The G-Patch Domain of Mason-Pfizer Monkey Virus Is a Part of Reverse Transcriptase

Křížová, Ivana; Hadravová, Romana; Štokrová, Jitka; Günterová, Jana; Doležal, Michal; Ruml, Tomáš; Rumlová, Michaela; Pichová, Iva

doi:10.1128/jvi.06638-11

Cited by 22 publications

(25 citation statements)

References 31 publications

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“…The 201 RKK 203 to AAA or GPG mutations in pSIT ⌬ProCANC M-PMV were made by SLIM mutagenesis (35). To introduce mutations in the M-PMV proviral vector pSARM4 (36), we first used a helper vector (MHelppUC19) encoding M-PMV SacI-Eco72I fragment, which was prepared as described previously (37,38). Mutations RKK/AAA and RKK/GPG were created by two-step PCR mutagenesis using primers carrying appropriate mutations and suitable NotI and XmaI restriction sites, respectively.…”

Section: Methodsmentioning

confidence: 99%

“…Infectivity of M-PMV wt and CA-CTD mutants was determined as described earlier (37,46). Briefly, HEK 293T cells were cotransfected with either wt or RKK/AAA mutant pSARM-EGFP expression vector, together with the glycoprotein expression vector pTMO.…”

Section: Methodsmentioning

confidence: 99%

“…Briefly, HEK 293T cells were cotransfected with either wt or RKK/AAA mutant pSARM-EGFP expression vector, together with the glycoprotein expression vector pTMO. At 48 h posttransfection, the culture supernatants were collected and filtered through a 0.45-m-pore-size filter, and each sample was normalized for capsid protein content by quantitative Western blotting (37). The volume of culture supernatant used to infect HEK 293T cells was adjusted to 4 ml with complete DMEM, and the cells were incubated for an additional 48 h. The cells were fixed with 4% formaldehyde, and the number of GFP-positive cells was determined using flow cytometry (BD FACSAria).…”

Section: Methodsmentioning

confidence: 99%

“…Reverse transcription-PCR (RT-PCR) was performed as described previously (37). Briefly, the HEK 293T cells were transfected with wt or RKK/AAA mutant proviral construct.…”

Section: Methodsmentioning

confidence: 99%

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Nucleic Acid Binding by Mason-Pfizer Monkey Virus CA Promotes Virus Assembly and Genome Packaging

Füzik

Píchalová

Schur

et al. 2016

J Virol

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The Gag polyprotein of retroviruses drives immature virus assembly by forming hexameric protein lattices. The assembly is primarily mediated by protein-protein interactions between capsid (CA) domains and by interactions between nucleocapsid (NC) domains and RNA. Specific interactions between NC and the viral RNA are required for genome packaging. Previously reported cryoelectron microscopy analysis of immature Mason-Pfizer monkey virus (M-PMV) particles suggested that a basic region (residues RKK) in CA may serve as an additional binding site for nucleic acids. Here, we have introduced mutations into the RKK region in both bacterial and proviral M-PMV vectors and have assessed their impact on M-PMV assembly, structure, RNA binding, budding/release, nuclear trafficking, and infectivity using in vitro and in vivo systems. Our data indicate that the RKK region binds and structures nucleic acid that serves to promote virus particle assembly in the cytoplasm. Moreover, the RKK region appears to be important for recruitment of viral genomic RNA into Gag particles, and this function could be linked to changes in nuclear trafficking. Together these observations suggest that in M-PMV, direct interactions between CA and nucleic acid play important functions in the late stages of the viral life cycle. IMPORTANCEAssembly of retrovirus particles is driven by the Gag polyprotein, which can self-assemble to form virus particles and interact with RNA to recruit the viral genome into the particles. Generally, the capsid domains of Gag contribute to essential proteinprotein interactions during assembly, while the nucleocapsid domain interacts with RNA. The interactions between the nucleocapsid domain and RNA are important both for identifying the genome and for self-assembly of Gag molecules. Here, we show that a region of basic residues in the capsid protein of the betaretrovirus Mason-Pfizer monkey virus (M-PMV) contributes to interaction of Gag with nucleic acid. This interaction appears to provide a critical scaffolding function that promotes assembly of virus particles in the cytoplasm. It is also crucial for packaging the viral genome and thus for infectivity. These data indicate that, surprisingly, interactions between the capsid domain and RNA play an important role in the assembly of M-PMV. The retroviral structural polyprotein Gag contains three conserved domains, matrix (MA), capsid (CA), and nucleocapsid (NC). Gag plays the primary role in immature particle assembly and viral genomic RNA (vRNA) recruitment and packaging.Retroviruses assemble via two different morphogenetic pathways; the first, historically referred to as C-type, wherein particle assembly occurs at the cell membrane, and the second, D-type, assembling in perinuclear regions. The pathogenic human viruses, HIV and human T-cell lymphotropic virus assemble via C-type intermediates, whereas M-PMV is the prototypic D-type retrovirus. The Gag polyprotein of M-PMV is first transported to an intracytoplasmic pericentriolar site, where particle assembly...

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

“…Reverse transcription-PCR (RT-PCR) was performed as described previously (37). Briefly, the HEK 293T cells were transfected with wt or RKK/AAA mutant proviral construct.…”

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

Nucleic Acid Binding by Mason-Pfizer Monkey Virus CA Promotes Virus Assembly and Genome Packaging

Füzik

Píchalová

Schur

et al. 2016

J Virol

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“…Introduction of SP-like domain mutations into M-PMV proviral vectors (pSARM4 and pSARM4-EGFP) was carried out in two cloning steps. First, the mutations created by two-step PCR were introduced into a helper vector (MHelppUC19) constructed by inserting M-PMV SacI-Eco72I fragments (nucleotides 1165 to 3275) into pUC19 (53). Following sequence verification, the SacI-Eco72I fragment of MHelppUC19 carrying the appropriate mutation was inserted into the M-PMV proviral constructs pSARM4 and pSARM-EGFP.…”

Section: Methodsmentioning

confidence: 99%

Role of Mason-Pfizer Monkey Virus CA-NC Spacer Peptide-Like Domain in Assembly of Immature Particles

Strohalmová-Bohmová

Spiwok

Lepšı́k

et al. 2014

J Virol

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The hexameric lattice of an immature retroviral particle consists of Gag polyprotein, which is the precursor of all viral structural proteins. Lentiviral and alpharetroviral Gag proteins contain a peptide sequence called the spacer peptide (SP), which is localized between the capsid (CA) and nucleocapsid (NC) domains. SP plays a critical role in intermolecular interactions during the assembly of immature particles of several retroviruses. Published models of supramolecular structures of immature particles suggest that in lentiviruses and alpharetroviruses, SP adopts a rod-like six-helix bundle organization. In contrast, Mason-Pfizer monkey virus (M-PMV), a betaretrovirus that assembles in the cytoplasm, does not contain a distinct SP sequence, and the CA-NC connecting region is not organized into a clear rod-like structure. Nevertheless, the CA-NC junction comprises a sequence critical for assembly of immature M-PMV particles. In the present work, we characterized this region, called the SP-like domain, in detail. We provide biochemical data confirming the critical role of the M-PMV SP-like domain in immature particle assembly, release, processing, and infectivity. Circular dichroism spectroscopy revealed that, in contrast to the SP regions of other retroviruses, a short SP-like domain-derived peptide (SPLP) does not form a purely helical structure in aqueous or helix-promoting solution. Using 8-Å cryo-electron microscopy density maps of immature M-PMV particles, we prepared computational models of the SP-like domain and indicate the structural features required for M-PMV immature particle assembly. IMPORTANCERetroviruses such as HIV-1 are of great medical importance. Using Mason-Pfizer monkey virus (M-PMV) as a model retrovirus, we provide biochemical and structural data confirming the general relevance of a short segment of the structural polyprotein Gag for retrovirus assembly and infectivity. Although this segment is critical for assembly of immature particles of lentiviruses, alpharetroviruses, and betaretroviruses, the organization of this domain is strikingly different. A previously published electron microscopic structure of an immature M-PMV particle allowed us to model this important region into the electron density map. The data presented here help explain the different packing of the Gag segments of various retroviruses, such as HIV, Rous sarcoma virus (RSV), and M-PMV. Such knowledge contributes to understanding the importance of this region and its structural flexibility among retroviral species. The region might play a key role in Gag-Gag interactions, leading to different morphological pathways of immature particle assembly.

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Characterization and in vitro assembly of tick‐borne encephalitis virus C protein

et al. 2020

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Tick‐borne encephalitis virus (TBEV), a member of flaviviruses, represents a serious health threat by causing human encephalitis mainly in central and eastern Europe, Russia, and northeastern Asia. As no specific therapy is available, there is an urgent need to understand all steps of the TBEV replication cycle at the molecular level. One of the critical events is the packaging of flaviviral genomic RNA by TBEV C protein to form a nucleocapsid. We purified recombinant TBEV C protein and used a combination of physical–chemical approaches, such as size‐exclusion chromatography, circular dichroism, NMR spectroscopies, and transmission electron microscopy, to analyze its structural stability and its ability to dimerize/oligomerize. We compared the ability of TBEV C protein to assemble in vitro into a nucleocapsid‐like structure with that of dengue C protein.

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The G-Patch Domain of Mason-Pfizer Monkey Virus Is a Part of Reverse Transcriptase

Cited by 22 publications

References 31 publications

Nucleic Acid Binding by Mason-Pfizer Monkey Virus CA Promotes Virus Assembly and Genome Packaging

Nucleic Acid Binding by Mason-Pfizer Monkey Virus CA Promotes Virus Assembly and Genome Packaging

Role of Mason-Pfizer Monkey Virus CA-NC Spacer Peptide-Like Domain in Assembly of Immature Particles

Characterization and in vitro assembly of tick‐borne encephalitis virus C protein

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