Solving a Levinthal's paradox for virus assembly identifies a unique antiviral strategy

Dykeman, Eric C.; Stockley, Peter G.; Twarock, Reidun

doi:10.1073/pnas.1319479111

Cited by 108 publications

(136 citation statements)

References 54 publications

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“…A hierarchy of PS CP affinities is an essential requirement of the PS-mediated assembly model (9) and is consistent with the sequence/structure variations in PSs PS1-5 on the genomic fragment. PS3 is the highest affinity site and the other PSs contribute to assembly efficiency but cannot trigger VLP formation alone.…”

Section: Natural Pss Act Cooperativelysupporting

confidence: 64%

“…Here we have used smFCS assays to probe the roles of RNA in STNV assembly at nanomolar concentrations, showing that it follows a two-stage PS-mediated mechanism, thus preventing assembly around noncognate RNAs. Even with relatively short PS fragments we have recreated assembly features seen with the intact genome, showing that CP recognition of degenerate PSs, and the latter's relative spacing along the genomic RNA, both contribute to efficient cooperative capsid assembly (9,41). These assays also validate the use of RNA SELEX against viral CPs, combined with theoretical analysis techniques pioneered by us, as a route for identifying PSs (15).…”

Section: Discussionmentioning

confidence: 65%

“…PSs are bound sequence-specifically by their cognate CPs, increasing the yield, rate and/or fidelity of assembly. PSmediated assembly has many potential advantages for the virus, including solving a viral version of the Levinthal Paradox (9). For the T = 3 MS2, there is a known assembly origin, the 19-nt-long coat protein gene translational operator (TR) stem-loop (10).…”

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confidence: 99%

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Revealing the density of encoded functions in a viral RNA

Patel

Dykeman

Coutts

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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We present direct experimental evidence that assembly of a single-stranded RNA virus occurs via a packaging signal-mediated mechanism. We show that the sequences of coat protein recognition motifs within multiple, dispersed, putative RNA packaging signals, as well as their relative spacing within a genomic fragment, act collectively to influence the fidelity and yield of capsid selfassembly in vitro. These experiments confirm that the selective advantages for viral yield and encapsidation specificity, predicted from previous modeling of packaging signal-mediated assembly, are found in Nature. Regions of the genome that act as packaging signals also function in translational and transcriptional enhancement, as well as directly coding for the coat protein, highlighting the density of encoded functions within the viral RNA. Assembly and gene expression are therefore direct molecular competitors for different functional folds of the same RNA sequence. The strongest packaging signal in the test fragment, encodes a region of the coat protein that undergoes a conformational change upon contact with packaging signals. A similar phenomenon occurs in other RNA viruses for which packaging signals are known. These contacts hint at an even deeper density of encoded functions in viral RNA, which if confirmed, would have profound consequences for the evolution of this class of pathogens.virus assembly | single-molecule fluorescence correlation spectroscopy | satellite tobacco necrosis virus | packaging signal

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Section: Natural Pss Act Cooperativelysupporting

confidence: 64%

Section: Discussionmentioning

confidence: 65%

mentioning

confidence: 99%

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Revealing the density of encoded functions in a viral RNA

Patel

Dykeman

Coutts

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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“…For Qβ and other ssRNA viruses, there is clearly an evolutionary mandate for efficient and accurate virion assembly (34). After the gRNA is replicated and coat proteins are produced, the rate-limiting step in virion production is encapsidation of the RNA (35).…”

Section: Discussionmentioning

confidence: 99%

Asymmetric cryo-EM structure of the canonical Allolevivirus Qβ reveals a single maturation protein and the genomic ssRNA in situ

Gorzelnik

Zhao

Reed

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Single-stranded (ss) RNA viruses infect all domains of life. To date, for most ssRNA virions, only the structures of the capsids and their associated protein components have been resolved to high resolution. Qβ, an ssRNA phage specific for the conjugative F-pilus, has a T = 3 icosahedral lattice of coat proteins assembled around its 4,217 nucleotides of genomic RNA (gRNA). In the mature virion, the maturation protein, A 2 , binds to the gRNA and is required for adsorption to the F-pilus. Here, we report the cryo-electron microscopy (cryo-EM) structures of Qβ with and without symmetry applied. The icosahedral structure, at 3.7-Å resolution, resolves loops not previously seen in the published X-ray structure, whereas the asymmetric structure, at 7-Å resolution, reveals A 2 and the gRNA. A 2 contains a bundle of α-helices and replaces one dimer of coat proteins at a twofold axis. The helix bundle binds gRNA, causing denser packing of RNA in its proximity, which asymmetrically expands the surrounding coat protein shell to potentially facilitate RNA release during infection. We observe a fixed pattern of gRNA organization among all viral particles, with the major and minor grooves of RNA helices clearly visible. A single layer of RNA directly contacts every copy of the coat protein, with one-third of the interactions occurring at operator-like RNA hairpins. These RNA-coat interactions stabilize the tertiary structure of gRNA within the virion, which could further provide a roadmap for capsid assembly.single-particle cryo-EM | Allolevivirus | ssRNA virus | genomic RNA | maturation protein S ingle-stranded (ss) RNA viruses are an abundant type of virus and infect all domains of life (1-4). One of the beststudied ssRNA virus systems is the Leviviridae, which infects Gram-negative bacteria via a variety of retractile pili (5); extensive genetic and biochemical studies have been performed on two of these phages: MS2 and Qβ (5-11). All of the Leviviridae have the same core genome, spanning 3.4-4.3 kb, encoding the maturation protein, the coat protein, and a subunit of RNAdependent RNA replicase (SI Appendix, Fig. S1) (10). The MS2-like phages, designated true leviviruses, have a fourth gene that encodes the lysis protein, whereas the Qβ-like phages, designated alloleviviruses, have the lysis function as an additional feature of the maturation protein (called A 2 in Qβ). Qβ also encodes a minor coat protein, called A 1 , arising from occasional readthrough of the stop codon of the major coat protein; it has been estimated that the A 1 protein replaces 3-10 copies of the major coat protein in the virion (11) and is required for infection (12). A 1 consists of a coat domain and a read-through domain separated by a flexible linker (13). Unlike most dsDNA phages, which use specialized protein machinery to pump their genomic DNA into a capsid preassembled around a protein scaffold (14-17), ssRNA viruses, including the Leviviridae, assemble their coat proteins around the genomic RNA (gRNA), presumably because the extremely small ...

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“…21,22 We envisage applications of our theory to the association of more complex molecules like DNA tiles [23][24][25] or virial caspids. 26 In Sec. II, we derive our theory while in Sec.…”

Section: Introductionmentioning

confidence: 99%

Communication: Free energy of ligand-receptor systems forming multimeric complexes

Michele

Bachmann

Parolini

et al. 2016

The Journal of Chemical Physics

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Ligand-receptor interactions are ubiquitous in biology and have become popular in materials in view of their applications to programmable self-assembly. Although complex functionalities often emerge from the simultaneous interaction of more than just two linker molecules, state of the art theoretical frameworks enable the calculation of the free energy only in systems featuring one-to-one ligand/receptor binding. In this Communication, we derive a general formula to calculate the free energy of systems featuring simultaneous direct interaction between an arbitrary number of linkers. To exemplify the potential and generality of our approach, we apply it to the systems recently introduced by Parolini et al. [ACS Nano 10, 2392

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Solving a Levinthal's paradox for virus assembly identifies a unique antiviral strategy

Cited by 108 publications

References 54 publications

Revealing the density of encoded functions in a viral RNA

Revealing the density of encoded functions in a viral RNA

Asymmetric cryo-EM structure of the canonical Allolevivirus Qβ reveals a single maturation protein and the genomic ssRNA in situ

Communication: Free energy of ligand-receptor systems forming multimeric complexes

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