Your search keyword '"Muromegalovirus physiology"' showing total 13 results

1. Evaluation of Bispecific T-Cell Engagers Targeting Murine Cytomegalovirus.

Author

Menschikowski H, Bednar C, Kübel S, Hermann M, Bauer L, Thomas M, Cordsmeier A, and Ensser A

Subjects

Animals, Mice, Humans, Antibodies, Bispecific pharmacology, Antibodies, Bispecific immunology, Cell Line, Herpesviridae Infections immunology, Herpesviridae Infections virology, Viral Envelope Proteins immunology, Viral Envelope Proteins genetics, Viral Envelope Proteins metabolism, T-Lymphocytes immunology, Muromegalovirus immunology, Muromegalovirus physiology

Abstract

Human cytomegalovirus is a ubiquitous herpesvirus that, while latent in most individuals, poses a great risk to immunocompromised patients. In contrast to directly acting traditional antiviral drugs, such as ganciclovir, we aim to emulate a physiological infection control using T cells. For this, we constructed several bispecific T-cell engager (BiTE) constructs targeting different viral glycoproteins of the murine cytomegalovirus and evaluated them in vitro for their efficacy. To isolate the target specific effect without viral immune evasion, we established stable reporter cell lines expressing the viral target glycoprotein B, and the glycoprotein complexes gN-gM and gH-gL, as well as nano-luciferase (nLuc). First, we evaluated binding capacities using flow cytometry and established killing assays, measuring nLuc-release upon cell lysis. All BiTE constructs proved to be functional mediators for T-cell recruitment and will allow a proof of concept for this treatment option. This might pave the way for strikingly safer immunosuppression in vulnerable patient groups.

Published

2024

2. Mesenchymal Stem Cell-Derived Exosomes Attenuate Murine Cytomegalovirus-Infected Pneumonia via NF-κB/NLRP3 Signaling Pathway.

Author

Chen F, Chen Z, Wu HT, Chen XX, Zhan P, Wei ZY, Ouyang Z, Jiang X, Shen A, Luo MH, Liu Q, Zhou YP, and Qin A

Subjects

Animals, Mice, Mice, Inbred C57BL, Macrophages immunology, Cytomegalovirus Infections therapy, Cytomegalovirus Infections virology, Lung virology, Lung pathology, Pneumonia, Viral therapy, Pneumonia, Viral virology, Herpesviridae Infections therapy, Herpesviridae Infections virology, Herpesviridae Infections immunology, Pneumonia therapy, Pneumonia virology, Exosomes metabolism, Mesenchymal Stem Cells metabolism, NLR Family, Pyrin Domain-Containing 3 Protein metabolism, NF-kappa B metabolism, Signal Transduction, Muromegalovirus physiology, Disease Models, Animal

Abstract

Reactivation and infection with cytomegalovirus (CMV) are frequently observed in recipients of solid organ transplants, bone marrow transplants, and individuals with HIV infection. This presents an increasing risk of allograft rejection, opportunistic infection, graft failure, and patient mortality. Among immunocompromised hosts, interstitial pneumonia is the most critical clinical manifestation of CMV infection. Recent studies have demonstrated the potential therapeutic benefits of exosomes derived from mesenchymal stem cells (MSC-exos) in preclinical models of acute lung injury, including pneumonia, ARDS, and sepsis. However, the role of MSC-exos in the pathogenesis of infectious viral diseases, such as CMV pneumonia, remains unclear. In a mouse model of murine CMV-induced pneumonia, we observed that intravenous administration of mouse MSC (mMSC)-exos reduced lung damage, decreased the hyperinflammatory response, and shifted macrophage polarization from the M1 to the M2 phenotype. Treatment with mMSC-exos also significantly reduced the infiltration of inflammatory cells and pulmonary fibrosis. Furthermore, in vitro studies revealed that mMSC-exos reversed the hyperinflammatory phenotype of bone marrow-derived macrophages infected with murine CMV. Mechanistically, mMSC-exos treatment decreased activation of the NF-κB/NLRP3 signaling pathway both in vivo and in vitro. In summary, our findings indicate that mMSC-exo treatment is effective in severe CMV pneumonia by reducing lung inflammation and fibrosis through the NF-κB/NLRP3 signaling pathway, thus providing promising therapeutic potential for clinical CMV infection.

Published

2024

3. The Viral G-Protein-Coupled Receptor Homologs M33 and US28 Promote Cardiac Dysfunction during Murine Cytomegalovirus Infection.

Author

Bonavita CM, White TM, Francis J, Farrell HE, Davis-Poynter NJ, and Cardin RD

Subjects

Humans, Animals, Mice, Receptors, Chemokine genetics, Viral Proteins metabolism, Cytomegalovirus physiology, Receptors, G-Protein-Coupled genetics, Receptors, G-Protein-Coupled metabolism, Muromegalovirus physiology, Myocarditis, Cytomegalovirus Infections, Heart Diseases

Abstract

Human cytomegalovirus (HCMV) is a ubiquitous pathogen that infects the majority of the world population and causes lifelong latent infection. HCMV has been shown to exacerbate cardiovascular diseases, including myocarditis, vascular sclerosis, and transplant vasculopathy. Recently, we have shown that murine CMV (MCMV) recapitulates the cardiovascular dysfunction observed in patients with HCMV-induced myocarditis. To understand the viral mechanisms involved in CMV-induced heart dysfunction, we further characterized cardiac function in response to MCMV and examined virally encoded G-protein-coupled receptor homologs (vGPCRs) US28 and M33 as potential factors that promote infection in the heart. We hypothesized that the CMV-encoded vGPCRs could exacerbate cardiovascular damage and dysfunction. Three viruses were used to evaluate the role of vGPCRs in cardiac dysfunction: wild-type MCMV, a M33-deficient virus (∆M33), and a virus with the M33 open reading frame (ORF) replaced with US28, an HCMV vGPCR (i.e., US28+). Our in vivo studies revealed that M33 plays a role in promoting cardiac dysfunction by increasing viral load and heart rate during acute infection. During latency, ΔM33-infected mice demonstrated reduced calcification, altered cellular gene expression, and less cardiac hypertrophy compared with wild-type MCMV-infected mice. Ex vivo viral reactivation from hearts was less efficient in ΔM33-infected animals. HCMV protein US28 expression restored the ability of the M33-deficient virus to reactivate from the heart. US28+ MCMV infection caused damage to the heart comparable with wild-type MCMV infection, suggesting that the US28 protein is sufficient to complement the function of M33 in the heart. Altogether, these data suggest a role for vGPCRs in viral pathogenesis in the heart and thus suggest that vGPCRs promote long-term cardiac damage and dysfunction.

Published

2023

4. Transcriptome Analysis of Retinal and Choroidal Pathologies in Aged BALB/c Mice Following Systemic Neonatal Murine Cytomegalovirus Infection.

Author

Zhang X, Xu J, Marshall B, Dong Z, Liu Y, Espinosa-Heidmann DG, and Zhang M

Subjects

Mice, Animals, Mice, Inbred BALB C, Choroid metabolism, Gene Expression Profiling, Eye Infections, Viral metabolism, Eye Infections, Viral pathology, Cytomegalovirus Infections, Muromegalovirus physiology

Abstract

Our previous studies have shown that systemic neonatal murine cytomegalovirus (MCMV) infection of BALB/c mice spread to the eye with subsequent establishment of latency in choroid/RPE. In this study, RNA sequencing (RNA-Seq) analysis was used to determine the molecular genetic changes and pathways affected by ocular MCMV latency. MCMV (50 pfu per mouse) or medium as control were injected intra-peritoneally (i.p.) into BALB/c mice at <3 days after birth. At 18 months post injection, the mice were euthanized, and the eyes were collected and prepared for RNA-Seq. Compared to three uninfected control eyes, we identified 321 differentially expressed genes (DEGs) in six infected eyes. Using the QIAGEN Ingenuity Pathway Analysis (QIAGEN IPA), we identified 17 affected canonical pathways, 10 of which function in neuroretinal signaling, with the majority of DEGs being downregulated, while 7 pathways function in upregulated immune/inflammatory responses. Retinal and epithelial cell death pathways involving both apoptosis and necroptosis were also activated. MCMV ocular latency is associated with upregulation of immune and inflammatory responses and downregulation of multiple neuroretinal signaling pathways. Cell death signaling pathways are also activated and contribute to the degeneration of photoreceptors, RPE, and choroidal capillaries.

Published

2023

5. Species-Specific Inhibition of Necroptosis by HCMV UL36.

Author

Muscolino E, Castiglioni C, Brixel R, Frascaroli G, and Brune W

Subjects

Animals, Apoptosis, Cell Line, Cytomegalovirus genetics, Herpesviridae metabolism, Herpesvirus 1, Human metabolism, Host-Pathogen Interactions, Mice, Molluscum contagiosum virus, Muromegalovirus physiology, Necrosis, Species Specificity, Viral Proteins genetics, Cytomegalovirus physiology, Necroptosis, Viral Proteins metabolism

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

6. Multiple Autonomous Cell Death Suppression Strategies Ensure Cytomegalovirus Fitness.

Author

Mandal P, Nagrani LN, Hernandez L, McCormick AL, Dillon CP, Koehler HS, Roback L, Alnemri ES, Green DR, and Mocarski ES

Subjects

Animals, Caspase 8 genetics, Caspase 8 metabolism, Macrophages virology, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mitochondria metabolism, Viral Proteins metabolism, Cell Death, Muromegalovirus genetics, Muromegalovirus physiology, Signal Transduction

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

7. The Role of Caspase-12 in Retinal Bystander Cell Death and Innate Immune Responses against MCMV Retinitis.

Author

Zhang X, Xu J, Marshall B, Dong Z, Smith SB, and Zhang M

Subjects

Animals, Caspase 12 genetics, Cytomegalovirus Retinitis genetics, Cytomegalovirus Retinitis virology, Female, In Situ Nick-End Labeling methods, Interferons biosynthesis, Male, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Knockout, Retina virology, Retinal Neurons virology, Signal Transduction genetics, Tumor Suppressor Protein p53 metabolism, Virus Replication genetics, Apoptosis genetics, Caspase 12 deficiency, Cytomegalovirus Retinitis enzymology, Immunity, Innate genetics, Muromegalovirus physiology, Retina enzymology, Retinal Neurons enzymology

Abstract

(1) Background: caspase-12 is activated during cytomegalovirus retinitis, although its role is presently unclear. (2) Methods: caspase-12 -/- (KO) or caspase-12 +/+ (WT) mice were immunosup eyes were analyzed by plaque assay, TUNEL assay, immunohistochemical staining, western blotting, and real-time PCR. (3) Results: increased retinitis and a more extensive virus spread were detected in the retina of infected eyes of KO mice compared to WT mice at day 14 p.i. Compared to MCMV injected WT eyes, mRNA levels of interferons α, β and γ were significantly reduced in the neural retina of MCMV-infected KO eyes at day 14 p.i. Although similar numbers of MCMV infected cells, similar virus titers and similar numbers of TUNEL-staining cells were detected in injected eyes of both KO and WT mice at days 7 and 10 p.i., significantly lower amounts of cleaved caspase-3 and p53 protein were detected in infected eyes of KO mice at both time points. (4) Conclusions: caspase-12 contributes to caspase-3-dependent and independent retinal bystander cell death during MCMV retinitis and may also play an important role in innate immunity against virus infection of the retina.

Published

2021

8. CD85k Contributes to Regulatory T Cell Function in Chronic Viral Infections.

Author

Estrada Brull A, Rost F, Oderbolz J, Kirchner FR, Leibundgut-Landmann S, Oxenius A, and Joller N

Subjects

Animals, Antigens, CD immunology, Antigens, CD metabolism, Cell Adhesion Molecules, Neuronal immunology, Cell Adhesion Molecules, Neuronal metabolism, Cell Line, Cells, Cultured, Herpesviridae Infections immunology, Herpesviridae Infections metabolism, Herpesviridae Infections virology, Lymphocytic Choriomeningitis immunology, Lymphocytic Choriomeningitis metabolism, Lymphocytic Choriomeningitis virology, Lymphocytic choriomeningitis virus physiology, Membrane Glycoproteins metabolism, Mice, Inbred C57BL, Muromegalovirus physiology, Receptors, Immunologic metabolism, T-Lymphocytes, Regulatory metabolism, T-Lymphocytes, Regulatory virology, Th1 Cells immunology, Th1 Cells metabolism, Lymphocytic choriomeningitis virus immunology, Membrane Glycoproteins immunology, Muromegalovirus immunology, Receptors, Immunologic immunology, T-Lymphocytes, Regulatory immunology

Abstract

Regulatory T cells (Tregs) prevent excessive immune responses and limit immune pathology upon infections. To fulfill this role in different immune environments elicited by different types of pathogens, Tregs undergo functional specialization into distinct subsets. During acute type 1 immune responses, type 1 Tregs are induced and recruited to the site of ongoing Th1 responses to efficiently control Th1 responses. However, whether a similar specialization process also takes place following chronic infections is still unknown. In this study, we investigated Treg specialization in persistent viral infections using lymphocytic choriomeningitis virus (LCMV) and murine cytomegalovirus (MCMV) infection as models for chronic and latent infections, respectively. We identify CD85k as a Th1-specific co-inhibitory receptor with sustained expression in persistent viral infections and show that recombinant CD85k inhibits LCMV-specific effector T cells. Furthermore, expression of the CD85k ligand ALCAM is induced on LCMV-specific and exhausted T cells during chronic LCMV infection. Finally, we demonstrate that type 1 Tregs arising during chronic LCMV infection suppress Th1 effector cells in an ALCAM-dependent manner. These results extend the current knowledge of Treg specialization from acute to persistent viral infections and reveal an important functional role of CD85k in Treg-mediated suppression of type 1 immunity.

Published

2020

9. 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

Cruz-Cosme R, Armstrong N, and Tang Q

Subjects

Animals, Gene Expression Regulation, Viral, Herpesviridae Infections virology, Mice, Muromegalovirus chemistry, Muromegalovirus physiology, RNA Stability, RNA, Messenger metabolism, Viral Proteins chemistry, Viral Proteins metabolism, Virus Replication, Herpesviridae Infections veterinary, Muromegalovirus genetics, Poly A genetics, RNA, Messenger chemistry, RNA, Messenger genetics, Viral Proteins genetics

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' 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' 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

10. Mouse Cytomegalovirus Differentially Exploits Cell Surface Glycosaminoglycans in a Cell Type-Dependent and MCK-2-Independent Manner.

Author

Pontejo SM and Murphy PM

Subjects

Animals, Cell Line, Chemokines, CC genetics, Fibroblasts virology, Mice, Mice, Inbred BALB C, RAW 264.7 Cells, Viral Proteins genetics, Viral Proteins metabolism, Viral Tropism, Chemokines, CC immunology, Chondroitin Sulfates metabolism, Host Microbial Interactions, Macrophages virology, Muromegalovirus physiology, Viral Proteins immunology, Virus Internalization

Abstract

Many viruses initiate interaction with target cells by binding to cell surface glycosaminoglycans (GAGs). Heparan sulfate (HS) appears to be particularly important in fibroblasts, epithelial cells and endothelial cells, where it represents the dominant GAG. How GAGs influence viral infectivity in HS-poor target cells such as macrophages has not been clearly defined. Here, we show that mouse cytomegalovirus (MCMV) targets HS in susceptible fibroblasts and cultured salivary gland acinar cells (SGACs), but not in macrophage cell lines and primary bone marrow-derived macrophages, where chondroitin sulfate was the dominant virus-binding GAG. MCK-2, an MCMV-encoded GAG-binding chemokine that promotes infection of macrophages as part of a gH/gL/MCK-2 entry complex, was dispensable for MCMV attachment to the cell surface and for direct infection of SGACs. Thus, MCMV tropism for target cells is markedly influenced by differential GAG expression, suggesting that the specificity of anti-GAG peptides now under development as HCMV therapeutics may need to be broadened for effective application as anti-viral agents.

Published

2019

11. Potential Application of TALENs against Murine Cytomegalovirus Latent Infections.

Author

Chen SJ and Chen YC

Subjects

Animals, Cytomegalovirus genetics, Cytomegalovirus Infections genetics, Cytomegalovirus Infections virology, Disease Models, Animal, Herpesviridae Infections genetics, Humans, Mice, Mice, Inbred BALB C, Muromegalovirus genetics, Muromegalovirus growth & development, Transcription Activator-Like Effector Nucleases genetics, Viral Proteins genetics, Viral Proteins metabolism, Virus Replication, Cytomegalovirus physiology, Cytomegalovirus Infections enzymology, Herpesviridae Infections enzymology, Herpesviridae Infections virology, Muromegalovirus physiology, Transcription Activator-Like Effector Nucleases metabolism, Virus Latency

Abstract

Cytomegalovirus (CMV) infections are still a global health problem, because the latent viruses persist in humans and cause recurring disease. Currently, there are no therapies for CMV latent infections and the therapies for active infections are limited by side effects and other problems. It is impossible to eradicate latent viruses in animals. HCMV (human CMV) is specific to human diseases; however, it is difficult to study HCMV due to its host specificity and long life cycle. Fortunately, MCMV (murine CMV) provides an excellent animal model. Here, three specific pairs of transcription activator-like effector nuclease (TALEN) plasmids (MCMV1-2, 3-4, and 5-6) were constructed to target the MCMV M80/80.5 sequence in order to test their efficacy in blocking MCMV lytic replication in NIH3T3 cell culture. The preliminary data showed that TALEN plasmids demonstrate specific targeting and cleavage in the MCMV M80/80.5 sequence and effectively inhibit MCMV growth in cell culture when the plasmid transfection is prior to the viral infection. The most specific pairs of TALEN plasmids (MCMV3-4) were further used to confirm the negative regulation of latent MCMV replication and gene expression in Balb/c mice. The injection of specific TALEN plasmids caused significant inhibition in the copy number level of immediately early gene (ie-1) DNA in five organs of mice, when compared with the controls. The result demonstrated that TALENs potentially provide an effective strategy to remove latent MCMV in animals., Competing Interests: The authors declare no conflict of interest.

Published

2019

12. Increased Viral Dissemination in the Brain and Lethality in MCMV-Infected, Dicer-Deficient Neonates.

Author

Ostermann E, Macquin C, Krezel W, Bahram S, and Georgel P

Subjects

Animals, Animals, Newborn, Disease Models, Animal, Encephalitis pathology, Encephalitis virology, Female, Mice, Inbred BALB C, Mice, Knockout, Survival Analysis, Whole Body Imaging, Brain pathology, Brain virology, Cytomegalovirus Infections pathology, Cytomegalovirus Infections virology, DEAD-box RNA Helicases deficiency, Muromegalovirus physiology, Ribonuclease III deficiency

Abstract

Among Herpesviruses, Human Cytomegalovirus (HCMV or HHV-5) represents a major threat during congenital or neonatal infections, which may lead to encephalitis with serious neurological consequences. However, as opposed to other less prevalent pathogens, the mechanisms and genetic susceptibility factors for CMV encephalitis are poorly understood. This lack of information considerably reduces the prognostic and/or therapeutic possibilities. To easily monitor the effects of genetic defects on brain dissemination following CMV infection we used a recently developed in vivo mouse model based on the neonatal inoculation of a MCMV genetically engineered to express Luciferase. Here, we further validate this protocol for live imaging, and demonstrate increased lethality associated with viral infection and encephalitis in mutant mice lacking Dicer activity. Our data indicate that miRNAs are important players in the control of MCMV pathogenesis and suggest that miRNA-based endothelial functions and integrity are crucial for CMV encephalitis.

Published

2015

13. The p36 isoform of murine cytomegalovirus m152 protein suffices for mediating innate and adaptive immune evasion.

Author

Fink A, Renzaho A, Reddehase MJ, and Lemmermann NA

Subjects

Animals, Cells, Cultured, Glycosylation, Histocompatibility Antigens Class I metabolism, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Nuclear Matrix-Associated Proteins metabolism, Nucleocytoplasmic Transport Proteins metabolism, Protein Binding, Protein Processing, Post-Translational, Immune Evasion, Membrane Glycoproteins immunology, Muromegalovirus immunology, Muromegalovirus physiology, Protein Isoforms immunology, Viral Proteins immunology

Abstract

The MHC-class I (MHC-I)-like viral (MHC-Iv) m152 gene product of murine cytomegalovirus (mCMV) was the first immune evasion molecule described for a member of the β-subfamily of herpesviruses as a paradigm for analogous functions of human cytomegalovirus proteins. Notably, by interacting with classical MHC-I molecules and with MHC-I-like RAE1 family ligands of the activatory natural killer (NK) cell receptor NKG2D, it inhibits presentation of antigenic peptides to CD8 T cells and the NKG2D-dependent activation of NK cells, respectively, thus simultaneously interfering with adaptive and innate immune recognition of infected cells. Although the m152 gene product exists in differentially glycosylated isoforms whose individual contributions to immune evasion are unknown, it has entered the scientific literature as m152/gp40, based on the quantitatively most prominent isoform but with no functional justification. By construction of a recombinant mCMV in which all three N-glycosylation sites are mutated (N61Q, N208Q, and N241Q), we show here that N-linked glycosylation is not essential for functional interaction of the m152 immune evasion protein with either MHC-I or RAE1. These data add an important functional detail to recent structural analysis of the m152/RAE1g complex that has revealed N-glycosylations at positions Asn61 and Asn208 of m152 distant from the m152/RAE1g interface.

Published

2013