Structural Basis for the dsRNA Specificity of the Lassa Virus NP Exonuclease

Hastie, Kathryn M.; King, Liam B.; Zandonatti, Michelle; Saphire, Erica Ollmann

doi:10.1371/journal.pone.0044211

Cited by 54 publications

(78 citation statements)

References 23 publications

(47 reference statements)

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“…As all arenaviruses encode a strong IFN antagonist NP, which inhibits the IFN induction through the conserved RNase domain (15)(16)(17)(18)(19)(20), we wondered what the respective roles are of pathogenic Z and NP in the IFN suppression during an authentic arenavirus infection. We thus generated rPICVs encoding a pathogenic Z protein (ZN LCMV ) in the backbone of an NP RNase catalytically inactive D380A mutant (NPm1).…”

Section: (I) the Z Proteins Of Pathogenic Arenaviruses But Not Nonpatmentioning

confidence: 99%

“…Ebola virus (EBOV) VP35 blocks RLR signaling through multiple mechanisms such as sequestering the RIG-i cofactor PKR activator (PACT), preventing the interactions of TBK1 and IKKε with IRFs, and inhibiting IRF7 activity (10-14). Arenaviral nucleoprotein (NP) strongly inhibits the production of type I IFNs through its DEDDH exoribonuclease (RNase) activity, possibly by degrading the immunostimulatory dsRNA substrates (15)(16)(17)(18)(19)(20).Arenaviruses are a diverse family of negative-strand enveloped RNA viruses with a bisegmented RNA genome, which encodes two proteins on each segment in an ambisense orientation-glycoprotein GPC and nucleoprotein NP on the S segment and L polymerase protein and the small matrix protein Z on the L segment (21). Arenaviruses can cause a wide spectrum of diseases in humans, with limited preventive or therapeutic options (22, 23).…”

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confidence: 99%

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The Z Proteins of Pathogenic but Not Nonpathogenic Arenaviruses Inhibit RIG-i-Like Receptor-Dependent Interferon Production

Xing

Liang

2015

J Virol

107

117

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Arenavirus pathogens cause a wide spectrum of diseases in humans ranging from central nervous system disease to lethal hemorrhagic fevers with few treatment options. The reason why some arenaviruses can cause severe human diseases while others cannot is unknown. We find that the Z proteins of all known pathogenic arenaviruses, lymphocytic choriomeningitis virus ( IMPORTANCEWe show that all known human-pathogenic arenaviruses share an innate immune suppression mechanism that is based on viral Z protein-mediated RLR inhibition. Our report offers important insights into the potential mechanism of arenavirus pathogenesis, provides a convenient way to evaluate the pathogenic potential of known and/or emerging arenaviruses, and reveals a novel target for the development of broad-spectrum therapies to treat this group of diverse pathogens. More broadly, our report provides a better understanding of the mechanisms of viral immune suppression and host-pathogen interactions. Intracellular RNA viruses are recognized by a family of cytosolic RNA helicase proteins called retinoic acid-inducible gene 1 (RIG-i)-like receptors (RLRs) to activate the antiviral and inflammatory signals (1, 2). The RLR members include RIG-i, Melanoma Differentiation-Associated protein 5 (MDA5), and Laboratory of Genetics and Physiology 2 (LGP2) (3-5). RIG-i recognizes short double-stranded RNA (dsRNA) with 5= triphosphate, while MDA5 recognizes long RNA duplexes (6). Upon ligand binding by the C-terminal domains (CTD) of RIG-i and MDA5, these proteins undergo conformational changes to activate the N-terminal CARD domains that mediate their interactions with the adaptor molecule mitochondrial antiviral signaling (MAVS)/IPS-1/virus-induced signaling adaptor (VISA)/Cardif to trigger the signaling cascades that consist of tumor necrosis factor (TNF) receptor-associated factors (TRAFs), TANK-binding kinase 1 (TBK1), and inhibitor-B kinase ε (IKKε) to activate transcription factors NF-B, interferon (IFN) regulatory factor 3 (IRF3), and IRF7, which induce the production of the type I IFNs and other cytokines (3). The RLR pathway is essential for host innate immunity to RNA viruses and is thus a major target of viral immune evasion mechanisms (4, 7). Influenza virus NS1 inhibits RIG-i activation by interacting with TRIM25 to prevent RIG-i ubiquitinylation (8). Paramyxovirus V protein binds and inhibits MDA5 (9). Ebola virus (EBOV) VP35 blocks RLR signaling through multiple mechanisms such as sequestering the RIG-i cofactor PKR activator (PACT), preventing the interactions of TBK1 and IKKε with IRFs, and inhibiting IRF7 activity (10-14). Arenaviral nucleoprotein (NP) strongly inhibits the production of type I IFNs through its DEDDH exoribonuclease (RNase) activity, possibly by degrading the immunostimulatory dsRNA substrates (15)(16)(17)(18)(19)(20).Arenaviruses are a diverse family of negative-strand enveloped RNA viruses with a bisegmented RNA genome, which encodes two proteins on each segment in an ambisense orientation-glycoprotein GPC and nuc...

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Section: (I) the Z Proteins Of Pathogenic Arenaviruses But Not Nonpatmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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The Z Proteins of Pathogenic but Not Nonpathogenic Arenaviruses Inhibit RIG-i-Like Receptor-Dependent Interferon Production

Xing

Liang

2015

J Virol

107

117

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“…The C-terminal domain of LASV NP is well known as a 3=-to-5= dsRNA-specific exonuclease (22,40,41). However, the function of the N-terminal domain is more complicated.…”

Section: Discussionmentioning

confidence: 99%

Structural and Functional Diversity of Nairovirus-Encoded Nucleoproteins

Wang

Long

Xü

et al. 2015

J Virol

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The nairoviruses include assorted tick-borne bunyaviruses that are emerging as causative agents of infectious diseases among humans and animals. As negative-sense single-stranded RNA (؊ssRNA) viruses, nairoviruses encode nucleoprotein (NP) that encapsidates the genomic RNA and further forms ribonucleoprotein (RNP) complex with viral RNA-dependent RNA polymerase (RdRp). We previously revealed that the monomeric NP encoded by Crimean-Congo hemorrhagic fever virus (CCHFV) presents a racket-shaped structure and shows unusual DNA-specific endonuclease activity. To examine the structural and biological variation of nairovirus-encoded NPs, here, we systematically solved the crystal structures of NPs encoded by various nairoviruses, including Hazara virus (HAZV), Kupe virus (KUPV), and Erve virus (ERVEV). Combined with biochemical analysis, our results generate a clearer picture to aid in the understanding of the functional diversity of nairovirus-encoded NPs and the formation of nairovirus RNPs. IMPORTANCENairoviruses comprise several tick-borne bunyaviruses that are emerging as causative agents of infectious diseases among humans and animals; however, little is known of the nairovirus genome assembly and transcription mechanisms. Based on the previous study of CCHFV NP reported by different research groups, we systematically investigate here the structural and functional diversity among three different nairoviruses. This work provides important information on nairovirus nucleoprotein function and the formation of RNPs. Bunyaviridae is the largest negative-sense, single-stranded (ϪssRNA) virus family and contains various pathogens that cause severe infectious diseases in humans, other animals, and plants (1). Over 300 members of the Bunyaviridae family are currently classified into five distinct genera, i.e., Orthobunyavirus, Hantavirus, Nairovirus, Phlebovirus, and Tospovirus (1). Bunyaviruses are characterized by their trisegmented negative-sense genome, in which the large (L) segment encodes RNA-dependent RNA polymerase (RdRp), the medium (M) segment encodes surface glycoproteins, and the small (S) segment encodes nucleocapsid (NP) protein (1). As in other ϪssRNA viruses, the genomic RNA of bunyaviruses does not exist as a naked RNA but must be encapsidated by viral NP to form a high-order NP-RNA complex, which further constructs a ribonucleoprotein (RNP) complex with viral RdRp (2, 3).The Nairovirus genus comprises a number of pathogens that cause infectious diseases in humans and livestock. Nairoviruses are transmitted by ticks, which distinguishes them from other members of the Bunyaviridae family (4). Based on antibody crossreactivities, nairoviruses are classified into seven serogroups (see Table S1 in the supplemental material) (5). CCHFV, which belongs to the CCHF serogroup, is the most notable pathogen: it causes CCHF in humans, with high mortality, and occurs spontaneously in more than 30 countries in Asia, the Middle East, southeastern Europe, and Africa (6). The high pathogenicity of CCHFV has led...

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“…For example, encapsidation of the entire genome of negative-sense single-stranded RNA (ssRNA) viruses by nucleoprotein (N) molecules prevents attacks by the host. Recently, N proteins have also been shown to possess secondary functions such as the exoribonuclease activity of the Lassa virus N protein that helps the virus evade host immune surveillance (1,2) or the endonuclease activity of the Crimean-Congo hemorrhagic fever virus (CCHFV) nucleoprotein (3). These additional roles for N protein were explained with the elucidation of the structure of the Lassa virus N protein that surprisingly revealed the presence of an exonuclease fold at the C terminus.…”

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confidence: 99%

Structure of the Leanyer orthobunyavirus nucleoprotein–RNA complex reveals unique architecture for RNA encapsidation

Niu

Shaw

Wang

et al. 2013

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

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Negative-stranded RNA viruses cover their genome with nucleoprotein (N) to protect it from the human innate immune system. Abrogation of the function of N offers a unique opportunity to combat the spread of the viruses. Here, we describe a unique fold of N from Leanyer virus (LEAV, Orthobunyavirus genus, Bunyaviridae family) in complex with single-stranded RNA refined to 2.78 Å resolution as well as a 2.68 Å resolution structure of LEAV N-ssDNA complex. LEAV N is made up of an N-and a C-terminal lobe, with the RNA binding site located at the junction of these lobes. The LEAV N tetramer binds a 44-nucleotide-long single-stranded RNA chain. Hence, oligomerization of N is essential for encapsidation of the entire genome and is accomplished by using extensions at the N and C terminus. Molecular details of the oligomerization of N are illustrated in the structure where a circular ring-like tertiary assembly of a tetramer of LEAV N is observed tethering the RNA in a positively charged cavity running along the inner edge. Hydrogen bonds between N and the C2 hydroxyl group of ribose sugar explain the specificity of LEAV N for RNA over DNA. In addition, base-specific hydrogen bonds suggest that some regions of RNA bind N more tightly than others. Hinge movements around F20 and V125 assist in the reversal of capsidation during transcription and replication of the virus. Electron microscopic images of the ribonucleoprotein complexes of LEAV N reveal a filamentous assembly similar to those found in phleboviruses.crystal structure | nucleoprotein complex with ssRNA | RNP

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Structural Basis for the dsRNA Specificity of the Lassa Virus NP Exonuclease

Cited by 54 publications

References 23 publications

The Z Proteins of Pathogenic but Not Nonpathogenic Arenaviruses Inhibit RIG-i-Like Receptor-Dependent Interferon Production

The Z Proteins of Pathogenic but Not Nonpathogenic Arenaviruses Inhibit RIG-i-Like Receptor-Dependent Interferon Production

Structural and Functional Diversity of Nairovirus-Encoded Nucleoproteins

Structure of the Leanyer orthobunyavirus nucleoprotein–RNA complex reveals unique architecture for RNA encapsidation

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