased MHCII(−) acinar infection; antiviral CD4(+) T cells were still primed, but their recruitment to the salivary glands was reduced, suggesting that engagement with local MHCII(+) DC is important for antiviral protection. As MCMV downregulates MHCII on infected DC, the DC participating in CD4 protection may thus be uninfected. NK cells and gamma interferon (IFN-γ) may also contribute to CD4(+) T cell-dependent virus control: CD4 T cell depletion reduced NK cell recruitment to the salivary glands, and both NK cell and IFN-γ depletion equalized infection between MHCII-disrupted and control mice. Taken together, these results suggest that CD4(+) T cells protect indirectly against infected acinar cells in the salivary gland via DC engagement, requiring the recruitment of NK cells and the action of IFN-γ. Congruence of these results with an established CD4(+) T cell/NK cell axis of gammaherpesvirus infection control suggests a common mode of defense against evasive viruses. IMPORTANCE Cytomegalovirus infections commonly cause problems in immunocompromised patients and in pregnancy. We lack effective vaccines. CD4(+) T cells play an important role in normal infection control, yet how they act has been unknown. Using murine cytomegalovirus as an accessible model, we show that CD4(+) T cells are unlikely to recognize infected cells directly. We propose that CD4(+) T cells interact with uninfected cells that present viral antigens and recruit other immune cells to attack infected targets. These data present a new outlook on understanding how CD4(+) T cell-directed control protects against persistent cytomegalovirus infection.

Published

2022

12. Heart Dysfunction Following Long-Term Murine Cytomegalovirus Infection: Fibrosis, Hypertrophy, and Tachycardia

Author

Timothy M. White, Rhonda D. Cardin, Cassandra M Bonavita, and Joseph Francis

Subjects

0301 basic medicine, Tachycardia, Human cytomegalovirus, Muromegalovirus, Myocarditis, Time Factors, murine cytomegalovirus, Viral pathogenesis, viruses, Immunology, Congenital cytomegalovirus infection, viral reactivation, Virus Replication, Salivary Glands, Muscle hypertrophy, 03 medical and health sciences, 0302 clinical medicine, heart function, Fibrosis, Virology, medicine, Animals, Humans, cytomegalovirus, Research Articles, Mice, Inbred BALB C, viral pathogenesis, business.industry, Myocardium, virus diseases, Heart, Herpesviridae Infections, Hypertrophy, medicine.disease, Virus Latency, Cytomegalovirus infection, 030104 developmental biology, Molecular Medicine, 030211 gastroenterology & hepatology, Female, Virus Activation, medicine.symptom, business, Spleen

Abstract

Human cytomegalovirus (HCMV) is associated with increased risk of chronic diseases of the heart and vasculature, including myocarditis, atherosclerosis, and transplant vasculopathy. To investigate CMV infection of the heart, murine cytomegalovirus (MCMV) was used to evaluate both acute and latent infection and the subsequent phenotypic and functional consequences of infection. Female BALB/c mice were intraperitoneally (i.p.) inoculated with 1 × 106 pfu of MCMV and evaluated at 14 and 50 days postinfection (dpi). At each time point, echocardiography was used to evaluate cardiac function and histology was conducted for phenotypic evaluation. MCMV replication in the heart was detected as early as 3 dpi and was no longer detectable at 14 dpi. Infected animals had significant cardiac pathology at 14 and 50 dpi when compared to uninfected controls. Histology revealed fibrosis of the heart as early as 14 dpi and the presence of white fibrous deposits on the surface of the heart. Functional evaluation showed significantly increased heart rate and muscle thickening in the latently infected animals when compared to the control animals. At 50 dpi, latent virus was measured by explant reactivation assay, demonstrating that MCMV establishes latency and is capable of reactivation from the heart, similar to other tissues such as spleen and salivary glands. Collectively, these studies illustrate that MCMV infection results in phenotypic alterations within the heart as early as 14 dpi, which progress to functional abnormalities during latency. These findings are similar to sinus tachycardia and hypertrophy of the heart muscle observed in cases of HCMV-induced acute myocarditis.

Published

2020

13. The Mouse Cytomegalovirus G Protein-Coupled Receptor Homolog, M33, Coordinates Key Features of In Vivo Infection via Distinct Components of Its Signaling Repertoire

Author

Jiawei Ma, Kimberley Bruce, Nicholas Davis-Poynter, Philip G. Stevenson, and Helen E. Farrell

Subjects

Mice, Inbred BALB C, Muromegalovirus, Immunology, Phospholipase C beta, Dendritic Cells, Herpesviridae Infections, GTP-Binding Protein alpha Subunits, Gi-Go, Microbiology, Salivary Glands, Receptors, G-Protein-Coupled, Mice, Viral Proteins, Virology, Insect Science, Mutation, Pathogenesis and Immunity, Animals, Virus Activation, Lymph Nodes, Viremia, Cyclic AMP Response Element-Binding Protein, Signal Transduction

Abstract

Common to all cytomegalovirus (CMV) genomes analyzed to date is the presence of G protein-coupled receptors (GPCR). Animal models of CMV provide insights into their role in viral fitness. The mouse cytomegalovirus (MCMV) GPCR, M33, facilitates dendritic cell (DC)-dependent viremia, the extravasation of blood-borne infected DCs to the salivary gland, and the frequency of reactivation events from latently infected tissue explants. Constitutive G protein-coupled M33 signaling is required for these phenotypes, although the contribution of distinct biochemical pathways activated by M33 is unknown. M33 engages G(q/11) to constitutively activate phospholipase C β (PLCβ) and downstream cyclic AMP response-element binding protein (CREB) in vitro. Identification of a MCMV M33 mutant (M33(ΔC38)) for which CREB signaling was disabled but PLCβ activation was preserved provided the opportunity to investigate their relevance in vivo. Following intranasal infection with MCMV M33(ΔC38), the absence of M33 CREB G(q/11)-dependent signaling correlated with reduced mobilization of lytically-infected DCs to the draining lymph node high endothelial venules (HEVs) and reduced viremia compared with wild type MCMV. In contrast, M33(ΔC38)-infected DCs within the vascular compartment extravasated to the salivary glands via a pertussis toxin-sensitive, G(i/o)-dependent, and CREB-independent mechanism. In the context of MCMV latency, spleen explants from M33(ΔC38)-infected mice were markedly attenuated for reactivation. Taken together, these data demonstrate that key features of the MCMV life cycle are coordinated in diverse tissues by distinct pathways of the M33 signaling repertoire. IMPORTANCE G protein-coupled receptors (GPCRs) act as cell surface molecular “switches” that regulate the cellular response to environmental stimuli. All cytomegalovirus (CMV) genomes analyzed to date possess GPCR homologs with phylogenetic evidence for independent gene capture events, signifying important in vivo roles. The mouse CMV (MCMV) GPCR homolog, designated M33, is important for cell-associated virus spread and the establishment and/or reactivation of latent MCMV infection. The signaling repertoire of M33 is distinct from cellular GPCRs and little is known of the relevance of component signaling pathways for in vivo M33 function. In this report, we showed that temporal and tissue-specific M33 signaling was required to facilitate in vivo infection. Understanding the relevance of the viral GPCR signaling profiles for in vivo function will provide opportunities for future targeted interventions.

Published

2022

14. The Synthesis and Anti-Cytomegalovirus Activity of Piperidine-4-Carboxamides

Author

Xin Guo, Ayan Kumar Ghosh, Robert F. Keyes, Francis Peterson, Michael Forman, David J. Meyers, and Ravit Arav-Boger

Subjects

Muromegalovirus, Molecular Structure, Herpesvirus 2, Human, Cytomegalovirus, Herpesvirus 1, Human, Microbial Sensitivity Tests, Viral Load, Virus Replication, Antiviral Agents, Mice, Structure-Activity Relationship, Infectious Diseases, Virology, Hepatocytes, Animals, Humans, cytomegalovirus, mouse cytomegalovirus, piperidine-4-carboxamides, add-on removal, Ganciclovir, Cells, Cultured

Abstract

Treatment options for human cytomegalovirus (CMV) remain limited and are associated with significant adverse effects and the selection of resistant CMV strains in transplant recipients and congenitally infected infants. Although most approved drugs target and inhibit the CMV DNA polymerase, additional agents with distinct mechanisms of action are needed for the treatment and prevention of CMV. In a large high throughput screen using our CMV-luciferase reporter Towne, we identified several unique inhibitors of CMV replication. Here, we synthesize and test in vitro 13 analogs of the original NCGC2955 hit (1). Analogs with no activity against the CMV-luciferase at 10 µM and 30 µM (2–6, 10–14) were removed from further analysis. Three analogs (7–9) inhibited CMV replication in infected human foreskin fibroblasts. The EC50 of (1) was 1.7 ± 0.6 µM and 1.99 ± 0.15 µM, based on luciferase and plaque assay, respectively. Compounds 7, 8, and 9 showed similar activities: the EC50 values of 7 were 0.21 ± 0.06 µM (luciferase) and 0.55 ± 0.06 (plaque), of 8: 0.28 ± 0.06 µM and 0.42 ± 0.07, and of 9: 0.30 ± 0.05 µM (luciferase) and 0.35 ± 0.07 (plaque). The CC50 for 7, 8, and 9 in non-infected human foreskin fibroblasts was > 500µM, yielding a selectivity index of >1500. Compounds 1, 7, and 8 were also tested in CMV-infected primary human hepatocytes and showed a dose–response against CMV by luciferase activity and viral protein expression. None of the active compounds inhibited herpes simplex virus 1 or 2. Compounds 7 and 8 inhibited mouse CMV replication in vitro. Both inhibited CMV at late stages of replication; 7 reduced virus yield at all late time points, although not to the same degree as letermovir. Finally, the activity of analog 8 was additive with newly identified CMV inhibitors (MLS8969, NFU1827, MSL8554, and MSL8091) and with ganciclovir. Further structural activity development should provide promising anti-CMV agents for use in clinical studies.

Published

2022

15. Characterization of M116.1p, a Murine Cytomegalovirus Protein Required for Efficient Infection of Mononuclear Phagocytes

Author

Barbara Adler, Daria Kveštak, Ana Vrbanović, Kristina Gotovac Jerčić, Vanda Juranić Lisnić, Berislav Lisnić, Maja Cokarić Brdovčak, Fran Borovečki, Hana Mahmutefendić Lučin, Tihana Lenac Rovis, Tina Ružić, Jelena Železnjak, Pero Lučin, Deni Oreb, and Stipan Jonjić

Subjects

Human cytomegalovirus, Muromegalovirus, Glycosylation, Transcription, Genetic, medicine.drug_class, viruses, Immunology, intranasal infection, Biology, virus entry, Virus Replication, Monoclonal antibody, medicine.disease_cause, Microbiology, Virus, Mice, Immune system, Viral Envelope Proteins, Virology, medicine, Animals, cytomegalovirus, macrophages, mononuclear phagocyte, mouse cytomegalovirus, viral assembly compartment, viral pathogenesis, Mononuclear Phagocyte System, Tropism, Infectivity, Membrane Glycoproteins, Virus Assembly, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, Virion, virus diseases, Cytomegalovirus, Herpesviridae Infections, Fibroblasts, Virus Internalization, medicine.disease, Virus-Cell Interactions, Insect Science, Tissue tropism, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti

Abstract

Broad tissue tropism of cytomegaloviruses (CMVs) is facilitated by different glycoprotein entry complexes, which are conserved between human CMV (HCMV) and murine CMV (MCMV). Among the wide array of cell types susceptible to the infection, mononuclear phagocytes (MNPs) play a unique role in the pathogenesis of the infection as they contribute both to the virus spread and immune control. CMVs have dedicated numerous genes for the efficient infection and evasion of macrophages and dendritic cells. In this study, we have characterized the properties and function of , a previously poorly described but highly transcribed MCMV gene region that encodes M116.1p, a novel protein necessary for the efficient infection of MNPs and viral spread . Our study further revealed that M116.1p shares similarities with its positional homologs in HCMV and RCMV, UL116 and R116, respectively, such as late kinetics of expression, N-glycosylation, localization to the virion assembly compartment, and interaction with gH—a member of the CMVs fusion complex. This study, therefore, expands our knowledge about virally encoded glycoproteins that play important roles in viral infectivity and tropism. Human cytomegalovirus (HCMV) is a species-specific herpesvirus that causes severe disease in immunocompromised individuals and immunologically immature neonates. Murine cytomegalovirus (MCMV) is biologically similar to HCMV, and it serves as a widely used model for studying the infection, pathogenesis, and immune responses to HCMV. In our previous work, we have identified the ORF as one of the most extensively transcribed regions of the MCMV genome without an assigned function. This study shows that the M116 locus codes for a novel protein, M116.1p, which shares similarities with UL116 and R116 in HCMV and RCMV, respectively, and is required for the efficient infection of mononuclear phagocytes and virus spread Furthermore, this study establishes the α-M116 monoclonal antibody and MCMV mutants lacking M116, generated in this work, as valuable tools for studying the role of macrophages and dendritic cells in limiting CMV infection following different MCMV administration routes.

Published

2022

16. Murine cytomegalovirus disseminates independently of CX3CR1, CCL2 or its m131/m129 chemokine homologue

Author

Kimberley Bruce, Philip G. Stevenson, Helen E. Farrell, and Alec J. Redwood

Subjects

0301 basic medicine, Muromegalovirus, Chemokine, Salivary gland infection, CX3C Chemokine Receptor 1, CD11c, CCL2, Virus Replication, medicine.disease_cause, Monocytes, Mice, Viral Proteins, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, Virology, CX3CR1, medicine, Animals, Receptor, Chemokine CCL2, Mice, Knockout, biology, Monocyte, Cytomegalovirus, Dendritic Cells, Herpesviridae Infections, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Chemokines, CC, Host-Pathogen Interactions, biology.protein, Protein Binding, 030215 immunology

Abstract

Cytomegaloviruses (CMVs) use myeloid cells to move within their hosts. Murine CMV (MCMV) colonizes the salivary glands for long-term shedding, and reaches them via CD11c+ infected cells. A need to recruit patrolling monocytes for systemic spread has been proposed, based on poor salivary gland infection in fractalkine receptor (CX3CR1)-deficient mice. We found no significant CX3CR1 dependence of salivary gland infection. CCL2 and the viral m131/m129 chemokine homologue were also redundant for acute MCMV spread, arguing against a need for inflammation or infection to recruit additional monocytes to the entry site. M131/m129 promoted salivary gland infection, but only after the initial seeding of infected cells to this site. Our data support the idea that MCMV disseminates by infecting and mobilizing tissue-resident dendritic cells.

Published

2019

17. Production- and Purification-Relevant Properties of Human and Murine Cytomegalovirus

Author

Sanda Ravlić, Marija Brgles, Lea Hiršl, Stipan Jonjić, and Beata Halassy

Subjects

Muromegalovirus, Virus Cultivation, purification, HCMV, MCMV, ion exchange chromatography, virus, ultracentrifugation, clarification, cytomegalovirus, viruses, Exosomes, Microbiology, Article, Cell Line, Mice, Virology, Animals, Humans, Cryopreservation, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, virus diseases, Chromatography, Ion Exchange, QR1-502, Infectious Diseases, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti

Abstract

There is a large unmet need for a prophylactic vaccine against human cytomegalovirus (HCMV) to combat the ubiquitous infection that is ongoing with this pathogen. A vaccination against HCMV could protect immunocompromised patients and prevent birth defects caused by congenital HCMV infections. Moreover, cytomegalovirus (CMV) has a number of features that make it a very interesting vector platform for gene therapy. In both cases, preparation of a highly purified virus is a prerequisite for safe and effective application. Murine CMV (MCMV) is by far the most studied model for HCMV infections with regard to the principles that govern the immune surveillance of CMVs. Knowledge transfer from MCMV and mice to HCMV and humans could be facilitated by better understanding and characterization of the biological and biophysical properties of both viruses. We carried out a detailed investigation of HCMV and MCMV growth kinetics as well as stability under the influence of clarification and different storage conditions. Further, we investigated the possibilities to concentrate and purify both viruses by ultracentrifugation and ion-exchange chromatography. Defective enveloped particles were not separately analyzed; however, the behavior of exosomes was examined during all experiments. The effectiveness of procedures was monitored using CCID50 assay, Nanoparticle tracking analysis, ELISA for host cell proteins, and quantitative PCR for host cell DNA. MCMV generally proved to be more robust in handling. Despite its greater sensitivity, HCMV was efficiently (100% recovery) purified and concentrated by anion-exchange chromatography using QA monolithic support. The majority of the host genomic DNA as well as most of the host cell proteins were removed by this procedure.

Published

2021

18. Emerging Mechanisms of G1/S Cell Cycle Control by Human and Mouse Cytomegaloviruses

Author

Boris Bogdanow, Quang Vinh Phan, and Lüder Wiebusch

Subjects

Muromegalovirus, G1 Phase, anaphase-promoting complex, Cytomegalovirus, Cell Cycle Checkpoints, DNA replication, Microbiology, QR1-502, S Phase, Mice, Virology, Cytomegalovirus Infections, Animals, Humans, cell cycle, Minireview, tumor suppressor genes, cyclins

Abstract

Cytomegaloviruses (CMVs) are among the largest pathogenic viruses in mammals. To enable replication of their long double-stranded DNA genomes, CMVs induce profound changes in cell cycle regulation. A hallmark of CMV cell cycle control is the establishment of an unusual cell cycle arrest at the G1/S transition, which is characterized by the coexistence of cell cycle stimulatory and inhibitory activities. While CMVs interfere with cellular DNA synthesis and cell division, they activate S-phase-specific gene expression and nucleotide metabolism. This is facilitated by a set of CMV gene products that target master regulators of G1/S progression such as cyclin E and A kinases, Rb-E2F transcription factors, p53-p21 checkpoint proteins, the APC/C ubiquitin ligase, and the nucleotide hydrolase SAMHD1. While the major themes of cell cycle regulation are well conserved between human and murine CMVs (HCMV and MCMV), there are considerable differences at the level of viral cell cycle effectors and their mechanisms of action. Furthermore, both viruses have evolved unique mechanisms to sense the host cell cycle state and modulate the infection program accordingly. This review provides an overview of conserved and divergent features of G1/S control by MCMV and HCMV.

Published

2021

19. nanoString evaluation of murine Cytomegalovirus transcription in vivo and in vitro

Author

Marion Griessl, Michael Gutknecht, Vanda Juranić-Lisnić, and Charles H. Cook

Subjects

Mice, Mice, Inbred BALB C, Muromegalovirus, Virology, Cytomegalovirus Infections, Animals, Cytomegalovirus, Transcriptome

Abstract

Next Generation Sequencing allows for deep analysis of transcriptional activity in cells and tissues, however it is still a cost intensive method that demands well versed data handling. Reverse transcription quantitative PCR (RT-qPCR) is the most commonly used method to measure gene expression levels, however the information gathered is quite small in comparison to NGS. A newer method called nanoString allows for highly multiplexed gene expression analysis by detecting mRNAs without the use of enzymes for reverse transcription or amplification even for single cells or low input material. The method can be done in 1.5 days and data are quickly analyzed by the accompanied user friendly software. Our aim was to investigate this new method and compare it to the existing alternatives, while investigating murine Cytomegalovirus (mCMV) infection and latency.mCMV infected murine embryonic fibroblasts (MEF), lung and salivary glands from BALB/c mice were evaluated at different stages of infection. A set of 30 custom designed nanoString probes were tested, 20 probes specific for mCMV genes, 6 probes for host genes known to be influenced by viral infection and 4 reference gene specific probes. nanoString counts were compared to published RNA-Seq RPKM.We found that nanoString can be used for analysis of cytomegalovirus gene expression during acute infection in vitro and in vivo, both for virus specific and host genes. Although some transcripts show different expression rates in comparison to NGS data, the most abundant transcripts are comparable. When tissues are infected, there are significantly fewer transcripts than in MEFs, and consistent with previous work there are significant differences in relevant abundance between MEF and tissues. We were unable to detect our viral transcripts of interest in latently infected tissue.For viruses with annotated transcriptomes, nanoString allows simultaneous quantitation of multiple virus and host genes. One huge advantage of the platform is rapid turnaround and simplicity of analysis. It should prove to be very useful to explore host virus interactions during acute infection, but it is unclear if it has adequate sensitivity for analysis during latency in immunocompetent mice.

Published

2021

20. A Live Olfactory Mouse Cytomegalovirus Vaccine, Attenuated for Systemic Spread, Protects against Superinfection

Author

Kimberley Bruce, Helen E. Farrell, and Philip G. Stevenson

Subjects

Human cytomegalovirus, Muromegalovirus, viruses, Immunology, Congenital cytomegalovirus infection, Cytomegalovirus, Biology, Nose, medicine.disease_cause, Vaccines, Attenuated, Microbiology, Proof of Concept Study, Cytomegalovirus Vaccines, Mice, Olfactory Mucosa, Immunity, Virology, Vaccines and Antiviral Agents, medicine, Animals, Mice, Inbred BALB C, Attenuated vaccine, Vaccination, virus diseases, medicine.disease, Immunity, Innate, Immunization, Insect Science, Superinfection, Cytomegalovirus Infections, Female, Cytomegalovirus vaccine, medicine.drug

Abstract

Vaccination against the betaherpesvirus, human cytomegalovirus (HCMV) is a public health goal. However, HCMV has proved difficult to vaccinate against. Vaccination against single HCMV determinants has not worked, suggesting that immunity to a wider antigenic profile may be required. Live attenuated vaccines provide the best prospects for protection, but the question remains as to how to balance vaccine virulence with safety. Animal models of HCMV infection provide insights into identifying targets for virus attenuation and understanding how host immunity blocks natural, mucosal infection. Here, we evaluated the vaccine potential of a mouse cytomegalovirus (MCMV) vaccine deleted of a viral G protein-coupled receptor (GPCR), designated M33, that renders it attenuated for systemic spread. A single noninvasive olfactory ΔM33 MCMV vaccine replicated locally, but as a result of the loss of the M33 GPCR, it failed to spread systemically and was attenuated for latent infection. Vaccination did not prevent host entry of a superinfecting MCMV but spread from the mucosa was blocked. This approach to vaccine design may provide a viable alternative for a safe and effective betaherpesvirus vaccine. IMPORTANCE Human cytomegalovirus (HCMV) is the most common cause of congenital infection for which a vaccine is not yet available. Subunit vaccine candidates have failed to achieve licensure. A live HCMV vaccine may prove more efficacious, but it faces safety hurdles which include its propensity to persist and to establish latency. Understanding how pathogens infect guide rational vaccine design. However, HCMV infections are asymptomatic and thus difficult to capture. Animal models of experimental infection provide insight. Here, we investigated the vaccine potential of a mouse cytomegalovirus (MCMV) attenuated for systemic spread and latency. We used olfactory vaccination and virus challenge to mimic its natural acquisition. We provide proof of concept that a single olfactory MCMV that is deficient in systemic spread can protect against wild-type MCMV superinfection and dissemination. This approach of deleting functional counterpart genes in HCMV may provide safe and effective vaccination against congenital HCMV disease.

Published

2021

21. Species-Specific Inhibition of Necroptosis by HCMV UL36

Author

Wolfram Brune, Renke Brixel, Giada Frascaroli, Claudia Castiglioni, and Elena Muscolino

Subjects

Human cytomegalovirus, Programmed cell death, M45, Muromegalovirus, RIPK1, Necroptosis, viruses, necroptosis, Cytomegalovirus, Apoptosis, Herpesvirus 1, Human, medicine.disease_cause, RIPK3, Microbiology, Herpesviridae, Article, Cell Line, Mice, Necrosis, Viral Proteins, herpesvirus, Species Specificity, Virology, medicine, Animals, HCMV, Molluscum contagiosum virus, biology, biology.organism_classification, medicine.disease, QR1-502, Cell biology, Infectious Diseases, Herpes simplex virus, Host-Pathogen Interactions, UL36, ICP6, MCMV, MLKL

Abstract

Viral infection activates cellular antiviral defenses including programmed cell death (PCD). Many viruses, particularly those of the Herpesviridae family, encode cell death inhibitors that antagonize different forms of PCD. While some viral inhibitors are broadly active in cells of different species, others have species-specific functions, probably reflecting the co-evolution of the herpesviruses with their respective hosts. Human cytomegalovirus (HCMV) protein UL36 is a dual cell death pathway inhibitor. It blocks death receptor-dependent apoptosis by inhibiting caspase-8 activation, and necroptosis by binding to the mixed lineage kinase domain-like (MLKL) protein and inducing its degradation. While UL36 has been shown to inhibit apoptosis in human and murine cells, the specificity of its necroptosis-inhibiting function has not been investigated. Here we show that UL36 interacts with both human and murine MLKL, but has a higher affinity for human MLKL. When expressed by a recombinant mouse cytomegalovirus (MCMV), UL36 caused a modest reduction of murine MLKL levels but did not inhibit necroptosis in murine cells. These data suggest that UL36 inhibits necroptosis, but not apoptosis, in a species-specific manner, similar to ICP6 of herpes simplex virus type 1 and MC159 of molluscum contagiosum virus. Species-specific necroptosis inhibition might contribute to the narrow host range of these viruses.

Published

2021

22. Impact of Dextran-Sodium-Sulfate-Induced Enteritis on Murine Cytomegalovirus Reactivation

Author

Alexandre Jentzer, Sébastien Fauteux-Daniel, Paul Verhoeven, Aymeric Cantais, Melyssa Yaugel Novoa, Fabienne Jospin, Blandine Chanut, Nicolas Rochereau, Thomas Bourlet, Xavier Roblin, Bruno Pozzetto, and Sylvie Pillet

Subjects

Inflammation, Muromegalovirus, Mice, Inbred BALB C, Sulfates, Sodium, Cytomegalovirus, Dextrans, Enteritis, Mice, Disease Models, Animal, Infectious Diseases, Virology, Cytomegalovirus Infections, murine cytomegalovirus, mouse model, viral reactivation, DSS-induced enteritis, Humans, Animals

Abstract

(1) Background: Ulcerative colitis (UC) is an inflammatory bowel disease that causes inflammation of the intestines, which participates in human cytomegalovirus (HCMV) reactivation from its latent reservoir. CMV-associated colitis plays a pejorative role in the clinical course of UC. We took advantage of a model of chemically induced enteritis to study the viral reactivation of murine CMV (MCMV) in the context of gut inflammation. (2) Methods: Seven-week-old BALB/c mice were infected by 3 × 103 plaque-forming units (PFU) of MCMV; 2.5% (w/v) DSS was administered in the drinking water from day (D) 30 to D37 post-infection to induce enteritis. (3) Results: MCMV DNA levels in the circulation decreased from D21 after infection until resolution of the acute infection. DSS administration resulted in weight loss, high disease activity index, elevated Nancy index shortening of the colon length and increase in fecal lipocalin. However, chemically induced enteritis had no impact on MCMV reactivation as determined by qPCR and immunohistochemistry of intestinal tissues. (4) Conclusions: Despite the persistence of MCMV in the digestive tissues after the acute phase of infection, the gut inflammation induced by DSS did not induce MCMV reactivation in intestinal tissues, thus failing to recapitulate inflammation-driven HCMV reactivation in human UC.

Published

2022

23. Tegument Protein pp150 Sequence-Specific Peptide Blocks Cytomegalovirus Infection

Author

John T. Bates, Gene L. Bidwell, Mohammad H. Hasan, Ritesh Tandon, and Dipanwita Mitra

Subjects

Human cytomegalovirus, Muromegalovirus, herpesviruses, peptide therapy, viruses, Congenital cytomegalovirus infection, Cytomegalovirus, Peptide, Microbiology, Virus, Article, Viral Matrix Proteins, Mice, Capsid, Virology, medicine, Animals, Humans, Viability assay, chemistry.chemical_classification, Chemistry, Virus Assembly, Cryoelectron Microscopy, nuclear egress, Virion, CMV, Viral tegument, biochemical phenomena, metabolism, and nutrition, medicine.disease, Phosphoproteins, QR1-502, Cell biology, Infectious Diseases, medicine.anatomical_structure, tegument, Cytomegalovirus Infections, Capsid Proteins, Nucleus

Abstract

Human cytomegalovirus (HCMV) tegument protein pp150 is essential for the completion of the final steps in virion maturation. Earlier studies indicated that three pp150nt (N-terminal one-third of pp150) conformers cluster on each triplex (Tri1, Tri2A and Tri2B), and extend towards small capsid proteins atop nearby major capsid proteins, forming a net-like layer of tegument densities that enmesh and stabilize HCMV capsids. Based on this atomic detail, we designed several peptides targeting pp150nt. Our data show significant reduction in virus growth upon treatment with one of these peptides (pep-CR2) with an IC50 of 1.33 μM and no significant impact on cell viability. Based on 3D modeling, pep-CR2 specifically interferes with the pp150–capsid binding interface. Cells pre-treated with pep-CR2 and infected with HCMV sequester pp150 in the nucleus, indicating a mechanistic disruption of pp150 loading onto capsids and subsequent nuclear egress. Furthermore, pep-CR2 effectively inhibits mouse cytomegalovirus (MCMV) infection in cell culture, paving the way for future animal testing. Combined, these results indicate that CR2 of pp150 is amenable to targeting by a peptide inhibitor, and can be developed into an effective antiviral.

Published

2021

24. Characterization of Murine Cytomegalovirus Infection and Induction of Calcification in Murine Aortic Vascular Smooth Muscle Cells (MOVAS)

Author

Brent A. Stanfield, Cassandra M Bonavita, Timothy M. White, and Rhonda D. Cardin

Subjects

Human cytomegalovirus, Mice, Inbred BALB C, Muromegalovirus, Vascular smooth muscle, viruses, Viral pathogenesis, Myocytes, Smooth Muscle, Congenital cytomegalovirus infection, virus diseases, Cytomegalovirus, Biology, medicine.disease, Virology, Article, Muscle, Smooth, Vascular, Pathogenesis, Mice, In vivo, Cell culture, Cytomegalovirus Infections, medicine, Animals, Humans, Calcification

Abstract

Human cytomegalovirus (HCMV) is a widespread pathogen that causes lifelong latent infection in the majority of the world population. HCMV is associated with increased incidence and severity of many cardiovascular diseases including myocarditis, atherosclerosis, and transplant vasculopathy. Due to the species-restricted nature of cytomegalovirus infection, murine cytomegalovirus (MCMV) is a useful model that recapitulates many of the features of HCMV infection of the cardiovascular system. While in vivo MCMV studies are able to answer many questions regarding pathogenesis of infection, in vitro experiments using cell lines are useful tools to further understand the potential underlying mechanisms. In this study, we characterize MCMV infection of the murine aortic smooth muscle cell line (MOVAS). Our findings demonstrate that MOVAS cells are permissive for MCMV infection, form plaques under carboxymethyl cellulose overlay, and produce progeny virus similar to NIH 3T3 murine embryonic fibroblasts. In addition, MCMV infection induces calcification in MOVAS cells similar to that seen in the epicardium of MCMV-infected hearts. We conclude that MOVAS cells are a useful in vitro tool for studying CMV-mediated cardiac calcification.

Published

2021

25. Multiple Autonomous Cell Death Suppression Strategies Ensure Cytomegalovirus Fitness

Author

Edward S. Mocarski, Heather S Koehler, Emad S. Alnemri, Linda Roback, Pratyusha Mandal, Anita Louise McCormick, Liliana Hernandez, Christopher P. Dillon, Douglas R. Green, and Lynsey N Nagrani

Subjects

Muromegalovirus, M45, BCL2 family, serine protease, TNF, Mice, cmvPCD, DNA virus, Caspase 8, Mice, Inbred BALB C, Cell Death, pyroptosis, extrinsic apoptosis, M41.1, Pyroptosis, apoptosis, QR1-502, Cell biology, mitochondria, vICA, Infectious Diseases, myeloid cells, Tumor necrosis factor alpha, UL36, MCMV, Signal Transduction, replication, Programmed cell death, RIPK1, vIRA, Necroptosis, necroptosis, Biology, IFN, RIPK3, Inhibitor of apoptosis, Microbiology, Article, Viral Proteins, intrinsic apoptosis, M38.5, herpesvirus, Virology, Animals, cytomegalovirus, HCMV, M36, Macrophages, vIBO Caspase-8, Intrinsic apoptosis, Mice, Inbred C57BL, vMIA, inflammation, Apoptosis

Abstract

Programmed cell death pathways eliminate infected cells and regulate infection-associated inflammation during pathogen invasion. Cytomegaloviruses encode several distinct suppressors that block intrinsic apoptosis, extrinsic apoptosis, and necroptosis, pathways that impact pathogenesis of this ubiquitous herpesvirus. Here, we expanded the understanding of three cell autonomous suppression mechanisms on which murine cytomegalovirus relies: (i) M38.5-encoded viral mitochondrial inhibitor of apoptosis (vMIA), a BAX suppressor that functions in concert with M41.1-encoded viral inhibitor of BAK oligomerization (vIBO), (ii) M36-encoded viral inhibitor of caspase-8 activation (vICA), and (iii) M45-encoded viral inhibitor of RIP/RHIM activation (vIRA). Following infection of bone marrow-derived macrophages, the virus initially deflected receptor-interacting protein kinase (RIPK)3-dependent necroptosis, the most potent of the three cell death pathways. This process remained independent of caspase-8, although suppression of this apoptotic protease enhances necroptosis in most cell types. Second, the virus deflected TNF-mediated extrinsic apoptosis, a pathway dependent on autocrine TNF production by macrophages that proceeds independently of mitochondrial death machinery or RIPK3. Third, cytomegalovirus deflected BCL-2 family protein-dependent mitochondrial cell death through combined TNF-dependent and -independent signaling even in the absence of RIPK1, RIPK3, and caspase-8. Furthermore, each of these cell death pathways dictated a distinct pattern of cytokine and chemokine activation. Therefore, cytomegalovirus employs sequential, non-redundant suppression strategies to specifically modulate the timing and execution of necroptosis, extrinsic apoptosis, and intrinsic apoptosis within infected cells to orchestrate virus control and infection-dependent inflammation. Virus-encoded death suppressors together hold control over an intricate network that upends host defense and supports pathogenesis in the intact mammalian host.

Published

2021

26. Transcripts expressed in cytomegalovirus latency coding for an antigenic IE/E phase peptide that drives 'memory inflation'

Author

Niels A. W. Lemmermann, Birgit Kühnapfel, Angélique Renzaho, Julia K Schmiedeke, Christof K. Seckert, and Marion Griessl

Subjects

0301 basic medicine, Microbiology (medical), Muromegalovirus, 030106 microbiology, Immunology, Antigen presentation, CD8-Positive T-Lymphocytes, Major histocompatibility complex, Virus, Epitope, Epitopes, 03 medical and health sciences, MHC class I, Animals, Immunology and Allergy, Cytotoxic T cell, Latency (engineering), Antigens, Viral, Gene, biology, Gene Expression Profiling, General Medicine, Virology, Virus Latency, Disease Models, Animal, 030104 developmental biology, Cytomegalovirus Infections, biology.protein, Immunologic Memory

Abstract

Roizman's definition of herpesviral latency, which applies also to cytomegaloviruses (CMVs), demands maintenance of reactivation-competent viral genomes after clearance of productive infection. It is more recent understanding that failure to complete the productive viral cycle for virus assembly and release does not imply viral gene silencing at all genetic loci and all the time. It rather appears that CMV latency is transcriptionally "noisy" in that silenced viral genes get desilenced from time to time in a stochastic manner, leading to "transcripts expressed in latency" (TELs). If a TEL happens to code for a protein that contains a CD8 T cell epitope, protein processing can lead to the presentation of the antigenic peptide and restimulation of cognate CD8 T cells during latency. This mechanism is discussed as a potential driver of epitope-selective accumulation of CD8 T cells over time, a phenomenon linked to CMV latency and known as "memory inflation" (MI). So far, expression of an epitope-encoding TEL was shown only for the major immediate-early (MIE) gene m123/ie1 of murine cytomegalovirus (mCMV), which codes for the prototypic MI-driving antigenic peptide YPHFMPTNL that is presented by the MHC class-I molecule Ld. The only known second MI-driving antigenic peptide of mCMV in the murine MHC haplotype H-2d is AGPPRYSRI presented by the MHC-I molecule Dd. This peptide is very special in that it is encoded by the early (E) phase gene m164 and by an overlapping immediate-early (IE) transcript governed by a promoter upstream of m164. If MI is driven by presentation of TEL-derived antigenic peptides, as the hypothesis says, one should find corresponding TELs. We show here that E-phase and IE-phase transcripts that code for the MI-driving antigenic peptide AGPPRYSRI are independently and stochastically expressed in latently infected lungs.

Published

2019

27. In vivo proof-of-concept for two experimental antiviral drugs, both directed to cellular targets, using a murine cytomegalovirus model

Author

Manfred Marschall, Regina Müller, Friedrich Hahn, Tobias Bäuerle, Eric Sonntag, Benedikt W. Grau, Lisa Seyler, Benedikt B. Kaufer, Pierre Tannig, Gunther Zischinsky, Luca D. Bertzbach, Svetlana B. Tsogoeva, Eldar Zent, Christina Wangen, Jan Eickhoff, and Matthias Baumann

Subjects

0301 basic medicine, Human cytomegalovirus, Muromegalovirus, 030106 microbiology, Congenital cytomegalovirus infection, Microbial Sensitivity Tests, Pharmacology, Virus Replication, Antiviral Agents, Proof of Concept Study, Mice, 03 medical and health sciences, In vivo, Virology, Animals, Medicine, Potency, Adverse effect, Mice, Knockout, Triazines, business.industry, Drugs, Investigational, medicine.disease, In vitro, Disease Models, Animal, 030104 developmental biology, Drug development, Viral replication, Cytomegalovirus Infections, Pyrazoles, business

Abstract

Infections with the human cytomegalovirus (HCMV) cause serious medical problems including organ rejection and congenital infection. Treatment of HCMV infections with currently available medication targeting viral enzymes is often accompanied with severe side effects and the occurrence of drug-resistant viruses. This demands novel therapeutical approaches like targeting genetically stable host cell proteins that are crucial for virus replication. Although numerous experimental drugs with promising in vitro efficacy have been identified, the lack of available data in animal models limits their potential for further clinical development. Recently, we described the very strong in vitro antiherpesviral activity of the NF-κB inhibitor TF27 and the CDK7 inhibitor LDC4297 at low nanomolar concentrations. In the present study, we present first data for the in vivo efficacy of both experimental drugs using an established cytomegalovirus animal model (murine CMV replication in immunodefective Rag -/- mice). The main findings of this study are (i) a strong inhibitory potency against beta- and gamma-herpesviruses of both compounds in vitro, (ii) even more important, a pronounced anticytomegaloviral activity also exerted in vivo, that resulted from (iii) a restriction of viral replication to the site of infection, thus preventing organ dissemination, (iv) in the absence of major compound-associated adverse events. Thus, we provide evidence for a strong antiviral potency in vivo and proof-of-concept for both drugs, which may encourage their further drug development, possibly including pharmacologically optimized derivatives, for a potential use in future antiherpesviral treatment.

Published

2019

28. Stochastic Episodes of Latent Cytomegalovirus Transcription Drive CD8 T-Cell 'Memory Inflation' and Avoid Immune Evasion

Author

Niels A. W. Lemmermann, Angélique Renzaho, Kirsten Freitag, Matthias J. Reddehase, Marion Griessl, and Christof K. Seckert

Subjects

CD4-Positive T-Lymphocytes, Gene Expression Regulation, Viral, 0301 basic medicine, Muromegalovirus, latent infection, Time Factors, Transcription, Genetic, effector memory CD8+ T cells, Antigen presentation, Immunology, Biology, Virus, Immediate-Early Proteins, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Animals, Cytotoxic T cell, Immunology and Allergy, Latency (engineering), Antigens, Viral, Lung, Gene, memory inflation, latency, Original Research, immune evasion, Mice, Inbred BALB C, Stochastic Processes, Models, Immunological, Herpesviridae Infections, RC581-607, Virology, Virus Latency, Disease Models, Animal, virus reactivation, antigen presentation, Phenotype, 030104 developmental biology, Host-Pathogen Interactions, gene expression, Female, Virus Activation, Immunologic diseases. Allergy, Immunologic Memory, CD8, 030215 immunology

Abstract

Acute infection with murine cytomegalovirus (mCMV) is controlled by CD8+ T cells and develops into a state of latent infection, referred to as latency, which is defined by lifelong maintenance of viral genomes but absence of infectious virus in latently infected cell types. Latency is associated with an increase in numbers of viral epitope-specific CD8+ T cells over time, a phenomenon known as “memory inflation” (MI). The “inflationary” subset of CD8+ T cells has been phenotyped as KLRG1+CD62L- effector-memory T cells (iTEM). It is agreed upon that proliferation of iTEM requires repeated episodes of antigen presentation, which implies that antigen-encoding viral genes must be transcribed during latency. Evidence for this has been provided previously for the genes encoding the MI-driving antigenic peptides IE1-YPHFMPTNL and m164-AGPPRYSRI of mCMV in the H-2d haplotype. There exist two competing hypotheses for explaining MI-driving viral transcription. The “reactivation hypothesis” proposes frequent events of productive virus reactivation from latency. Reactivation involves a coordinated gene expression cascade from immediate-early (IE) to early (E) and late phase (L) transcripts, eventually leading to assembly and release of infectious virus. In contrast, the “stochastic transcription hypothesis” proposes that viral genes become transiently de-silenced in latent viral genomes in a stochastic fashion, not following the canonical IE-E-L temporal cascade of reactivation. The reactivation hypothesis, however, is incompatible with the finding that productive virus reactivation is exceedingly rare in immunocompetent mice and observed only under conditions of compromised immunity. In addition, the reactivation hypothesis fails to explain why immune evasion genes, which are regularly expressed during reactivation in the same cells in which epitope-encoding genes are expressed, do not prevent antigen presentation and thus MI. Here we show that IE, E, and L genes are transcribed during latency, though stochastically, not following the IE-E-L temporal cascade. Importantly, transcripts that encode MI-driving antigenic peptides rarely coincide with those that encode immune evasion proteins. As immune evasion can operate only in cis, that is, in a cell that simultaneously expresses antigenic peptides, the stochastic transcription hypothesis explains why immune evasion is not operative in latently infected cells and, therefore, does not interfere with MI.

Published

2021

29. Hematopoietic cell-mediated dissemination of murine cytomegalovirus is regulated by NK cells and immune evasion

Author

Renee G. Espinosa Trethewy, Shunchuan Zhang, Lindsey M. Bishop, Meaghan H. Hancock, Finn Grey, Lauren E. Springer, Han Zhi Rao, and Christopher M. Snyder

Subjects

Muromegalovirus, Respiratory System, NK cells, CD8-Positive T-Lymphocytes, Virus Replication, Salivary Glands, Epithelium, Mice, White Blood Cells, 0302 clinical medicine, Animal Cells, Medicine and Health Sciences, Cytotoxic T cell, Biology (General), Immunity, Cellular, Mice, Inbred BALB C, 0303 health sciences, T Cells, Herpesviridae Infections, Killer Cells, Natural, Haematopoiesis, medicine.anatomical_structure, Cellular Types, Anatomy, Research Article, QH301-705.5, Immune Cells, T cell, Immunology, Cytotoxic T cells, Bone Marrow Cells, Biology, Major histocompatibility complex, Microbiology, 03 medical and health sciences, Exocrine Glands, Immune system, Mucous Membranes, Immunity, Virology, Genetics, medicine, Animals, Molecular Biology, Immune Evasion, 030304 developmental biology, Blood Cells, Macrophages, Biology and Life Sciences, Cell Biology, RC581-607, Hematopoietic Stem Cells, Viral Replication, Mice, Inbred C57BL, Nasal Mucosa, Biological Tissue, Viral replication, biology.protein, Parasitology, Immunologic diseases. Allergy, Digestive System, CD8, 030215 immunology

Abstract

Cytomegalovirus (CMV) causes clinically important diseases in immune compromised and immune immature individuals. Based largely on work in the mouse model of murine (M)CMV, there is a consensus that myeloid cells are important for disseminating CMV from the site of infection. In theory, such dissemination should expose CMV to cell-mediated immunity and thus necessitate evasion of T cells and NK cells. However, this hypothesis remains untested. We constructed a recombinant MCMV encoding target sites for the hematopoietic specific miRNA miR-142-3p in the essential viral gene IE3. This virus disseminated poorly to the salivary gland following intranasal or footpad infections but not following intraperitoneal infection in C57BL/6 mice, demonstrating that dissemination by hematopoietic cells is essential for specific routes of infection. Remarkably, depletion of NK cells or T cells restored dissemination of this virus in C57BL/6 mice after intranasal infection, while dissemination occurred normally in BALB/c mice, which lack strong NK cell control of MCMV. These data show that cell-mediated immunity is responsible for restricting MCMV to hematopoietic cell-mediated dissemination. Infected hematopoietic cells avoided cell-mediated immunity via three immune evasion genes that modulate class I MHC and NKG2D ligands (m04, m06 and m152). MCMV lacking these 3 genes spread poorly to the salivary gland unless NK cells were depleted, but also failed to replicate persistently in either the nasal mucosa or salivary gland unless CD8+ T cells were depleted. Surprisingly, CD8+ T cells primed after intranasal infection required CD4+ T cell help to expand and become functional. Together, our data suggest that MCMV can use both hematopoietic cell-dependent and -independent means of dissemination after intranasal infection and that cell mediated immune responses restrict dissemination to infected hematopoietic cells, which are protected from NK cells during dissemination by viral immune evasion. In contrast, viral replication within mucosal tissues depends on evasion of T cells., Author summary Cytomegalovirus (CMV) is a common cause of disease in immune compromised individuals as well as a common cause of congenital infections leading to disease in newborns. The virus is thought to enter primarily via mucosal barrier tissues, such as the oral and nasal mucosa. However, it is not clear how the virus escapes these barrier tissues to reach distant sites. In this study, we used a mouse model of CMV infection. Our data illustrate a complex balance between the immune system and viral infection of “myeloid cells”, which are most commonly thought to carry the virus around the body after infection. In particular, our data suggest that robust immune responses at the site of infection force the virus to rely on myeloid cells to escape the site of infection. Moreover, viral genes designed to evade these immune responses were needed to protect the virus during and after its spread to distant sites. Together, this work sheds light on the mechanisms of immune control and viral survival during CMV infection of mucosal tissues and spread to distant sites of the body.

Published

2021

30. Prophylactic and therapeutic HBV vaccination by an HBs-expressing cytomegalovirus vector lacking an interferon antagonist in mice

Author

Shangqing Yang, Ulf Dittmer, Yinping Lu, Dongliang Yang, Xuecheng Yang, Hongming Huang, Mirko Trilling, Mengji Lu, Xuemei Feng, Dan Zhu, Wenqing Zhou, Jia Liu, Meike Rückborn, and Vu Thuy Khanh Le-Trilling

Subjects

0301 basic medicine, Male, HBsAg, Hepatitis B virus, Muromegalovirus, Immunology, Medizin, Biology, CD8-Positive T-Lymphocytes, medicine.disease_cause, Virus Replication, Antiviral Agents, Gene product, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Hepatitis B, Chronic, Interferon, medicine, Immunology and Allergy, Animals, Hepatitis B Vaccines, Vector (molecular biology), Cells, Cultured, Hepatitis B Surface Antigens, Vaccination, virus diseases, STAT2 Transcription Factor, Virology, digestive system diseases, Mice, Inbred C57BL, 030104 developmental biology, Immunization, Liver, Female, Interferons, 030215 immunology, medicine.drug

Abstract

Cytomegalovirus (CMV)-based vaccines show promising effects against chronic infections in nonhuman primates. Therefore, we examined the potential of hepatitis B virus (HBV) vaccines based on mouse CMV (MCMV) vectors expressing the small HBsAg. Immunological consequences of vaccine virus attenuation were addressed by either replacing the dispensable gene m157 ("MCMV-HBsȍ) or the gene M27 ("ΔM27-HBs"), the latter encodes a potent IFN antagonist targeting the transcription factor STAT2. M27 was chosen, since human CMV encodes an analogous gene product, which also induced proteasomal STAT2 degradation by exploiting Cullin RING ubiquitin ligases. Vaccinated mice were challenged with HBV through hydrodynamic injection. MCMV-HBs and ΔM27-HBs vaccination achieved accelerated HBV clearance in serum and liver as well as robust HBV-specific CD8+ T-cell responses. When we explored the therapeutic potential of MCMV-based vaccines, especially the combination of ΔM27-HBs prime and DNA boost vaccination resulted in increased intrahepatic HBs-specific CD8+ T-cell responses and HBV clearance in persistently infected mice. Our results demonstrated that vaccines based on a replication competent MCMV attenuated through the deletion of an IFN antagonist targeting STAT2 elicit robust anti-HBV immune responses and mediate HBV clearance in mice in prophylactic and therapeutic immunization regimes.

Published

2021

31. Inhibition of autophagy by 3-methyladenine restricts murine cytomegalovirus replication

Author

Zhan Zhang, Yuan Yuan Lu, Yidan Bi, Sai-nan Shu, Ting Xi, Lin-Lin Zhang, Xing-lou Liu, Feng Fang, Yuan Huang, and Xinyan Zhang

Subjects

Programmed cell death, Muromegalovirus, Apoptosis, Biology, Virus Replication, 03 medical and health sciences, RIPK1, Mice, 0302 clinical medicine, Virology, medicine, Autophagy, Animals, 030212 general & internal medicine, Fibroblast, Antigens, Viral, Caspase 3, Adenine, Embryo, Chloroquine, Herpesviridae Infections, Molecular biology, Virus Release, Mice, Inbred C57BL, Infectious Diseases, medicine.anatomical_structure, Viral replication, 030211 gastroenterology & hepatology, sense organs

Abstract

Background Cytomegalovirus (CMV) induced autophagy affects virus replication and survival of the infected cells. The purpose of this study was to investigate the role of autophagy inhibition by 3-methyladenine (3-MA) on murine cytomegalovirus (MCMV) replication and whether it is associated with caspase-3 dependent apoptosis. Methods The eyecup isolated from adult C57BL/6J mice (6-8 weeks old) and mouse embryo fibroblast cells (MEFs) were infected with MCMV K181 strain, followed by the treatment of 3-methyladenine (3-MA), chloroquine(CQ) or rapamycin to block or stimulate autophagy. Results In cultured MEFs, the ratio of LC3I/II was reduced at 24 hours post infection (h.p.i.), but was increased at 48h.p.i. In the eyecup culture, LC3I/II ratio was also decreased at 4 and 7days post infection (d.p.i.). In addition, caspase-3 cleavage was increased at 48h.p.i. in MEFs and also elevated in MCMV infected eyecups at 4, 7, 10 and 14d.p.i. 3-MA treatment significantly inhibited the virus replication in MEFs and eyecups. The expression of early antigen (EA) of MCMV was also decreased in MEFs and eyecups. Meanwhile, cleaved caspase-3 dependent cell death was promoted with the presence of 3-MA in MCMV infected MEFs and eyecups, while RIPK1/RIPK3/MLKL pathway was inhibited by 3-MA in eyecups. Conclusions Inhibition of autophagy by 3-MA restricts virus replication and promotes caspase-3 dependent apoptosis in the eyecup and MEFs with MCMV infection. It can be explained that during the early period of MCMV infection, suppressed autophagy process directly reduced virus release, but later caspase-3 dependent apoptosis dominated and resulted in decreased virus replication. This article is protected by copyright. All rights reserved.

Published

2020

32. Screening and validation of differentially expressed microRNAs and target genes in hypertensive mice induced by cytomegalovirus infection

Author

Hua Zhong, Lamei Wang, Yan Tang, Fang He, Xiaoni Zhang, YunZhong Shi, Zhen Huang, Yongmin Liu, Na Tang, and Dongmei Xi

Subjects

0301 basic medicine, Untranslated region, Muromegalovirus, Biophysics, Blood Pressure, 030204 cardiovascular system & hematology, Biology, Biochemistry, Mice, 03 medical and health sciences, 0302 clinical medicine, Virology, Host-Microbe Interactions, microRNA, Animals, Binding site, Receptor, 3' Untranslated Regions, Molecular Biology, Gene, Diagnostics & Biomarkers, Research Articles, miRNA, Reporter gene, Messenger RNA, Binding Sites, essential hypertension, Computational Biology, High-Throughput Nucleotide Sequencing, Herpesviridae Infections, Cell Biology, Receptor, Endothelin A, Molecular biology, Cytomegalovirus infection, Mice, Inbred C57BL, Reverse transcription polymerase chain reaction, Disease Models, Animal, MicroRNAs, 030104 developmental biology, Gene Expression Regulation, Cardiovascular System & Vascular Biology, NIH 3T3 Cells, Signal Transduction

Abstract

Introduction: Multiple studies have suggested an association between cytomegalovirus (CMV) infection and essential hypertension (EH). MicroRNAs (miRNAs) play a critical role in the development of EH by regulating the expression of specific target genes. However, little is known about the role of miRNAs in CMV-induced EH. In the present study, we compared the miRNA expression profiles of samples from normal and murine cytomegalovirus (MCMV)-infected C57BL/6 mice using high-throughput sequencing analysis. Methods: We collected the thoracic aorta, heart tissues, and peripheral blood from 20 normal mice and 20 MCMV-infected mice. We identified differentially expressed miRNAs in the peripheral blood samples and predicted their target genes using bioinformatics tools. We then experimentally validated them using quantitative reverse transcription polymerase chain reaction (qRT-PCR) and the target genes with double luciferase reporter gene assay. Results: We found 118 differentially expressed miRNAs, among which 9 miRNAs were identified as potential MCMV infection-induced hypertension regulators. We then validated the expression of two candidate miRNAs, mmu-miR-1929-3p and mcmv-miR-m01-4-5p, using qRT-PCR. Furthermore, the dual-luciferase reporter gene assay revealed that the 3′-untranslated region (UTR) of endothelin A receptor (Ednra) messenger RNA (mRNA) contained a binding site for mmu-miR-1929-3p. Collectively, our data suggest that MCMV infection can raise the blood pressure and reduce mmu-miR-1929-3p expression in C57BL/6 mice. Moreover, we found that mmu-miR-1929-3p targets the 3′-UTR of the Ednra mRNA. Conclusion: This novel regulatory axis could aid the development of new approaches for the clinical prevention and control of EH.

Published

2020

33. Inconsistent reversal of HIV-1 latency ex vivo by antigens of HIV-1, CMV, and other infectious agents

Author

Thomas Vollbrecht, Bryson Menke, Nikesh M. Kumar, John C. Guatelli, Douglas D. Richman, Michelli F. Oliveira, and Aaron O. Angerstein

Subjects

Adult, CD4-Positive T-Lymphocytes, Male, Muromegalovirus, T cell, HIV Infections, Viremia, Peripheral blood mononuclear cell, Interferon-gamma, 03 medical and health sciences, 0302 clinical medicine, Latent Virus, Antigen, Virology, medicine, Humans, RNA, Messenger, Antigens, Latency (engineering), Aged, 030304 developmental biology, Antigen Presentation, 0303 health sciences, biology, Research, Virion, Dendritic Cells, CD4 T cell, Middle Aged, medicine.disease, Virus Latency, Infectious Diseases, medicine.anatomical_structure, Latency, HIV-1, biology.protein, RNA, Viral, Female, Virus Activation, Antibody, Immunologic Memory, Ex vivo, 030215 immunology

Abstract

Background A reservoir of replication-competent but latent virus is the main obstacle to a cure for HIV-1 infection. Much of this reservoir resides in memory CD4 T cells. We hypothesized that these cells can be reactivated with antigens from HIV-1 and other common pathogens to reverse latency. Results We obtained mononuclear cells from the peripheral blood of antiretroviral-treated patients with suppressed viremia. We tested pools of peptides and proteins derived from HIV-1 and from other pathogens including CMV for their ability to reverse latency ex vivo by activation of memory responses. We assessed activation of the CD4 T cells by measuring the up-regulation of cell-surface CD69. We assessed HIV-1 expression using two assays: a real-time PCR assay for virion-associated viral RNA and a droplet digital PCR assay for cell-associated, multiply spliced viral mRNA. Reversal of latency occurred in a minority of cells from some participants, but no single antigen induced HIV-1 expression ex vivo consistently. When reversal of latency was induced by a specific peptide pool or protein, the extent was proportionally greater than that of T cell activation. Conclusions In this group of patients in whom antiretroviral therapy was started during chronic infection, the latent reservoir does not appear to consistently reside in CD4 T cells of a predominant antigen-specificity. Peptide-antigens reversed HIV-1 latency ex vivo with modest and variable activity. When latency was reversed by specific peptides or proteins, it was proportionally greater than the extent of T cell activation, suggesting partial enrichment of the latent reservoir in cells of specific antigen-reactivity.

Published

2020

34. Repair of an Attenuated Low-Passage Murine Cytomegalovirus Bacterial Artificial Chromosome Identifies a Novel Spliced Gene Essential for Salivary Gland Tropism

Author

Catherine A. Forbes, Lee M. Smith, Laura L. Masters, Baca Chan, Berislav Lisnić, Stipan Jonjić, Alec J. Redwood, Shay Leary, and Vanda Juranić Lisnić

Subjects

sgg1, Human cytomegalovirus, Chromosomes, Artificial, Bacterial, Muromegalovirus, viruses, Immunology, DNA, Recombinant, Genome, Viral, Biology, Tropism, Microbiology, Salivary Glands, Virus, Mice, Open Reading Frames, Viral Proteins, Exon, G4, Virology, medicine, Animals, Humans, Gene, BAC, Mice, Inbred BALB C, Bacterial artificial chromosome, sgg1.1, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, MCMV, tissue tropism, virus diseases, Herpesviridae Infections, medicine.disease, Killer Cells, Natural, Mice, Inbred C57BL, Open reading frame, Insect Science, Mutation, Tissue tropism, Pathogenesis and Immunity, Female, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti

Abstract

The cloning of herpesviruses as bacterial artificial chromosomes (BACs) has revolutionized the study of herpesvirus biology, allowing rapid and precise manipulation of viral genomes. Several clinical strains of human cytomegalovirus (HCMV) have been cloned as BACs; however, no low-passage strains of murine CMV (MCMV), which provide a model mimicking these isolates, have been cloned. Here, the low-passage G4 strain of was BAC cloned. G4 carries an m157 gene that does not ligate the natural killer (NK) cell-activating receptor, Ly49H, meaning that unlike laboratory strains of MCMV, this virus replicates well in C57BL/6 mice. This BAC clone exhibited normal replication during acute infection in the spleen and liver but was attenuated for salivary gland tropism. Next-generation sequencing revealed a C-to-A mutation at nucleotide position 188422, located in the 3′ untranslated region of sgg1, a spliced gene critical for salivary gland tropism. Repair of this mutation restored tropism for the salivary glands. Transcriptional analysis revealed a novel spliced gene within the sgg1 locus. This small open reading frame (ORF), sgg1.1, starts at the 3′ end of the first exon of sgg1 and extends exon 2 of sgg1. This shorter spliced gene is prematurely terminated by the nonsense mutation at nt 188422. Sequence analysis of tissue culture-passaged virus demonstrated that sgg1.1 was stable, although other mutational hot spots were identified. The G4 BAC will allow studies in a broader range of mice, avoiding the strong NK cell responses seen in B6 mice with other MCMV BAC-derived MCMVs. Murine cytomegalovirus (MCMV) is widely used as a model of human CMV (HCMV) infection. However, this model relies on strains of MCMV that have been serially passaged in the laboratory for over four decades. These laboratory strains have been cloned as bacterial artificial chromosomes (BACs), which permits rapid and precise manipulation. Low-passage strains of MCMV add to the utility of the mouse model of HCMV infection but do not exist as cloned BACs. This study describes the first such low-passage MCMV BAC. This BAC-derived G4 was initially attenuated , with subsequent full genomic sequencing revealing a novel spliced transcript required for salivary gland tropism. These data suggest that MCMV, like HCMV, undergoes tissue culture adaptation that can limit growth and supports the use of BAC clones as a way of standardizing viral strains and minimizing interlaboratory strain variation.

Published

2020

35. TNF Signaling Dictates Myeloid and Non-Myeloid Cell Crosstalk to Execute MCMV-Induced Extrinsic Apoptosis

Author

Pratyusha Mandal, A. Louise McCormick, and Edward S. Mocarski

Subjects

0301 basic medicine, Muromegalovirus, Myeloid, TNF, lcsh:QR1-502, lcsh:Microbiology, Mice, 0302 clinical medicine, DNA virus, Myeloid Cells, Mice, Knockout, Caspase 8, pyroptosis, extrinsic apoptosis, Pyroptosis, Intracellular Signaling Peptides and Proteins, apoptosis, Infectious Diseases, medicine.anatomical_structure, vICA, cell death, 030220 oncology & carcinogenesis, Tumor necrosis factor alpha, UL36, Caspase-8, MCMV, Signal Transduction, Programmed cell death, replication, Cell Survival, Necroptosis, necroptosis, Biology, IFN, Article, 03 medical and health sciences, Viral Proteins, intrinsic apoptosis, Virology, medicine, Animals, Humans, Autocrine signalling, cytomegalovirus, HCMV, Innate immune system, M36, Tumor Necrosis Factor-alpha, Macrophages, Intrinsic apoptosis, Endothelial Cells, Dendritic Cells, 030104 developmental biology, inflammation, Cancer research, NIH 3T3 Cells

Abstract

Cytomegaloviruses all encode the viral inhibitor of caspase-8-induced apoptosis (vICA). After binding to this initiator caspase, vICA blocks caspase-8 proteolytic activity and ability to activate caspase-3 and/or caspase-7. In this manner, vICA has long been known to prevent apoptosis triggered via tumor necrosis factor (TNF) family death receptor-dependent extrinsic signaling. Here, we employ fully wild-type murine cytomegalovirus (MCMV) and vICA-deficient MCMV (∆M36) to investigate the contribution of TNF signaling to apoptosis during infection of different cell types. ∆M36 shows the expected ability to kill mouse splenic hematopoietic cells, bone marrow-derived macrophages (BMDM), and dendritic cells (BMDC). Antibody blockade or genetic elimination of TNF protects myeloid cells from death, and caspase-8 activation accompanies cell death. Interferons, necroptosis, and pyroptotic gasdermin D (GSDMD) do not contribute to myeloid cell death. Human and murine fibroblasts or murine endothelial cells (SVEC4-10) normally insensitive to TNF become sensitized to ∆M36-induced apoptosis when treated with TNF or TNF-containing BMDM-conditioned medium. We demonstrate that myeloid cells are the natural source of TNF that triggers apoptosis in either myeloid (autocrine) or non-myeloid cells (paracrine) during ∆M36 infection of mice. Caspase-8 suppression by vICA emerges as key to subverting innate immune elimination of a wide variety of infected cell types.

Published

2020

36. Murine cytomegaloviruses m139 targets DDX3 to curtail interferon production and promote viral replication

Author

Eleonore Ostermann, Christoph Krisp, Giada Frascaroli, Hartmut Schlüter, Melanie M. Brinkmann, Olha Puhach, Wolfram Brune, and HIRI, Helmholtz-Institut für RNA-basierte Infektionsforschung, Josef-Shneider Strasse 2, 97080 Würzburg, Germany.

Subjects

Cytomegalovirus Infection, Human cytomegalovirus, Muromegalovirus, Viral Diseases, Virus Replication, Biochemistry, Epithelium, DEAD-box RNA Helicases, Mice, White Blood Cells, Medical Conditions, Animal Cells, Transcription (biology), Interferon, Gene expression, Medicine and Health Sciences, Biology (General), Cells, Cultured, Mice, Inbred BALB C, 0303 health sciences, 030302 biochemistry & molecular biology, Herpesviridae Infections, RNA Helicase A, Precipitation Techniques, Enzymes, Cell biology, Ubiquitin ligase, Infectious Diseases, medicine.anatomical_structure, Female, Cellular Types, Anatomy, Oxidoreductases, Luciferase, Research Article, medicine.drug, QH301-705.5, Immune Cells, Immunology, DNA construction, Biology, Research and Analysis Methods, Microbiology, Virus, 03 medical and health sciences, Virology, Genetics, medicine, Animals, Immunoprecipitation, Gene family, Molecular Biology, Gene, 030304 developmental biology, Blood Cells, Macrophages, Endothelial Cells, Biology and Life Sciences, Proteins, Epithelial Cells, Interferon-beta, Cell Biology, RC581-607, medicine.disease, Viral Replication, Cell nucleus, Biological Tissue, Molecular biology techniques, Viral replication, Plasmid Construction, Enzymology, biology.protein, Parasitology, Interferons, Immunologic diseases. Allergy

Abstract

Cytomegaloviruses (CMV) infect many different cell types and tissues in their respective hosts. Monocytes and macrophages play an important role in CMV dissemination from the site of infection to target organs. Moreover, macrophages are specialized in pathogen sensing and respond to infection by secreting cytokines and interferons. In murine cytomegalovirus (MCMV), a model for human cytomegalovirus, several genes required for efficient replication in macrophages have been identified, but their specific functions remain poorly understood. Here we show that MCMV m139, a gene of the conserved US22 gene family, encodes a protein that interacts with the DEAD box helicase DDX3, a protein involved in pathogen sensing and interferon (IFN) induction, and the E3 ubiquitin ligase UBR5. DDX3 and UBR5 also participate in the transcription, processing, and translation of a subset of cellular mRNAs. We show that m139 inhibits DDX3-mediated IFN-α and IFN-β induction and is necessary for efficient viral replication in bone-marrow derived macrophages. In vivo, m139 is crucial for viral dissemination to local lymph nodes and to the salivary glands. An m139-deficient MCMV also replicated to lower titers in SVEC4-10 endothelial cells. This replication defect was not accompanied by increased IFN-β transcription, but was rescued by knockout of either DDX3 or UBR5. Moreover, m139 co-localized with DDX3 and UBR5 in viral replication compartments in the cell nucleus. These results suggest that m139 inhibits DDX3-mediated IFN production in macrophages and antagonizes DDX3 and UBR5-dependent functions related to RNA metabolism in endothelial cells., Author summary Human cytomegalovirus is an opportunistic pathogen that causes severe infections in immunocompromised individuals. The virus infects certain cell types, such as macrophages and endothelial cells, to ensure its dissemination within the body. Little is known about the viral factors that promote a productive infection of these cell types. The identification of critical viral factors and the molecular pathways they target can lead to the development of novel antiviral treatment strategies. Using the mouse cytomegalovirus as a model, we studied the viral m139 gene, which is important for virus replication in macrophages and endothelial cells and for dissemination in the mouse. This gene encodes a protein that interacts with the host proteins DDX3 and UBR5. Both proteins are involved in gene expression, and the RNA helicase DDX3 also participates in mounting an innate antiviral response. By interacting with DDX3 and UBR5, m139 ensures efficient viral replication in endothelial cells. Importantly, we identify m139 as a new viral DDX3 inhibitor, which curtails the production of interferon by macrophages.

Published

2020

37. One of the Triple Poly(A) Signals in the M112-113 Gene Is Important and Sufficient for Stabilizing the M112-113 mRNA and the Replication of Murine Cytomegalovirus

Author

Qiyi Tang, Najealicka Armstrong, and Ruth Cruz-Cosme

Subjects

0106 biological sciences, 0301 basic medicine, Gene Expression Regulation, Viral, Muromegalovirus, gene activation, M112-113, TATA box, viruses, RNA Stability, lcsh:QR1-502, IE3, bacterial artificial chromosome (BAC), Biology, Virus Replication, 01 natural sciences, Article, lcsh:Microbiology, Rodent Diseases, 03 medical and health sciences, Mice, Viral Proteins, Plasmid, stomatognathic system, 010608 biotechnology, Virology, Gene expression, Animals, RNA, Messenger, Gene, Regulation of gene expression, poly(A) signal (PAS), Messenger RNA, Bacterial artificial chromosome, virus diseases, Herpesviridae Infections, Cell biology, 030104 developmental biology, Infectious Diseases, Viral replication, cytomegalovirus (CMV), major immediate early (MIE), Poly A

Abstract

The M112-113 gene is the first early gene of the murine cytomegalovirus (MCMV), and its expression is activated by the immediate-early 3 (IE3) protein during MCMV infection in permissive cells. At its 5&prime, terminus, a 10-bp motif, upstream of the TATA box of the M112-113 gene, was identified to bind to IE3, and it is necessary for IE3 to activate M112-113 gene expression (Perez KJ et al. 2013 JVI). At the 3&prime, terminus of the M112-113 gene, three poly(A) signals (PASs) are arranged closely, forming a PAS cluster. We asked whether it is necessary to have the PAS cluster for the M112-113 gene and wondered which PAS is required or important for M112-113 gene expression. In this study, we mutated one, two, or all three PASs in expressing plasmids. Then, we applied bacterial artificial chromosome (BAC) techniques to mutate PASs in viruses. Gene expression and viral replication were analyzed. We found that not all three PASs are needed for M112-113 gene expression. Moreover, we revealed that just one of the three poly(A)s is enough for MCMV replication. However, the deletion of all three PASs did not kill MCMV, although it significantly attenuated viral replication. Finally, an mRNA stability assay was performed and demonstrated that PASs are important to stabilize M112-113 mRNA. Therefore, we conclude that just one of the PASs of the M112-113 gene is sufficient and important for MCMV replication through the stabilization of M112-113 mRNA.

Published

2020

38. Multiple gene targeting siRNAs for down regulation of Immediate Early-2 (Ie2) and DNA polymerase genes mediated inhibition of novel rat Cytomegalovirus (strain All-03)

Author

Ashwaq Ahmed Abdullah, Faez Firdaus Abdullah Jesse, M. L. Mohd-Azmi, Mustapha Mohamed Noordin, Che Azurahanim Che Abdullah, Krishnan Nair Balakrishnan, and Jamilu Abubakar Bala

Subjects

0301 basic medicine, Ganciclovir, Gene Expression Regulation, Viral, Muromegalovirus, DNA polymerase, Down-Regulation, Cytomegalovirus, Replication, DNA-Directed DNA Polymerase, Transfection, Virus Replication, lcsh:Infectious and parasitic diseases, Cell Line, Immediate-Early Proteins, 03 medical and health sciences, Viral Proteins, 0302 clinical medicine, Cytopathogenic Effect, Viral, Virology, Gene expression, medicine, Animals, lcsh:RC109-216, RNA, Small Interfering, Gene, Cytopathic effect, Gene knockdown, biology, Research, Gene targeting, Fibroblasts, Small interfering RNA, Rats, 030104 developmental biology, Infectious Diseases, 030220 oncology & carcinogenesis, Gene Targeting, biology.protein, Combinations, medicine.drug

Abstract

Background Cytomegalovirus (CMV) is an opportunistic pathogen that causes severe complications in congenitally infected newborns and non-immunocompetent individuals. Developing an effective vaccine is a major public health priority and current drugs are fronting resistance and side effects on recipients. In the present study, with the aim of exploring new strategies to counteract CMV replication, several anti-CMV siRNAs targeting IE2 and DNA polymerase gene regions were characterized and used as in combinations for antiviral therapy. Methods The rat embryo fibroblast (REF) cells were transfected with multi siRNA before infecting with CMV strain ALL-03. Viral growth inhibition was measured by tissue culture infectious dose (TCID50), cytopathic effect (CPE) and droplet digital PCR (ddPCR) while IE2 and DNA polymerase gene knockdown was determined by real-time PCR. Ganciclovir was deployed as a control to benchmark the efficacy of antiviral activities of respective individual siRNAs. Results There was no significant cytotoxicity encountered for all the combinations of siRNAs on REF cells analyzed by MTT colorimetric assay (P > 0.05). Cytopathic effects (CPE) in cells infected by RCMV ALL-03 had developed significantly less and at much slower rate compared to control group. The expression of targeted genes was downregulated successfully resulted in significant reduction (P Conclusions In conclusion. The study demonstrated a tremendous promise of innovative approach with the deployment of combined siRNAs targeting at several genes simultaneously with the aim to control CMV replication in host cells.

Published

2020

39. Virus infection is controlled by hematopoietic and stromal cell sensing of murine cytomegalovirus through STING

Author

Wayne M. Yokoyama, Glen N. Barber, Bijal A. Parikh, Liping Yang, Jennifer Poursine-Laurent, and Sytse J. Piersma

Subjects

0301 basic medicine, Muromegalovirus, Cell type, Stromal cell, Mouse, QH301-705.5, Hematopoietic System, viruses, Science, Plasmacytoid dendritic cell, Biology, General Biochemistry, Genetics and Molecular Biology, Virus, 03 medical and health sciences, Immunology and Inflammation, 0302 clinical medicine, Immune system, Interferon, medicine, NK cell, Biology (General), cytomegalovirus, Microbiology and Infectious Disease, General Immunology and Microbiology, General Neuroscience, Membrane Proteins, hemic and immune systems, Herpesviridae Infections, General Medicine, MyD88, Virology, eye diseases, Haematopoiesis, Sting, 030104 developmental biology, Myeloid Differentiation Factor 88, type I interferon, Medicine, Stromal Cells, Research Article, 030215 immunology, medicine.drug, STING

Abstract

Recognition of DNA viruses, such as cytomegaloviruses (CMVs), through pattern-recognition receptor (PRR) pathways involving MyD88 or STING constitute a first-line defense against infections mainly through production of type I interferon (IFN-I). However, the role of these pathways in different tissues is incompletely understood, an issue particularly relevant to the CMVs which have broad tissue tropisms. Herein, we contrasted anti-viral effects of MyD88 versus STING in distinct cell types that are infected with murine CMV (MCMV). Bone marrow chimeras revealed STING-mediated MCMV control in hematological cells, similar to MyD88. However, unlike MyD88, STING also contributed to viral control in non-hematological, stromal cells. Infected splenic stromal cells produced IFN-I in a cGAS-STING-dependent and MyD88-independent manner, while we confirmed plasmacytoid dendritic cell IFN-I had inverse requirements. MCMV-induced natural killer cytotoxicity was dependent on MyD88 and STING. Thus, MyD88 and STING contribute to MCMV control in distinct cell types that initiate downstream immune responses.

Published

2020

40. Murine cytomegalovirus M25 proteins sequester the tumor suppressor protein p53 in nuclear accumulations

Author

Karen Wagner, Matthias Selbach, Martina Dezeljin, Lars Steinbrück, Martin Messerle, Boris Bogdanow, Katarzyna M Szymańska-de Wijs, Lüder Wiebusch, Ivana Kutle, Berislav Cuvalo, Rainer Niedenthal, and Stipan Jonjić

Subjects

p53, Muromegalovirus, Immunoprecipitation, Immunology, Mutant, Microbiology, 03 medical and health sciences, Mice, Viral Proteins, Virology, Gene family, Animals, Humans, Gene, M25 proteins, cytomegalovirus, 030304 developmental biology, Host factor, Cell Nucleus, 0303 health sciences, biology, 030306 microbiology, virus host cell interaction, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, Transfection, Viral tegument, Herpesviridae Infections, HCT116 Cells, Cell biology, Virus-Cell Interactions, HEK293 Cells, Insect Science, biology.protein, Mdm2, Tumor Suppressor Protein p53, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti

Abstract

To ensure productive infection, herpesviruses utilize tegument proteins and nonstructural regulatory proteins to counteract cellular defense mechanisms and to reprogram cellular pathways. The M25 proteins of mouse cytomegalovirus (MCMV) belong to the betaherpesvirus UL25 gene family that encodes viral proteins implicated with regulatory functions. Through affinity purification and mass spectrometric analysis, we discovered the tumor suppressor protein p53 as a host factor interacting with the M25 proteins. M25-p53 interaction in infected and transfected cells was confirmed by coimmunoprecipitation. Moreover, the proteins colocalized in nuclear dot-like structures upon both infection and inducible expression of the two M25 isoforms. p53 accumulated in wild-type MCMV-infected cells, while this did not occur upon infection with a mutant lacking the M25 gene. Both M25 proteins were able to mediate the effect, identifying them as the first CMV proteins responsible for p53 accumulation during infection. Interaction with M25 proteins led to substantial prolongation of the half-life of p53. In contrast to the higher abundance of the p53 protein in wild-type MCMV-infected cells, the transcript levels of the prominent p53 target genes Cdkn1a and Mdm2 were diminished compared to cells infected with the ΔM25 mutant, and this was associated with reduced binding of p53 to responsive elements within the respective promoters. Notably, the productivity of the M25 deletion mutant was partially rescued on p53-negative fibroblasts. We propose that the MCMV M25 proteins sequester p53 molecules in the nucleus of infected cells, reducing their availability for activating a subset of p53-regulated genes, thereby dampening the antiviral role of p53. IMPORTANCE Host cells use a number of factors to defend against viral infection. Viruses are, however, in an arms race with their host cells to overcome these defense mechanisms. The tumor suppressor protein p53 is an important sensor of cell stress induced by oncogenic insults or viral infections, which upon activation induces various pathways to ensure the integrity of cells. Viruses have to counteract many functions of p53, but complex DNA viruses such as cytomegaloviruses may also utilize some p53 functions for their own benefit. In this study, we discovered that the M25 proteins of mouse cytomegalovirus interact with p53 and mediate its accumulation during infection. Interaction with the M25 proteins sequesters p53 molecules in nuclear dot-like structures, limiting their availability for activation of a subset of p53-regulated target genes. Understanding the interaction between viral proteins and p53 may allow to develop new therapeutic strategies against cytomegalovirus and other viruses.

Published

2020

41. Host-Adapted Gene Families Involved in Murine Cytomegalovirus Immune Evasion

Author

Sara Becker, Annette Fink, Jürgen Podlech, Matthias J. Reddehase, and Niels A. Lemmermann

Subjects

Muromegalovirus, CD8 T cells, Review, CD8-Positive T-Lymphocytes, co-evolution, Microbiology, Mice, Viral Proteins, Virology, Animals, Antigens, Viral, cytomegalovirus, memory inflation, adoptive cell transfer, Immune Evasion, latent infection/latency, QR1-502, Killer Cells, Natural, Mice, Inbred C57BL, antiviral protection, Disease Models, Animal, antigen presentation, Infectious Diseases, Cytomegalovirus Infections, Host-Pathogen Interactions, gene family

Abstract

Cytomegaloviruses (CMVs) are host species-specific and have adapted to their respective mammalian hosts during co-evolution. Host-adaptation is reflected by “private genes” that have specialized in mediating virus-host interplay and have no sequence homologs in other CMV species, although biological convergence has led to analogous protein functions. They are mostly organized in gene families evolved by gene duplications and subsequent mutations. The host immune response to infection, both the innate and the adaptive immune response, is a driver of viral evolution, resulting in the acquisition of viral immune evasion proteins encoded by private gene families. As the analysis of the medically relevant human cytomegalovirus by clinical investigation in the infected human host cannot make use of designed virus and host mutagenesis, the mouse model based on murine cytomegalovirus (mCMV) has become a versatile animal model to study basic principles of in vivo virus-host interplay. Focusing on the immune evasion of the adaptive immune response by CD8+ T cells, we review here what is known about proteins of two private gene families of mCMV, the m02 and the m145 families, specifically the role of m04, m06, and m152 in viral antigen presentation during acute and latent infection.

Published

2022

42. Human cytomegalovirus US28 allows dendritic cell exit from lymph nodes

Author

Philip G. Stevenson, Kimberley Bruce, Nicholas Davis-Poynter, Jiawei Ma, and Helen E. Farrell

Subjects

0301 basic medicine, Human cytomegalovirus, Muromegalovirus, Congenital cytomegalovirus infection, Cytomegalovirus, Biology, Viral Proteins, 03 medical and health sciences, Chemokine receptor, Cell Movement, Virology, medicine, Animals, Humans, Receptor, Cells, Cultured, G protein-coupled receptor, Mice, Inbred BALB C, Animal Structures, virus diseases, Dendritic Cells, Dendritic cell, medicine.disease, In vitro, Extravasation, 030104 developmental biology, Cytomegalovirus Infections, Host-Pathogen Interactions, Receptors, Chemokine, Lymph Nodes

Abstract

Human cytomegalovirus (HCMV) colonizes blood-borne dendritic cells (DCs). They express US28, a viral G protein-coupled receptor (GPCR). In vitro functions have been described for US28, but how it contributes to host colonization has been unclear. The murine CMV (MCMV) M33 GPCR promotes DC recirculation. We show that US28 shares this function. Thus, DC recirculation is also available to HCMV via US28, and inhibiting US28 G protein-dependent signalling has the potential to reduce systemic infection. We show that M33 also promotes systemic infection through infected DC extravasation.

Published

2018

43. Mouse Cytomegalovirus m153 Protein Stabilizes Expression of the Inhibitory NKR-P1B Ligand Clr-b

Author

Isabella S Sampaio, David H. Margulies, Bebhinn Treanor, Stipan Jonjić, Astrid Krmpotić, Branka Popović, Oscar A. Aguilar, Mir Munir A. Rahim, Jackeline Samaniego, James R. Carlyle, Mulualem E. Tilahun, Marina Babić, David S.J. Allan, Mithunah Krishnamoorthy, and Andrew P. Makrigiannis

Subjects

Muromegalovirus, Cell, Virus Replication, Mice, Nkrp1-Clr, 0302 clinical medicine, host-pathogen interactions, Receptors, Immunologic, Receptor, Mice, Knockout, 0303 health sciences, biology, Innate lymphoid cell, Herpesviridae Infections, Viral Load, mouse cytomegalovirus, 3. Good health, Cell biology, Killer Cells, Natural, MCMV, m145 family, missing-self recognition, natural killer cell, natural killer cells, viral immune evasion, medicine.anatomical_structure, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti, NK Cell Lectin-Like Receptor Subfamily B, Signal Transduction, Immunology, Microbiology, Natural killer cell, Viral Matrix Proteins, 03 medical and health sciences, Immune system, Downregulation and upregulation, Virology, MHC class I, medicine, Animals, Lectins, C-Type, 030304 developmental biology, Innate immune system, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, Genetic Complementation Test, Immunity, Innate, Mice, Inbred C57BL, Gene Expression Regulation, Insect Science, NIH 3T3 Cells, biology.protein, Pathogenesis and Immunity, 030215 immunology

Abstract

Natural killer (NK) cells are a subset of innate lymphoid cells (ILC) capable of recognizing stressed and infected cells through multiple germ line-encoded receptor-ligand interactions. Missing-self recognition involves NK cell sensing of the loss of host-encoded inhibitory ligands on target cells, including MHC class I (MHC-I) molecules and other MHC-I-independent ligands. Mouse cytomegalovirus (MCMV) infection promotes a rapid host-mediated loss of the inhibitory NKR-P1B ligand Clr-b (encoded by ) on infected cells. Here we provide evidence that an MCMV m145 family member, m153, functions to stabilize cell surface Clr-b during MCMV infection. Ectopic expression of m153 in fibroblasts augments Clr-b cell surface levels. Moreover, infections using -deficient MCMV mutants (Δm144-m158 and Δm153) show an accelerated and exacerbated Clr-b downregulation. Importantly, enhanced loss of Clr-b during Δm153 mutant infection reverts to wild-type levels upon exogenous m153 complementation in fibroblasts. While the effects of m153 on Clr-b levels are independent of transcription, imaging experiments revealed that the m153 and Clr-b proteins only minimally colocalize within the same subcellular compartments, and tagged versions of the proteins were refractory to coimmunoprecipitation under mild-detergent conditions. Surprisingly, the Δm153 mutant possesses enhanced virulence , independent of both Clr-b and NKR-P1B, suggesting that m153 potentially targets additional host factors. Nevertheless, the present data highlight a unique mechanism by which MCMV modulates NK ligand expression. Cytomegaloviruses are betaherpesviruses that in immunocompromised individuals can lead to severe pathologies. These viruses encode various gene products that serve to evade innate immune recognition. NK cells are among the first immune cells that respond to CMV infection and use germ line-encoded NK cell receptors (NKR) to distinguish healthy from virus-infected cells. One such axis that plays a critical role in NK recognition involves the inhibitory NKR-P1B receptor, which engages the host ligand Clr-b, a molecule commonly lost on stressed cells (“missing-self”). In this study, we discovered that mouse CMV utilizes the m153 glycoprotein to circumvent host-mediated Clr-b downregulation, in order to evade NK recognition. These results highlight a novel MCMV-mediated immune evasion strategy.

Published

2019

44. The C-terminal part of the human cytomegalovirus terminase subunit pUL51 is central for terminase complex assembly

Author

Sebastian Neuber, Martin Messerle, Eva Maria Borst, and Karen Wagner

Subjects

Protein Conformation, alpha-Helical, 0301 basic medicine, Human cytomegalovirus, Muromegalovirus, Protein subunit, In silico, Cytomegalovirus, Gene Expression, Sequence alignment, Transfection, Genome, Cell Line, Viral Proteins, 03 medical and health sciences, Virology, medicine, Humans, Protein Interaction Domains and Motifs, Amino Acid Sequence, Peptide sequence, Genetics, Endodeoxyribonucleases, biology, Epithelial Cells, Fibroblasts, biology.organism_classification, medicine.disease, Recombinant Proteins, Intrinsically Disordered Proteins, Protein Subunits, 030104 developmental biology, Mutation, Sequence Alignment, Nuclear localization sequence, HeLa Cells, Plasmids

Abstract

The cleavage and packaging of the human cytomegalovirus (HCMV) genome is accomplished by the viral terminase, comprising pUL56 and pUL89, and the recently identified pUL51 subunit. Since knowledge about pUL51 is scarce, we aimed at identifying pUL51 domains that are important for terminase assembly. In silico analysis suggested that the N-terminal half of pUL51 is intrinsically disordered, and that α-helices are present in the C-terminal part. Linker-scanning mutagenesis of pUL51 in the context of the viral genome revealed that amino acid insertions into the predicted α-helices are not compatible with viral growth, whereas upon mutagenesis of the putatively disordered parts interaction with pUL56 and pUL89 was retained and viral progeny was produced. Replacement of pUL51 with the closely related M51 protein of mouse cytomegalovirus did not lead to viable virus, indicating that M51 cannot substitute for pUL51, and swapping the M51 and UL51 N- and C-termini demonstrated the critical role of the pUL51 C-terminal part in building the terminase complex. Notably, the pUL51 C-terminus alone turned out to be sufficient to enable terminase assembly, its nuclear localization and plaque formation. Using HCMV mutants expressing differently tagged pUL51 versions, we did not detect oligomerization of pUL51, as has been proposed for the pUL51 orthologues of other herpesviruses. These data provide an insight into the interaction of pUL51 with the other two terminase components, and provide the basis for unravelling the mode of action of novel antiviral drugs targeting the HCMV terminase.

Published

2018

45. The Effects of IL10 and NK Cells on the Susceptibility to Mouse Cytomegalovirus in BALB/c Mice despite the Compensation of IFNγ

Author

Xinglou Liu, Sai-nan Shu, Yuanyuan Lu, Yi Liao, Ya-Nan Zhang, Yuan Huang, Feng Fang, and Ting Xi

Subjects

Cytotoxicity, Immunologic, Muromegalovirus, Spleen, Real-Time Polymerase Chain Reaction, Salivary Glands, BALB/c, Flow cytometry, Interferon-gamma, Mice, chemistry.chemical_compound, Immunity, Virology, Lactate dehydrogenase, medicine, Animals, Cytotoxicity, Mice, Inbred BALB C, biology, medicine.diagnostic_test, Herpesviridae Infections, Viral Load, Flow Cytometry, biology.organism_classification, Molecular biology, Killer Cells, Natural, Mice, Inbred C57BL, Interleukin 10, Infectious Diseases, medicine.anatomical_structure, chemistry, Female, Interleukin 18, Disease Susceptibility

Abstract

Objective: The aim of this study was to determine which factors lead to the susceptibility to mouse cytomegalovirus (MCMV) in the spleens of BALB/c mice. Methods: BALB/c and C57BL/6 mice were randomly divided into a control group and an infection group and sacrificed on day 0, 1, 3, 7, 14, and 28 postinfection. The cytotoxicity of NK cells was determined by evaluating lactate dehydrogenase contents. Flow cytometry was used to analyze activated NK cells, IFNγ+ NK cells, and total NK cells in the spleen. The pathological changes of spleens in each group were analyzed by HE staining. The expression of IL10, IL18, IFNγ, Thpok, and IFNβ of spleens was determined by quantitative reverse transcriptase PCR. The viral loads of MCMV in spleens and salivary glands were also detected. Results: We found that spleen NK cells and IL10 in C57BL/6 mice possessed more powerful immunity to MCMV than BALB/c mice. In BALB/c mice, combined effects of the cytotoxicity of NK cells and IFNγ in spleens still ended up with deficient control of infection. Conclusion: The functional shortage of NK cells and inappropriate expression of IL10 result in the susceptibility to MCMV in BALB/c mice.

Published

2018

46. Cytomegalovirus Infection and Inflammation in Developing Brain

Author

Fran Krstanović, Stipan Jonjić, William J. Britt, and Ilija Brizić

Subjects

0301 basic medicine, Human cytomegalovirus, Muromegalovirus, medicine.medical_specialty, Central nervous system, Congenital cytomegalovirus infection, Inflammation, Review, Microbiology, immune response, mouse cytomegalovirus, Mice, CMV tropism, 03 medical and health sciences, 0302 clinical medicine, Immune system, Virology, Animals, Humans, Medicine, cytomegalovirus, latency, Fetus, business.industry, BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences, Brain, virus diseases, central nervous system, medicine.disease, QR1-502, 3. Good health, Cytomegalovirus infection, Disease Models, Animal, Viral Tropism, congenital HCMV infection, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, inflammation, Cytomegalovirus Infections, Immunology, Histopathology, medicine.symptom, BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti, business, 030217 neurology & neurosurgery

Abstract

Human cytomegalovirus (HCMV) is a highly prevalent herpesvirus that can cause severe disease in immunocompromised individuals and immunologically immature fetuses and newborns. Most infected newborns are able to resolve the infection without developing sequelae. However, in severe cases, congenital HCMV infection can result in life-threatening pathologies and permanent damage of organ systems that possess a low regenerative capacity. Despite the severity of the problem, HCMV infection of the central nervous system (CNS) remains inadequately characterized to date. Cytomegaloviruses (CMVs) show strict species specificity, limiting the use of HCMV in experimental animals. Infection following intraperitoneal administration of mouse cytomegalovirus (MCMV) into newborn mice efficiently recapitulates many aspects of congenital HCMV infection in CNS. Upon entering the CNS, CMV targets all resident brain cells, consequently leading to the development of widespread histopathology and inflammation. Effector functions from both resident cells and infiltrating immune cells efficiently resolve acute MCMV infection in the CNS. However, host-mediated inflammatory factors can also mediate the development of immunopathologies during CMV infection of the brain. Here, we provide an overview of the cytomegalovirus infection in the brain, local immune response to infection, and mechanisms leading to CNS sequelae.

Published

2021

47. Determination of suitable reference genes for RT-qPCR analysis of murine Cytomegalovirus in vivo and in vitro

Author

Marion Griessl, Michael Gutknecht, and Charles H. Cook

Subjects

0301 basic medicine, Hypoxanthine Phosphoribosyltransferase, Muromegalovirus, Cell type, 030106 microbiology, Gene Expression, Biology, Real-Time Polymerase Chain Reaction, Article, Mice, 03 medical and health sciences, In vivo, Reference genes, Virology, Gene expression, Animals, Lung, Gene, Mice, Inbred BALB C, Glyceraldehyde-3-Phosphate Dehydrogenases, Herpesviridae Infections, Molecular biology, In vitro, Reverse transcriptase, 030104 developmental biology, Real-time polymerase chain reaction, Liver, NIH 3T3 Cells, Algorithms

Abstract

Reverse transcription quantitative PCR (RT-qPCR) is the most commonly used method to evaluate gene expression. Reliable qPCR results are highly dependent on accurate normalization using suitable reference genes. We investigated expression of commonly used reference genes during murine Cytomegalovirus (mCMV) infection and latency to determine those genes least perturbed by infection. Following mCMV infection in BALB/c mice, lung, salivary gland, liver, spleen and kidney were evaluated. Liver sinusoidal endothelial cells and NIH-3T3 cells were also evaluated. RT-qPCR was performed during acute and latent mCMV infection for 11 commonly used reference genes with comparisons made to uninfected samples. Normfinder, BestKeeper, GeNorm and the comparative delta CT method produced comparable analyses that were combined in RefFinder to generate an overall ranking. Ppia, B2m and Gapdh are the most stable reference genes for in vitro infection studies. For in vivo studies the most suitable reference genes were highly tissue and cell type dependent. Comparing infected and uninfected groups revealed viral influence on transcription of some genes. We provide reference gene guidelines for investigations of gene expression for mCMV Smith strain infection of Balb/cJ mice or NIH-3T3 cells. These results also suggest careful consideration of reference genes for different host tissues evaluated.

Published

2017

48. Tetrahalogenated benzimidazole D-ribonucleosides are active against rat cytomegalovirus

Author

Elke Bogner, Ina Woskobojnik, John C. Drach, Rebekka Adfeldt, Sebastian Voigt, Alexandra Dittmer, and Leroy B. Townsend

Subjects

0301 basic medicine, Muromegalovirus, Benzimidazole, Enzyme complex, Halogenation, Concatemer, 030106 microbiology, Cell Culture Techniques, Viral Plaque Assay, Biology, Cleavage (embryo), Antiviral Agents, Models, Biological, Green fluorescent protein, 03 medical and health sciences, chemistry.chemical_compound, Virology, DNA Packaging, Animals, Pharmacology, Gel electrophoresis, Endodeoxyribonucleases, Tissue Scaffolds, Nucleosides, Herpesviridae Infections, Molecular biology, Rats, Microscopy, Electron, 030104 developmental biology, chemistry, Biochemistry, Cell culture, Benzimidazoles, Collagen, Ribonucleosides, DNA

Abstract

Background Benzimidazole D-ribonucleosides are potent and selective inhibitors of CMV infection that have been shown to target the viral terminase, the enzyme complex responsible for viral DNA cleavage into single unit-length genomes and subsequent DNA packaging into procapsids. Here, we evaluated the viral inhibition by benzimidazole D-ribonucleosides against rat cytomegalovirus (RCMV). Methods Antiviral activity of compounds Cl4RB and BTCRB against RCMV was quantified by measurement of plaque formation. Yield assays and electron microscopy of thin sections was performed using RCMV-infected cells in the presence or absence of the compounds. The effects of Cl4RB and BTCRB on cleavage of concatemers was analyzed by pulsed-field gel electrophoresis. To characterize the behaviour of the antiviral compounds in a more physiological environment, a 3D cell culture model was employed where cells are embedded in an extracellular matrix using rat-tail collagen I. Results Both compounds had an inhibitory effect against RCMV-E. Electron microscopy revealed that only few virions were formed in RCMV-E infected cells in the presence of the compounds. Pulsed-field gel electrophoresis showed that DNA concatemers failed to be processed in the presence of the compounds. Yield Assays showed a comparable viral growth in the 3D vs. 2D cell culture as well as inhibition in the presence of Cl4RB or BTCRB for RCMV-E/GFP. Conclusions These results demonstrate that the tetrahalogenated benzimidazole D-ribonucleosides are effective against RCMV-E by preventing cleavage of concatemeric DNA and nuclear egress of mature capsids.

Published

2017

49. Cytomegalovirus Evades TRAIL-Mediated Innate Lymphoid Cell 1 Defenses

Author

Thomas S. Griffith, Bryan McDonald, Gaelle Picarda, Rachid El Morabiti, Nicolas Thiault, Shilpi Verma, Chris A. Benedict, and Raima Ghosh

Subjects

Muromegalovirus, Cell type, Immunology, Mutant, Cytomegalovirus, Cellular Response to Infection, Biology, Microbiology, Salivary Glands, Immunophenotyping, TNF-Related Apoptosis-Inducing Ligand, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Virology, Animals, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Effector, Innate lymphoid cell, Phenotype, Immunity, Innate, Lymphocyte Subsets, Killer Cells, Natural, Liver, Viral replication, 030220 oncology & carcinogenesis, Insect Science, Cytomegalovirus Infections, Host-Pathogen Interactions, Tumor necrosis factor alpha, Biomarkers

Abstract

Cytomegalovirus (CMV) establishes a lifelong infection facilitated, in part, by circumventing immune defenses mediated by tumor necrosis factor (TNF)-family cytokines. An example of this is the mouse CMV (MCMV) m166 protein, which restricts expression of the TNF-related apoptosis-inducing ligand (TRAIL) death receptors, promoting early-phase replication. We show here that replication of an MCMV mutant lacking m166 is also severely attenuated during viral persistence in the salivary glands (SG). Depleting group I innate lymphoid cells (ILCs) or infecting Trail(−/−) mice completely restored persistent replication of this mutant. Group I ILCs are comprised of two subsets, conventional natural killer cells (cNK) and tissue-resident cells often referred to as innate lymphoid type I cells (ILC1). Using recently identified phenotypic markers to discriminate between these two cell types, their relative expression of TRAIL and gamma interferon (IFN-γ) was assessed during both early and persistent infection. ILC1 were found to be the major TRAIL expressers during both of these infection phases, with cNK expressing very little, indicating that it is ILC1 that curtail replication via TRAIL in the absence of m166-imposed countermeasures. Notably, despite high TRAIL expression by SG-resident ILC1, IFN-γ production by both ILC1 and cNK was minimal at this site of viral persistence. Together these results highlight TRAIL as a key ILC1-utilized effector molecule that can operate in defense against persistent infection at times when other innate control mechanisms may be muted and highlight the importance for the evolution of virus-employed countermeasures. IMPORTANCE Cytomegalovirus (a betaherpesvirus) is a master at manipulating immune responses to promote its lifelong persistence, a result of millions of years of coevolution with its host. Using a one-of-a-kind MCMV mutant unable to restrict expression of the TNF-related apoptosis-inducing ligand death receptors (TRAIL-DR), we show that TRAIL-DR signaling significantly restricts both early and persistent viral replication. Our results also reveal that these defenses are employed by TRAIL-expressing innate lymphoid type I cells (ILC1) but not conventional NK cells. Overall, our results are significant because they show the key importance of viral counterstrategies specifically neutralizing TRAIL effector functions mediated by a specific, tissue-resident subset of group I ILCs.

Published

2019

50. Parthanatos-associated proteins are stimulated intraocularly during development of experimental murine cytomegalovirus retinitis in mice with retrovirus-induced immunosuppression

Author

Richard D. Dix, Jessica Carter, Jay J. Oh, and Judee Grace Nemeño

Subjects

Human cytomegalovirus, Programmed cell death, Muromegalovirus, Poly Adenosine Diphosphate Ribose, Glycoside Hydrolases, Necroptosis, viruses, Congenital cytomegalovirus infection, Poly (ADP-Ribose) Polymerase-1, Retinitis, Biology, Retina, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Murine Acquired Immunodeficiency Syndrome, Virology, medicine, Animals, 030212 general & internal medicine, RNA, Messenger, Parthanatos, Cell Death, Pyroptosis, virus diseases, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Infectious Diseases, Retroviridae, Apoptosis, Cytomegalovirus Retinitis, Disease Progression, 030211 gastroenterology & hepatology, Female, Cytomegalovirus retinitis

Abstract

The mechanisms that contribute to retinal tissue destruction during the onset and progression of AIDS-related human cytomegalovirus (HCMV) retinitis remain unclear. Evidence for the stimulation of multiple cell death pathways including apoptosis, necroptosis, and pyroptosis during the pathogenesis of experimental murine cytomegalovirus (MCMV) retinitis in mice with retrovirus-induced immunosuppression (MAIDS) has been reported. Parthanatos is a caspase-independent cell death pathway mediated by rapid overactivation of poly (ADP-ribose) polymerase-1 (PARP-1) and distinct from other cell death pathways. Using the MAIDS model of MCMV retinitis, studies were performed to test the hypothesis that intraocular MCMV infection of mice with MAIDS stimulates parthanatos-associated messenger RNAs (mRNAs) and proteins within the eye during the development of retinal necrosis that takes place by 10 days after MCMV infection. MCMV-infected eyes of MAIDS mice exhibited significant stimulation of PARP-1 mRNA and proteins at 3 days after infection but declined thereafter at 6 and 10 days after infection. Additional studies showed the intraocular stimulation of mRNAs or proteins before MCMV retinitis development for two additional participants in parthanatos, polymer of ADP-ribose and poly (ADP-ribose) glycohydrolase. These results provide new evidence for a role for parthanatos during MAIDS-related MCMV retinitis that may also extend to AIDS-related HCMV retinitis.

Published

2019