ER reorganization and intracellular retention of CD58 are functionally independent properties of the human cytomegalovirus ER resident glycoprotein UL148

Nguyen, Christopher; Aj, Domma; Zhang, H; Kamil, Jeremy P.

doi:10.1101/746438

Cited by 3 publications

(4 citation statements)

References 54 publications

(86 reference statements)

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“…Although intracellular forms of CD58 are, in our hands, refractory to detection by standard indirect immunofluorescence protocols (not shown), it seems reasonable to hypothesize that UL148 sequesters CD58 into the unusual ER structures that it induces. Nonetheless, recent work from our laboratory identified charged-cluster-to-alanine mutants of UL148 that prevent cell surface presentation of CD58 but fail to reorganize the ER (67). Likewise, the chimpanzee CMV homolog of UL148 appears to prevent cell surface presentation of CD58 without reorganizing the ER (67).…”

Section: Discussionmentioning

confidence: 99%

“…Nonetheless, recent work from our laboratory identified charged-cluster-to-alanine mutants of UL148 that prevent cell surface presentation of CD58 but fail to reorganize the ER (67). Likewise, the chimpanzee CMV homolog of UL148 appears to prevent cell surface presentation of CD58 without reorganizing the ER (67). Although we cannot exclude the possibility that ER reorganization may prove crucial for a hitherto unidentified immune evasion function of UL148, these observations argue that ER remodeling is not required for CD58 retention, per se .…”

Section: Discussionmentioning

confidence: 99%

“…This suggests that UL148 plays essential roles during natural infection. Given that ER reorganization appears to be dispensable for CD58 retention (67), it would not be unreasonable to hypothesize that the striking effects of UL148 on the organelle may reflect additional roles of UL148 that contribute to viral persistence in vivo .…”

Section: Discussionmentioning

confidence: 99%

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The Human Cytomegalovirus Nonstructural Glycoprotein UL148 Reorganizes the Endoplasmic Reticulum

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Nguyen

Siddiquey

et al. 2019

mBio

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Perturbations to endoplasmic reticulum (ER) morphology occur during infection with various intracellular pathogens and in certain genetic disorders. We identify that a human cytomegalovirus (HCMV) gene product, UL148, profoundly reorganizes the ER during infection and is sufficient to do so when expressed on its own. Our results reveal that UL148-dependent reorganization of the ER is a prominent feature of HCMV-infected cells. Moreover, we find that this example of virally induced organelle remodeling requires the integrated stress response (ISR), a stress adaptation pathway that contributes to a number of disease states. Since ER reorganization accompanies roles of UL148 in modulation of HCMV cell tropism and in evasion of antiviral immune responses, our results may have implications for understanding the mechanisms involved. Furthermore, our findings provide a basis to utilize UL148 as a tool to investigate organelle responses to stress and to identify novel drugs targeting the ISR.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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The Human Cytomegalovirus Nonstructural Glycoprotein UL148 Reorganizes the Endoplasmic Reticulum

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Nguyen

Siddiquey

et al. 2019

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“…Interestingly, this ER remodeling is enhanced by PERK activation as treatment with ISRIB or a PERK inhibitor delayed the formation of UL148 foci [169]. This remodeling of the ER also appears to be an evolutionary distinct mechanism of human UL140 to control ER reorganization and UPR activation, as the chimpanzee of macaque UL148 do not perform this function [171].…”

Section: Cytomegalovirus (Cmv) and The Uprmentioning

confidence: 99%

Herpesviruses and the Unfolded Protein Response

Johnston

McCormick

2019

Preprint

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Herpesviruses usurp cellular stress responses to avoid immune detection while simultaneously promoting viral replication and spread. The unfolded protein response (UPR) is an evolutionarily conserved stress response that is activated when the protein load in the ER saturates its chaperone folding capacity causing an accrual of misfolded proteins. Through translational and transcriptional reprogramming, the UPR aims to restore protein homeostasis; however, if this fails the cell undergoes apoptosis. It is commonly thought that many enveloped viruses, including herpesviruses, may activate the UPR due to saturation of the ER with nascent glycoproteins and thus these viruses may have evolved mechanisms to evade the potentially negative effects of UPR signaling. Over the past fifteen years there has been considerable effort to provide evidence that different viruses may reprogram the UPR to promote viral replication. Here we provide an overview of the molecular events of UPR activation, signaling and transcriptional outputs, and highlight key findings that demonstrate that the UPR is an important cellular stress response that herpesviruses have hijacked to facilitate persistent infection.

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Endoplasmic Reticulum (ER) Reorganization and Intracellular Retention of CD58 Are Functionally Independent Properties of the Human Cytomegalovirus ER-Resident Glycoprotein UL148

Nguyen

Domma

Kamil

2020

J Virol

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The human cytomegalovirus (HCMV) endoplasmic reticulum (ER)-resident glycoprotein UL148 is posited to play roles in immune evasion and regulation of viral cell tropism. UL148 prevents cell surface presentation of the immune cell costimulatory ligand CD58 while promoting maturation and virion incorporation of glycoprotein O, a receptor binding subunit for an envelope glycoprotein complex involved in entry. Meanwhile, UL148 activates the unfolded protein response (UPR) and causes large-scale reorganization of the ER. In order to determine whether the seemingly disparate effects of UL148 are related or discrete, we generated six charged cluster-to-alanine (CCTA) mutants within the UL148 ectodomain and compared them to wild-type UL148, both in the context of infection studies using recombinant viruses and in ectopic expression experiments, assaying for effects on ER remodeling and CD58 surface presentation. Two mutants, targeting charged clusters spanning residues 79 to 83 (CC3) and 133 to 136 (CC4), retained the potential to impede CD58 surface presentation. Of the six mutants, only CC3 retained the capacity to reorganize the ER, but it showed a partial phenotype. Wild-type UL148 accumulates in a detergent-insoluble form during infection. However, all six CCTA mutants were fully soluble, which implies a relationship between insolubility and organelle remodeling. Additionally, we found that the chimpanzee cytomegalovirus UL148 homolog suppresses surface presentation of CD58 but fails to reorganize the ER, while the homolog from rhesus cytomegalovirus shows neither activity. Collectively, our findings illustrate various degrees of functional divergence between homologous primate cytomegalovirus immunevasins and suggest that the capacity to cause ER reorganization is unique to HCMV UL148. IMPORTANCE In myriad examples, viral gene products cause striking effects on cells, such as activation of stress responses. It can be challenging to decipher how such effects contribute to the biological roles of the proteins. The HCMV glycoprotein UL148 retains CD58 within the ER, thereby preventing it from reaching the cell surface, where it functions to stimulate cell-mediated antiviral responses. Intriguingly, UL148 also triggers the formation of large, ER-derived membranous structures and activates the UPR, a set of signaling pathways involved in adaptation to ER stress. We demonstrate that the potential of UL148 to reorganize the ER and to retain CD58 are separable by mutagenesis and, possibly, by evolution, since chimpanzee cytomegalovirus UL148 retains CD58 but does not remodel the ER. Our findings imply that ER reorganization contributes to other roles of UL148, such as modulation of alternative viral glycoprotein complexes that govern the virus’ ability to infect different cell types.

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ER reorganization and intracellular retention of CD58 are functionally independent properties of the human cytomegalovirus ER resident glycoprotein UL148

Cited by 3 publications

References 54 publications

The Human Cytomegalovirus Nonstructural Glycoprotein UL148 Reorganizes the Endoplasmic Reticulum

The Human Cytomegalovirus Nonstructural Glycoprotein UL148 Reorganizes the Endoplasmic Reticulum

Herpesviruses and the Unfolded Protein Response

Endoplasmic Reticulum (ER) Reorganization and Intracellular Retention of CD58 Are Functionally Independent Properties of the Human Cytomegalovirus ER-Resident Glycoprotein UL148

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