Laboratory Strains of Murine Cytomegalovirus Are Genetically Similar to but Phenotypically Distinct from Wild Strains of Virus

Smith, Lorraine P.; McWhorter, Andrea R.; Masters, Laura; Shellam, Geoffrey; Redwood, Alec

doi:10.1128/jvi.00160-08

Cited by 65 publications

(76 citation statements)

References 37 publications

(34 reference statements)

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“…Murine cytomegalovirus 1 (MCMV), also called Murid herpesvirus 1 (MuHV-1), is a betaherpesvirus of the house mouse and one of its most studied pathogens, because it serves as a laboratory model for human cytomegalovirus (HCMV) infection, which can be highly pathogenic for immunocompromised individuals (1). Almost all laboratory research on MCMV uses either the Smith or the K181 strain of the virus (2). The Smith strain was originally isolated from salivary gland tissue of laboratory mice in the United States in 1954 (3), and the K181 strain was selected by repeated passage of the prototype Smith strain in mouse submaxillary glands (2).…”

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“…Almost all laboratory research on MCMV uses either the Smith or the K181 strain of the virus (2). The Smith strain was originally isolated from salivary gland tissue of laboratory mice in the United States in 1954 (3), and the K181 strain was selected by repeated passage of the prototype Smith strain in mouse submaxillary glands (2). These strains have been serially passaged in vivo and in vitro-in the case of the Smith virus, for more than 50 years.…”

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confidence: 99%

“…Apart from the two standard MCMV laboratory strains, several strains have been isolated from wild house mice in Australia, Beacon Island, and Macquarie Island, and their whole genomes have been sequenced (2,4,5). These strains are genetically different from strains Smith and K181 (4) and show in vivo replication kinetics different from those of the standard strains (5), suggesting that the patterns of host resistance to MCMV described for inbred mice are not applicable to all MCMV strains (2). All of these strains have been isolated either from a single subspecies of mouse, Mus musculus domesticus, or from lab mice, which are derived mostly from M. m. domesticus stocks (6).…”

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Murine Cytomegalovirus Is Not Restricted to the House Mouse Mus musculus domesticus: Prevalence and Genetic Diversity in the European House Mouse Hybrid Zone

Bellocq

Baird

Albrechtová

et al. 2015

J Virol

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Murine cytomegalovirus (MCMV) is a betaherpesvirus of the house mouse, Mus musculus domesticus. It is a common infectious agent of wild mice and a highly studied pathogen of the laboratory mouse. Betaherpesviruses are specific to their hosts, and it is not known if other Mus taxa carry MCMV or if it is restricted to M. m. domesticus. We sampled mice over a 145-km transect of Bavaria-Bohemia crossing a hybrid zone between M. m. domesticus and Mus musculus musculus in order to investigate the occurrence of MCMV in two Mus subspecies and to test the limits of the specificity of the virus for its host. We hypothesized that if the two subspecies carry MCMV and if the virus is highly specific to its host, C ytomegaloviruses (CMVs) are enveloped double-stranded DNA viruses (family Herpesviridae, subfamily Betaherpesvirinae) that have coevolved with their vertebrate hosts. Murine cytomegalovirus 1 (MCMV), also called Murid herpesvirus 1 (MuHV-1), is a betaherpesvirus of the house mouse and one of its most studied pathogens, because it serves as a laboratory model for human cytomegalovirus (HCMV) infection, which can be highly pathogenic for immunocompromised individuals (1). Almost all laboratory research on MCMV uses either the Smith or the K181 strain of the virus (2). The Smith strain was originally isolated from salivary gland tissue of laboratory mice in the United States in 1954 (3), and the K181 strain was selected by repeated passage of the prototype Smith strain in mouse submaxillary glands (2). These strains have been serially passaged in vivo and in vitro-in the case of the Smith virus, for more than 50 years. Apart from the two standard MCMV laboratory strains, several strains have been isolated from wild house mice in Australia, Beacon Island, and Macquarie Island, and their whole genomes have been sequenced (2, 4, 5). These strains are genetically different from strains Smith and K181 (4) and show in vivo replication kinetics different from those of the standard strains (5), suggesting that the patterns of host resistance to MCMV described for inbred mice are not applicable to all MCMV strains (2). All of these strains have been isolated either from a single subspecies of mouse, Mus musculus domesticus, or from lab mice, which are derived mostly from M. m. domesticus stocks (6).Several studies have investigated the occurrence of antibodies

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Murine Cytomegalovirus Is Not Restricted to the House Mouse Mus musculus domesticus: Prevalence and Genetic Diversity in the European House Mouse Hybrid Zone

Bellocq

Baird

Albrechtová

et al. 2015

J Virol

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“…Although no selfligands for activating Ly49H B6 receptors have been reported, inhibitory Ly49C-like receptors bind with high affinity to MHC-I molecules, precluding an easy assessment of additional ligand recognition during infection (15, 32). Further, inoculation of (33). This suggests that in natural settings, m157 is under both selective negative and positive pressures, depending on the NK cell repertoire and H-2 background.…”

Section: Discussionmentioning

confidence: 99%

Viral MHC Class I–like Molecule Allows Evasion of NK Cell Effector Responses In Vivo

Pyzik

Dumaine

Charbonneau

et al. 2014

The Journal of Immunology

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The outcome of mouse CMV (MCMV) infection varies among different inbred mouse strains depending on NK cell effector functions governed through recognition receptor triggering. NK cells from different mouse strains possess diverse repertoires of activating or inhibitory Ly49 receptors, which share some of their polymorphic MHC class I (MHC-I) ligands. By examining the NK cell response to MCMV infection in novel BALB substrains congenic for different MHC (or H-2 in mice) haplotypes, we show that recognition of viral MHC-I–like protein m157 by inhibitory Ly49C receptor allows escape from NK cell control of viral replication. Dominant inhibition by Ly49C bound to self–H-2b encoded MHC-I molecules masks this effect, which only becomes apparent in distinct H-2 haplotypes, such as H-2f. The recognition of m157-expressing cells by Ly49C resulted in both decreased NK cell killing in vitro and reduced rejection in vivo. Further, control of infection with m157-deletant (Δm157) MCMV was improved in mice carrying H-2 molecules unrecognized by Ly49C but allowing expansion of NK cell effectors expressing activating Ly49L receptors. Hence, our study is the first, to our knowledge, to demonstrate that MHC-I mimicry strategies used by MCMV to avoid NK cell control are biologically relevant during in vivo viral infection. Of value for human studies is that only a few genetic assortments conditional on the repertoires of viral MHC-I–like proteins/host NK receptors/MHC haplotypes should allow efficient protection against CMV infection.

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“…By contrast, RCMV-E encoded two orthologues of C-type lectin-like proteins, RCTL and RCTL2 (Ettinger et al, 2012;Voigt et al, 2007), which are absent in MCMV but share 48.8 and 26.8 % amino acid sequence similarity, respectively, with the only C-type lectin-like protein encoded by RCMV-M, the product of the r153 gene (Brocchieri et al, 2005). Twenty RCMV-E ORFs lacked orthologues in other CMVs including isolates from wild mice strains (Smith et al, 2008). The gene products of 2 of English and Berlin RCMV isolates form an ancient clade these 20 putative ORFs displayed high sequence similarity to cellular proteins, thereby implying that they were likely captured from the host.…”

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confidence: 99%

Rat cytomegalovirus (RCMV) English isolate and a newly identified Berlin isolate share similarities with but are separate as an anciently diverged clade from Mouse CMV and the Maastricht isolate of RCMV

Geyer

Ettinger

Møller

et al. 2015

Journal of General Virology

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The genome of the rat cytomegalovirus (RCMV) English isolate (MuHV-8) differs significantly from the RCMV Maastricht isolate (MuHV-2) and other cytomegaloviruses (CMVs) in its size, base composition and genomic content. Analysis of the RCMV-Berlin isolate, MuHV-8, revealed that the two MuHV-8 isolates are highly similar in genome size and content, indicating that the smaller genome size (202 946 bp) compared to other known CMVs was not the result of an accidental deletion during passage in tissue culture. Surprisingly, the proteins encoded in MuHV-8 shared more overall similarity with their orthologues from mouse CMV (MuHV-1) compared to their orthologues in rat CMV (MuHV-2). Phylogenetic analyses of conserved viral genes showed that the two MuHV-8 isolates are from the same species and represent a unique clade that is distinct from other rodent CMVs.

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Laboratory Strains of Murine Cytomegalovirus Are Genetically Similar to but Phenotypically Distinct from Wild Strains of Virus

Cited by 65 publications

References 37 publications

Murine Cytomegalovirus Is Not Restricted to the House Mouse Mus musculus domesticus: Prevalence and Genetic Diversity in the European House Mouse Hybrid Zone

Murine Cytomegalovirus Is Not Restricted to the House Mouse Mus musculus domesticus: Prevalence and Genetic Diversity in the European House Mouse Hybrid Zone

Viral MHC Class I–like Molecule Allows Evasion of NK Cell Effector Responses In Vivo

Rat cytomegalovirus (RCMV) English isolate and a newly identified Berlin isolate share similarities with but are separate as an anciently diverged clade from Mouse CMV and the Maastricht isolate of RCMV

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