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TitleThe RNA-Binding Protein of a Double-Stranded RNA Virus Acts like a Scaffold Protein.
Journal, issue, pagesJ Virol, Vol. 92, Issue 19, Year 2018
Publish dateOct 1, 2018
AuthorsCarlos P Mata / Johann Mertens / Juan Fontana / Daniel Luque / Carolina Allende-Ballestero / David Reguera / Benes L Trus / Alasdair C Steven / José L Carrascosa / José R Castón /
PubMed AbstractInfectious bursal disease virus (IBDV), a nonenveloped, double-stranded RNA (dsRNA) virus with a T=13 icosahedral capsid, has a virion assembly strategy that initiates with a precursor particle based ...Infectious bursal disease virus (IBDV), a nonenveloped, double-stranded RNA (dsRNA) virus with a T=13 icosahedral capsid, has a virion assembly strategy that initiates with a precursor particle based on an internal scaffold shell similar to that of tailed double-stranded DNA (dsDNA) viruses. In IBDV-infected cells, the assembly pathway results mainly in mature virions that package four dsRNA segments, although minor viral populations ranging from zero to three dsRNA segments also form. We used cryo-electron microscopy (cryo-EM), cryo-electron tomography, and atomic force microscopy to characterize these IBDV populations. The VP3 protein was found to act as a scaffold protein by building an irregular, ∼40-Å-thick internal shell without icosahedral symmetry, which facilitates formation of a precursor particle, the procapsid. Analysis of IBDV procapsid mechanical properties indicated a VP3 layer beneath the icosahedral shell, which increased the effective capsid thickness. Whereas scaffolding proteins are discharged in tailed dsDNA viruses, VP3 is a multifunctional protein. In mature virions, VP3 is bound to the dsRNA genome, which is organized as ribonucleoprotein complexes. IBDV is an amalgam of dsRNA viral ancestors and traits from dsDNA and single-stranded RNA (ssRNA) viruses. Structural analyses highlight the constraint of virus evolution to a limited number of capsid protein folds and assembly strategies that result in a functional virion. We report the cryo-EM and cryo-electron tomography structures and the results of atomic force microscopy studies of the infectious bursal disease virus (IBDV), a double-stranded RNA virus with an icosahedral capsid. We found evidence of a new inner shell that might act as an internal scaffold during IBDV assembly. The use of an internal scaffold is reminiscent of tailed dsDNA viruses, which constitute the most successful self-replicating system on Earth. The IBDV scaffold protein is multifunctional and, after capsid maturation, is genome bound to form ribonucleoprotein complexes. IBDV encompasses numerous functional and structural characteristics of RNA and DNA viruses; we suggest that IBDV is a modern descendant of ancestral viruses and comprises different features of current viral lineages.
External linksJ Virol / PubMed:30021893 / PubMed Central
MethodsEM (single particle) / EM (subtomogram averaging)
Resolution20.6 - 54.3 Å
Structure data

EMDB-3507:
IBDV E1-1A population
Method: EM (single particle) / Resolution: 28.2 Å

EMDB-3509:
IBDV E1-1B population
Method: EM (single particle) / Resolution: 20.6 Å

EMDB-3510:
IBDV E1-2 population
Method: EM (single particle) / Resolution: 23.8 Å

EMDB-3511:
IBDV E1 population
Method: EM (subtomogram averaging) / Resolution: 49.5 Å

EMDB-3512:
IBDV E2 population
Method: EM (subtomogram averaging) / Resolution: 54.3 Å

EMDB-3513:
IBDV E3 population
Method: EM (subtomogram averaging) / Resolution: 53.3 Å

EMDB-3514:
IBDV E4 population
Method: EM (subtomogram averaging) / Resolution: 53.2 Å

EMDB-3515:
IBDV E5 population
Method: EM (subtomogram averaging) / Resolution: 47.2 Å

EMDB-3516:
IBDV E6 population
Method: EM (subtomogram averaging) / Resolution: 47.8 Å

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