2016
DOI: 10.1128/jvi.01547-16
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Long and Short Isoforms of the Human Cytomegalovirus UL138 Protein Silence IE Transcription and Promote Latency

Abstract: The UL133-138 locus present in clinical strains of human cytomegalovirus (HCMV) encodes proteins required for latency and reactivation in CD34؉ hematopoietic progenitor cells and virion maturation in endothelial cells. The encoded proteins form multiple homo-and hetero-interactions and localize within secretory membranes. One of these genes, UL136 gene, is expressed as at least five different protein isoforms with overlapping and unique functions. Here we show that another gene from this locus, the UL138 gene,… Show more

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Cited by 33 publications
(47 citation statements)
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“…The opposing regulation of EGFR by UL135 and UL138 may alter the cellular state, and, in turn, impact programs of viral gene expression contributing to virus-mediated control of latency and reactivation. Consistent with this notion, UL138 has also been shown to impede demethylation of histones associated with the viral genome required for expression of IE genes [97], suggesting that UL138 regulates signaling cascades which will ultimately impact the chromatin state of the viral genome. Therefore, control over a homeostatic regulator like EGFR may effectively allow the virus to hardwire itself into the host cell to sense and respond to changes in the state of the cell.…”
Section: Discussionmentioning
confidence: 92%
“…The opposing regulation of EGFR by UL135 and UL138 may alter the cellular state, and, in turn, impact programs of viral gene expression contributing to virus-mediated control of latency and reactivation. Consistent with this notion, UL138 has also been shown to impede demethylation of histones associated with the viral genome required for expression of IE genes [97], suggesting that UL138 regulates signaling cascades which will ultimately impact the chromatin state of the viral genome. Therefore, control over a homeostatic regulator like EGFR may effectively allow the virus to hardwire itself into the host cell to sense and respond to changes in the state of the cell.…”
Section: Discussionmentioning
confidence: 92%
“…The putative amino-terminal transmembrane sequences of UL138 are largely absent in a naturally occurring isomer that initiates translation from the internal methionine-16 codon (29), expressing an N-terminally truncated short isoform. It is not known which isoform, i.e., the (full-length) long isoform or the short isoform, is more important during clinical infection.…”
mentioning
confidence: 99%
“…It is not known which isoform, i.e., the (full-length) long isoform or the short isoform, is more important during clinical infection. In vitro, the long isoform (expressed from methionine-1) is the major species; however, the short isoform is expressed and appears to play a role in the establishment and maintenance of latency (29). Latency establishment and maintenance in vitro are most efficient when the two isoforms of UL138 are naturally simultaneously expressed from the wild-type (WT) gene (29).…”
mentioning
confidence: 99%
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