Distinct Roles for Nucleic Acid in In Vitro Assembly of Purified Mason-Pfizer Monkey Virus CANC Proteins

Ulbrich, Pavel; Haubova, Sarka; Nermut, M. V.; Hunter, Eric; Rumlová, Michaela; Ruml, Tomáš

doi:10.1128/jvi.02694-05

Cited by 34 publications

(55 citation statements)

References 83 publications

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“…Particles of XMRV ⌬ProCANC and ⌬10CANC were not detected if the in vitro assembly was carried out in the absence of nucleic acid or at an NaCl concentration higher than 0.5 M (data not shown), suggesting that assembly must be initiated by the addition of nucleic acids under suitable conditions. Similar assembly requirements have been observed for the in vitro-assembled particles of RSV CANC (8), HIV-1 CANC (8,21,22), and M-PMV ⌬ProCANC (57).…”

Section: Resultssupporting

confidence: 51%

“…It is known that the prevention of ␤-hairpin formation (by either the deletion or substitution of Pro1 or by N-terminal extension of CA) can shift the assembly mode to formation of immature-virus-like structures (21,46,50,57,61). We therefore decided to truncate the XMRV CANC construct by the deletion of the first proline residue (⌬ProCANC) with the aim of assembling immature-like structures.…”

Section: Resultsmentioning

confidence: 99%

“…1). To study the ability of XMRV CA and CANC to assemble into VLPs, we used both bacterial and in vitro assembly systems (50,57). TEM of thinsectioned E. coli BL21(DE3) expressing XMRV CA and CANC showed amorphous inclusion bodies instead of assembled mature-core-like structures ( Fig.…”

Section: Resultsmentioning

confidence: 99%

“…A number of studies have mimicked the assembly of both immature virus particles and mature cores in vitro using purified recombinant Gag-derived capsid-nucleocapsid (CANC) proteins (8,21,22,31,41,57,68). Although the in vitro assembly of retroviral genera, including the lentivirus HIV-1 (8,12,21,22), the betaretrovirus Mason-Pfizer monkey virus (M-PMV) (31,57), and the alpharetrovirus RSV (8,40,41,68), has been intensively studied, there is a lack of information on the in vitro assembly of gammaretroviruses. In vitro assembly was achieved by using His-tagged MLV CA molecules anchored to Ni 2ϩ -chelating lipid nanotubes as an assembly substrate (24).…”

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confidence: 99%

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In Vitro Assembly of Virus-Like Particles of a Gammaretrovirus, the Murine Leukemia Virus XMRV

Hadravová

Marco

Ulbrich

et al. 2012

J Virol

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Immature retroviral particles are assembled by self-association of the structural polyprotein precursor Gag. During maturation the Gag polyprotein is proteolytically cleaved, yielding mature structural proteins, matrix (MA), capsid (CA), and nucleocapsid (NC), that reassemble into a mature viral particle. Proteolytic cleavage causes the N terminus of CA to fold back to form a ␤-hairpin, anchored by an internal salt bridge between the N-terminal proline and the inner aspartate. Using an in vitro assembly system of capsid-nucleocapsid protein (CANC), we studied the formation of virus-like particles (VLP) of a gammaretrovirus, the xenotropic murine leukemia virus (MLV)-related virus (XMRV). We show here that, unlike other retroviruses, XMRV CA and CANC do not assemble tubular particles characteristic of mature assembly. The prevention of ␤-hairpin formation by the deletion of either the N-terminal proline or 10 initial amino acids enabled the assembly of ⌬ProCANC or ⌬10CANC into immature-like spherical particles. Detailed three-dimensional (3D) structural analysis of these particles revealed that below a disordered N-terminal CA layer, the C terminus of CA assembles a typical immature lattice, which is linked by rod-like densities with the RNP.

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Section: Resultssupporting

confidence: 51%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

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In Vitro Assembly of Virus-Like Particles of a Gammaretrovirus, the Murine Leukemia Virus XMRV

Hadravová

Marco

Ulbrich

et al. 2012

J Virol

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“…The importance of RNA for assembly is well documented by in vitro assembly studies with various retroviruses, e.g., Rous sarcoma virus (RSV), HIV, murine leukemia virus (MLV), and M-PMV (5)(6)(7)(8)(9)(10)(11). Although cellular RNA is sufficient to promote Gag assembly (12), formation of an infectious retrovirus requires specific packaging of the viral genome (vRNA) into the assembling Gag particle.…”

mentioning

confidence: 99%

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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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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Distinct Roles for Nucleic Acid in In Vitro Assembly of Purified Mason-Pfizer Monkey Virus CANC Proteins

Cited by 34 publications

References 83 publications

In Vitro Assembly of Virus-Like Particles of a Gammaretrovirus, the Murine Leukemia Virus XMRV

In Vitro Assembly of Virus-Like Particles of a Gammaretrovirus, the Murine Leukemia Virus XMRV

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

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

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