Human cytomegalovirus encodes three G protein-coupled receptor homologues

Chee, Mark S.; Satchwell, Sandra C.; Preddie, E.; Weston, Kathleen; Barrell, Bart

doi:10.1038/344774a0

Cited by 260 publications

(172 citation statements)

References 52 publications

Supporting

Mentioning

170

Contrasting

Unclassified

Order By: Relevance

“…Previously, four genes encoding vGPCRs have been identified in the HCMV genome (US27, US28, UL33, and UL78) (4). Although a recent study has suggested that the HCMV genome contains an additional 11 genes that putatively encode proteins possessing 7 transmembrane domains (5), these genes seem to lack other sequences characteristic of the family of GPCR genes.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Constitutive Signaling of the Human Cytomegalovirus-encoded Receptor UL33 Differs from That of Its Rat Cytomegalovirus Homolog R33 by Promiscuous Activation of G Proteins of the Gq, Gi, and Gs Classes

Casarosa¹,

Gruijthuijsen

Michel

et al. 2003

Journal of Biological Chemistry

View full text Add to dashboard Cite

The human cytomegalovirus (HCMV) UL33 gene is conserved among all ␤-herpesviruses and encodes a protein that shows sequence similarity with chemokine receptors belonging to the family of G protein-coupled receptors. Here, we show that HCMV UL33 is predominantly transcribed as a spliced mRNA of which the 5 terminus is localized 55 bp upstream of the start codon. Like its homolog from rat cytomegalovirus (RCMV), R33, UL33 activates multiple signaling pathways in a ligandindependent manner. Although both receptors constitutively activate phospholipase C via G q/11 , and partially via G i/o -mediated pathways, they exhibit profound differences in the modulation of cAMP-responsive element (CRE) activation. R33 constitutively inhibits, whereas UL33 constitutively enhances CRE-mediated transcription. For R33, the inhibition of CRE-driven transcription is entirely G i/o -mediated. For UL33, however, CREmediated transcription is modulated not only through coupling to G␣ i/o but also through coupling to G␣ s. In addition, UL33 was found to enhance CRE activation through the Rho/p38 pathway, via G␤␥. Interestingly, by studying chimeric UL33/R33 proteins, we found the Cterminal cytoplasmic tail of UL33, but not that of R33, to be responsible for the activation of G i/o proteins. A UL33-deficient variant of HCMV was generated to analyze UL33-signaling properties in a physiologically relevant model system. Data obtained with infected cells show that HCMV induces CRE activation, and this effect is, at least in part, dependent on UL33 expression. Taken together, our data indicate that constitutive signaling of UL33 differs from that of R33 by promiscuous activation of G proteins of the G q , G i/o , as well as G s class. Thus, HCMV may effectively use UL33 to orchestrate multiple signaling networks within infected cells.

show abstract

Section: Discussionmentioning

confidence: 99%

“…Within the HCMV genome, four genes encoding GPCRs have previously been identified (US27, US28, UL33, and UL78) (4). Recently, it has been suggested that the HCMV genome may contain additional putative GPCR genes (5).…”

mentioning

confidence: 99%

Constitutive Signaling of the Human Cytomegalovirus-encoded Receptor UL33 Differs from That of Its Rat Cytomegalovirus Homolog R33 by Promiscuous Activation of G Proteins of the Gq, Gi, and Gs Classes

Casarosa¹,

Gruijthuijsen

Michel

et al. 2003

Journal of Biological Chemistry

View full text Add to dashboard Cite

show abstract

“…Sequences encoding functional GPCRs have also been found in the genome of a number of DNA viruses, including human cytomegalovirus (HCMV) (Bankier et al, 1991;Chee et al, 1990), herpes virus saimiri (HVS) (Nicholas et al, 1992) and Kaposi's sarcoma associated herpesvirus (KSHV) (Arvanitakis et al, 1997). The HCMV, which infects leukocytes, ®broblasts and epithelial cells, contains in its genome three predicted open reading frames, UL27, UL28, and UL33, encoding typical GPCRs, which are believed to represent functional chemokine receptors (Ahuja and Murphy, 1993;Neote et al, 1993).…”

Section: Oncogenic Potential Of G Protein-coupled Receptorsmentioning

confidence: 99%

Cell growth control by G protein-coupled receptors: from signal transduction to signal integration

1998

View full text Add to dashboard Cite

“…These genes can be arranged into four groups based on sequence homology, genome location, and function of the respective gene product. One group (the US28 family) consists of two GCR genes: US27 and US28 (23). Both are exclusively present within an unconserved region of the HCMV genome (22).…”

Section: Discussionmentioning

confidence: 99%

“…The KSHV chemokine receptor was also shown to stimulate cellular proliferation (4), transformation, and angiogenesis (7). A distinctive set of chemokine-like receptors is exclusively encoded by betaherpesviruses: HCMV UL33 (23), rat cytomegalovirus (RCMV) R33 (9), murine cytomegalovirus (MCMV) M33 (54), and human herpesvirus 6 and 7 (HHV-6 and -7) U12 (33,49). Recently, we found that the RCMV R33 gene is essential for the pathogenesis of viral infection in vivo and that unlike wild-type (wt) virus, an RCMV R33 null mutant could neither enter nor replicate in salivary gland epithelial cells of infected rats (9).…”

mentioning

confidence: 99%

Deletion of the R78 G protein-coupled receptor gene from rat cytomegalovirus results in an attenuated, syncytium-inducing mutant strain

Vink¹

1999

Journal of Clinical Virology

View full text Add to dashboard Cite

The rat cytomegalovirus (RCMV) R78 gene belongs to an uncharacterized class of viral G protein-coupled receptor (GCR) genes. The predicted amino acid sequence of the R78 open reading frame (ORF) shows 25 and 20% similarity with the gene products of murine cytomegalovirus M78 and human cytomegalovirus UL78, respectively. The R78 gene is transcribed throughout the early and late phases of infection in rat embryo fibroblasts (REF) in vitro. Transcription of R78 was found to result in three different mRNAs: (i) a 1.8-kb mRNA containing the R78 sequence, (ii) a 3.7-kb mRNA containing both R77 and R78 sequences, and (iii) a 5.7-kb mRNA containing at least ORF R77 and ORF R78 sequences. To investigate the function of the R78 gene, we generated two different recombinant virus strains: an RCMV R78 null mutant (RCMV⌬R78a) and an RCMV mutant encoding a GCR from which the putative intracellular C terminus has been deleted (RCMV⌬R78c). These recombinant viruses replicated with a 10-to 100-fold-lower efficiency than wild-type (wt) virus in vitro. Interestingly, unlike wt virus-infected REF, REF infected with the recombinants develop a syncytium-like appearance. A striking difference between wt and recombinant viruses was also seen in vivo: a considerably higher survival was seen among recombinant virus-infected rats than among RCMV-infected rats. We conclude that the RCMV R78 gene encodes a novel GCR-like polypeptide that plays an important role in both RCMV replication in vitro and the pathogenesis of viral infection in vivo.

show abstract

Human cytomegalovirus encodes three G protein-coupled receptor homologues

Cited by 260 publications

References 52 publications

Constitutive Signaling of the Human Cytomegalovirus-encoded Receptor UL33 Differs from That of Its Rat Cytomegalovirus Homolog R33 by Promiscuous Activation of G Proteins of the Gq, Gi, and Gs Classes

Constitutive Signaling of the Human Cytomegalovirus-encoded Receptor UL33 Differs from That of Its Rat Cytomegalovirus Homolog R33 by Promiscuous Activation of G Proteins of the Gq, Gi, and Gs Classes

Cell growth control by G protein-coupled receptors: from signal transduction to signal integration

Deletion of the R78 G protein-coupled receptor gene from rat cytomegalovirus results in an attenuated, syncytium-inducing mutant strain

Contact Info

Product

Resources

About