Retroviral Rem protein requires processing by signal peptidase and retrotranslocation for nuclear function

Byun, Hyewon; Halani, Nimita; Mertz, Jennifer A.; Ali, Almas F.; Lozano, Mary M.; Dudley, Jaquelin P.

doi:10.1073/pnas.1004303107

Cited by 36 publications

(126 citation statements)

References 30 publications

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“…Inhibition of proteasomal activity led to preferential accumulation of the Rem precursor relative to the cleaved MMTV-SP product, indicating that full-length Rem is an unstable intermediate (7). Rem activity was partially inhibited by expression of a dominant-negative p97 protein (48), which is consistent with a role for this ATPase in extraction of MMTV-SP from the ER membrane (7).…”

supporting

confidence: 60%

“…Mutation of the signal peptidase cleavage site in either rem or env cDNA was shown to prevent Rem cleavage and activity in an assay based on a reporter plasmid derived from the 3= end of the MMTV genome (7,31). In addition, green fluorescent protein (GFP)-tagged Rem with mutations in the signal peptidase cleavage site were unstable and exhibited very low level fluorescence compared to wild-type GFPtagged Rem (7), which is consistent with misfolding and targeting to the proteasome. Removal of the NLS also prevents Rem activity (31), indicating that MMTV-SP must function in the nucleus.…”

mentioning

confidence: 84%

“…Expression vectors for RemGFP, GFPRem, untagged Rem, and their L71P mutants have been previously described (7,31). The signal peptidase cleavage site (GFP-V96RG98R) and glycosylation site (GFP-N127QN143Q) mutants have also been previously reported (7).…”

Section: Methodsmentioning

confidence: 99%

“…Our recent experiments revealed that MMTV-SP is generated from either the Rem or the Env proteins by signal peptidase cleavage in the endoplasmic reticulum (ER) (7). Mutation of the signal peptidase cleavage site in either rem or env cDNA was shown to prevent Rem cleavage and activity in an assay based on a reporter plasmid derived from the 3= end of the MMTV genome (7,31).…”

mentioning

confidence: 99%

“…Removal of the NLS also prevents Rem activity (31), indicating that MMTV-SP must function in the nucleus. Thus, MMTV-SP has a unique trafficking pattern in virally infected cells involving retrotranslocation from the ER lumen prior to nuclear function (7,13).…”

mentioning

confidence: 99%

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supporting

confidence: 60%

mentioning

confidence: 84%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Requirements for Mouse Mammary Tumor Virus Rem Signal Peptide Processing and Function

Byun

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et al. 2012

J Virol

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Retroviral Replication

Pedersen

Pyrz

Duch

2011

Encyclopedia of Life Sciences

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Retroviruses are enveloped animal ribonucleic acid (RNA) viruses that replicate via a deoxyribonucleic acid (DNA) intermediate, which is integrated into the host genome as a provirus. Interaction of the viral envelope protein with a target cell receptor triggers entry of the viral nucleoprotein core by fusion of viral and cellular membranes. After entry, the viral enzymes reverse transcriptase and integrase mediate reverse transcription of viral RNA and integration of the resulting double‐stranded DNA copy of the viral genome, respectively. Expression of viral RNA and proteins from proviral DNA utilises the transcription and translation machinery of the host. Retrovirus particles are assembled through protein–protein and protein–lipid interactions, released from the cell by budding, and subsequently matured by a viral protease . A provirus can be transmitted through the germline from parents to offspring as an endogenous retrovirus. Host cell restriction factors target multiple steps of retroviral replication in a complex interplay of virus–host interactions. Key Concepts: Reverse transcription and integration into the host genome are hallmarks of retroviral replication. The viral RNA genome contains a packaging signal for selective encapsidation into viral particles and a binding site for a tRNA primer for initiation of reverse transcription. The integrated virus contains long‐terminal repeats harbouring signals for transciptional initiation and polyadenylation, which define the retroviral transcription unit. Open reading frames for Gag, Pol and Env are found in all retroviruses, but some retroviruses encode additional proteins such as Tat and Rev of HIV‐1. A stop‐codon between gag and pol can be bypassed by read‐through or frame‐shifting during translation of retroviral mRNA to make the Gag–Pol polyprotein. Retroviruses have specialised strategies for export of unspliced genomic‐length viral RNA from the nucleus. The metastable retroviral envelope protein drives the fusion of viral and cellular membranes by a type I fusion mechanism to allow retroviral entry in a receptor‐dependent manner. The retroviral protease is required for maturation of viral particles after their release from producer cells by budding. A retrovirus can integrate into the genome of germ cells and become part of the genetic material transmitted from parents to offspring. A provirus can be maintained through species diversification as an endogenous retrovirus that may serve as a marker of phylogenetic relationship and evolutionary distance.

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Retroviral Replication

Pedersen

Mikkelsen

2021

Encyclopedia of Life Sciences

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Retroviruses, are enveloped animal ribonucleic acid (RNA) viruses that replicate via a deoxyribonucleic acid (DNA) intermediate, which is integrated into the host genome as a provirus. Expression of viral RNA and proteins from proviral DNA utilises the transcription and translation machinery of the host. Retrovirus particles are assembled through protein–protein, protein–RNA and protein–lipid interactions, released from the cell by budding and subsequently matured by a viral protease. Interaction of the viral envelope protein with a target cell receptor triggers entry of the viral nucleoprotein core by fusion of viral and cellular membranes. After entry, the viral enzymes reverse transcriptase and integrase mediate reverse transcription of viral RNA and integration of the resulting double‐stranded DNA copy of the viral genome, respectively. A provirus can be transmitted through the germ line from parents to offspring as an endogenous retrovirus. Multiple steps of retroviral replication can be targeted by host cell restriction factors in a complex interplay of virus–host interactions. Key Concepts Reverse transcription and integration into the host genome are hallmarks of retroviral replication. The viral RNA genome contains a packaging signal for selective encapsidation into viral particles and a binding site for a tRNA primer for initiation of reverse transcription. The integrated virus contains long‐terminal repeats harbouring signals for transcriptional initiation and polyadenylation, which define the retroviral transcription unit. Open reading frames for Gag, Pol and Env are found in all retroviruses, but some retroviruses encode additional proteins such as Tat and Rev of HIV‐1. A stop codon between gag and pol can be bypassed by readthrough or frameshifting during translation of retroviral mRNA to make the Gag–Pol polyprotein. Retroviruses have specialised strategies for export of unspliced genomic‐length viral RNA from the nucleus. The metastable retroviral envelope protein drives the fusion of viral and cellular membranes by a type I fusion mechanism to allow retroviral entry in a receptor‐dependent manner. The retroviral protease is required for maturation of viral particles after their release from producer cells by budding. A retrovirus can integrate into the genome of germ cells and become part of the genetic material transmitted from parents to offspring. A provirus can be maintained through species diversification as an endogenous retrovirus that may serve as a marker of phylogenetic relationship and evolutionary distance. A battery of diverse host cell restriction factors operates at multiple steps of retroviral replication.

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Retroviral Rem protein requires processing by signal peptidase and retrotranslocation for nuclear function

Cited by 36 publications

References 30 publications

Requirements for Mouse Mammary Tumor Virus Rem Signal Peptide Processing and Function

Requirements for Mouse Mammary Tumor Virus Rem Signal Peptide Processing and Function

Retroviral Replication

Retroviral Replication

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