Nidovirus RNA polymerases: Complex enzymes handling exceptional RNA genomes

Posthuma, Clara C.; Velthuis, Aartjan J.W. te; Snijder, Eric J.

doi:10.1016/j.virusres.2017.01.023

Cited by 115 publications

(135 citation statements)

References 140 publications

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“…This result indicates that 1B can exert an effect on the HEL domain to promote the interaction, which is also consistent with the finding that EAV nsp10 1B interacts with the HEL domain (37). For nsp9, it is expected that there is cross talk between the NiRAN domain and RdRp (63). We actually have some evidence to support this possibility (unpublished data).…”

Section: Insight Into the Interactions Of Nsp9 And Nsp10 With Membransupporting

confidence: 87%

Mapping the Nonstructural Protein Interaction Network of Porcine Reproductive and Respiratory Syndrome Virus

Song

Liu

Gao

et al. 2018

J Virol

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Porcine reproductive and respiratory syndrome virus (PRRSV) is a positivestranded RNA virus belonging to the family Arteriviridae. Synthesis of the viral RNA is directed by replication/transcription complexes (RTC) that are mainly composed of a network of PRRSV nonstructural proteins (nsps) and likely cellular proteins. Here, we mapped the interaction network among PRRSV nsps by using yeast two-hybrid screening in conjunction with coimmunoprecipitation (co-IP) and cotransfection assays. We identified a total of 24 novel interactions and found that the interactions were centered on open reading frame 1b (ORF1b)-encoded nsps that were mainly connected by the transmembrane proteins nsp2, nsp3, and nsp5. Interestingly, the interactions of the core enzymes nsp9 and nsp10 with transmembrane proteins did not occur in a straightforward manner, as they worked in the co-IP assay but were poorly capable of finding each other within intact mammalian cells. Further proof that they can interact within cells required the engineering of N-terminal truncations of both nsp9 and nsp10. However, despite the poor colocalization relationship in cotransfected cells, both nsp9 and nsp10 came together with membrane proteins (e.g., nsp2) at the viral replication and transcription complexes (RTC) in PRRSV-infected cells. Thus, our results indicate the existence of a complex interaction network among PRRSV nsps and raise the possibility that the recruitment of key replicase proteins to membrane-associated nsps may involve some regulatory mechanisms during infection. IMPORTANCE Synthesis of PRRSV RNAs within host cells depends on the efficient and correct assembly of RTC that takes places on modified intracellular membranes. As an important step toward dissecting this poorly understood event, we investigated the interaction network among PRRSV nsps. Our studies established a comprehensive interaction map for PRRSV nsps and revealed important players within the network. The results also highlight the likely existence of a regulated recruitment of the PRRSV core enzymes nsp9 and nsp10 to viral membrane nsps during PRRSV RTC assembly. Downloaded fromframe 1a (ORF1a) and ORF1b (Fig. 1A), which specify replicase nonstructural proteins (nsps) important for viral RNA synthesis and for antagonizing host antiviral immunity (8,9). Upon virus entry, ORF1a is translated from the incoming genome to produce replicase polyprotein pp1a, which is further matured into at least 10 nsps (e.g., nsp1␣, nsp1␤, nsp2 to nsp6, nsp7␣, nsp7␤, and nsp8) by virus-encoded proteases within nsp1␣, nsp1␤, nsp2, and nsp4 (7, 10, 11). In addition, there exist isoforms for nsp2, and one of them (nsp2TF) is made via a Ϫ2 frameshift mechanism (12, 13). On the other hand, translation of ORF1b, an open reading frame that specifies replicase proteins nsp9, nsp10, nsp11, and nsp12, involves a Ϫ1 ribosome frameshift (14-16).Synthesis of PRRSV RNA within host cells depends on the efficient and correct assembly of replication and transcription complexes (RTC) that coordinate the tran-FI...

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Section: Insight Into the Interactions Of Nsp9 And Nsp10 With Membransupporting

confidence: 87%

Mapping the Nonstructural Protein Interaction Network of Porcine Reproductive and Respiratory Syndrome Virus

Song

Liu

Gao

et al. 2018

J Virol

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“…The PRRSV nsp9 encodes the function of viral RdRp and is the engine driving viral RNA synthesis Beerens et al 2007;Posthuma et al 2017); it is encoded within ORF1b and translated through the C-terminal extension of nsp8 during infection (Meulenberg et al 1993;Kappes and Faaberg 2015). However, it is not clear whether the mature form of nsp9 retains nsp8, although the nsp8-9 does not contain the predictable cleavage sites for nsp2 or nsp4.…”

Section: Discussionmentioning

confidence: 99%

“…The nsp9 replicase protein is a critical determinant for the fatal virulence of the Chinese HP-PRRSV (Li et al 2014;Xu et al 2018;Zhao et al 2018). This protein specifies the putative function of viral RNA-dependent RNA polymerase (RdRp) and is the major engine for catalyzing the viral RNA synthesis during PRRSV infection Beerens et al 2007;Posthuma et al 2017). Comparative bioinformatics analyses based on the studies of equine arteritis virus (EAV) and other positive-stranded RNA viruses have localized the viral RdRp domain to the C-terminal half of nsp9 (Gorbalenya et al 1989) and assigned nidovirus RdRp-associated nucleotidyltransferase domain (NiRAN) to the N-terminal region of ORF1b-encoded portion (Lehmann et al 2015).…”

Section: Introductionmentioning

confidence: 99%

“…Comparative bioinformatics analyses based on the studies of equine arteritis virus (EAV) and other positive-stranded RNA viruses have localized the viral RdRp domain to the C-terminal half of nsp9 (Gorbalenya et al 1989) and assigned nidovirus RdRp-associated nucleotidyltransferase domain (NiRAN) to the N-terminal region of ORF1b-encoded portion (Lehmann et al 2015). As a result of the frameshift strategy, nsp9, the first protein within ORF1b, is expressed during infection as the C-terminal extension of nsp8, a small viral nsp that is encoded by ORF1a (Fang and Snijder 2010;Posthuma et al 2017). However, it has remained unclear whether the mature form of nsp9 in virus-infected cells still retains nsp8.…”

Section: Introductionmentioning

confidence: 99%

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Identification of Nonstructural Protein 8 as the N-Terminus of the RNA-Dependent RNA Polymerase of Porcine Reproductive and Respiratory Syndrome Virus

Liu

Chai

et al. 2018

Virol. Sin.

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Porcine reproductive and respiratory syndrome virus (PRRSV) is a member within the family Arteriviridae of the order Nidovirales. Replication of this positive-stranded RNA virus within the host cell involves expression of viral replicase proteins encoded by two ORFs, namely ORF1a and ORF1b. In particular, translation of ORF1b depends on a -1-ribosomal frameshift strategy. Thus, nonstructural protein 9 (nsp9), the first protein within ORF1b that specifies the function of the viral RNA-dependent RNA polymerase, is expressed as the C-terminal extension of nsp8, a small nsp that is encoded by ORF1a. However, it has remained unclear whether the mature form of nsp9 in virus-infected cells still retains nsp8, addressing which is clearly critical to understand the biological function of nsp9. By taking advantage of specific antibodies to both nsp8 and nsp9, we report the following findings. (1) In infected cells, PRRSV nsp9 was identified as a major product with a size between 72 and 95 kDa (72-95 KDa form), which exhibited the similar mobility on the gel to the in vitro expressed nsp8-9 ORF1b , but not the ORF1b-coded portion (nsp9 ORF1b ). (2) The antibodies to nsp8, but not to nsp7 or nsp10, could detect a major product that had the similar mobility to the 72-95 KDa form of nsp9. Moreover, nsp9 could be co-immunoprecipitated by antibodies to nsp8, and vice versa. (3) Neither nsp4 nor nsp2 PLP2 was able to cleave nsp8-nsp9 in vitro. Together, our studies provide experimental evidence to suggest that nsp8 is an N-terminal extension of nsp9. Our findings here paves way for further charactering the biological function of PRRSV nsp9.

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“…[125][126][127][128] This is important as ssRNA replicases do not possess sufficient helicase activity to unwind longer double stranded RNA (dsRNA) duplex structures. [130] Notably, a Nidovirus with a genome larger than 40 kb was recently described by Saberi et al, suggesting that maintenance of large RNA genomes by these mechanisms might be possible. Thus, close coordination is required to avoid steric clashes between the replicase and translating ribosomes.…”

Section: Potential and Limitations Of Protein-catalyzed Rna Replicationmentioning

confidence: 99%

Templated Self‐Replication in Biomimetic Systems

et al. 2019

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nanostructures and nanopatterns. [13][14][15] The specificity of the molecular recognitions between replicative units is concomitant with the encoding and transmission of information, with the degree of specificity determining the fidelty and capacity of information transfer against competing background interactions in noisy "chemical" environments. [16] However, the ability to replicate in this manner does not imply the ability to transmit additional heritable information-simple replicators can only replicate information related to recognition and template directed autocatalysis as this information is intrinsically linked to phenotype. In contrast to most artificial autocatalytic replicators, living systems (including viruses) store the key instructions for replication on an inheritable genetic system rather than in the native structures of the individual sub-components. This decoupling of phenotype and genotype enables heredity and open-ended evolution, the possibility of an indefinite increase in complexity, as evolutionary innovations aquired by natural selection are anchored in the genotype only. [17,18] The most prominent self-replicating molecules are nucleic acids, which form the fundamental basis for information storage and propagation in biological systems. The ability of polynucleic acids to store information is self-evident, and based upon the ability to form cognate Watson-Crick base pair interactions. Nucleic acid systems may have also formed the first genetic replicators in biology. The RNA world hypothesis postulates a stage in the origin of life in which RNA proliferated before the emergence of DNA and proteins. To do this, RNA must be able to carry out several key roles: information storage, catalysis, and (self-) replication. Multiple examples of catalytic RNAs (ribozymes) are known both from nature and in vitro selection experiments, [19][20][21][22] but there is no fossil evidence of an RNA capable of (self-)replication without the involvement of proteins.While minimal nucleic acid-only systems with replicationlike properties have been identified by directed evolution and engineering, limitations such as low activity, lack of generality, and poor information capacity limit their usefulness in bottomup synthetic biology, except in origin of life research. For the creation of more complex biological in vitro systems, RNA or DNA replication mechanisms involving more powerful protein enzymes are likely to be necessary. Even so, the achievement of self-sustained in vitro self-replication inspired by the central dogma of molecular biology is currently hampered by the requirement to encode and efficiently express the enormous A key characteristic of living systems is the storage and replication of information, and as such the development of self-replicating systems capable of heredity is of great importance to the fields of synthetic biology and origin of life research. In this review, the design and implementation of self-replicating systems in the context of bottom-up synthetic biology is discusse...

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Nidovirus RNA polymerases: Complex enzymes handling exceptional RNA genomes

Cited by 115 publications

References 140 publications

Mapping the Nonstructural Protein Interaction Network of Porcine Reproductive and Respiratory Syndrome Virus

Mapping the Nonstructural Protein Interaction Network of Porcine Reproductive and Respiratory Syndrome Virus

Identification of Nonstructural Protein 8 as the N-Terminus of the RNA-Dependent RNA Polymerase of Porcine Reproductive and Respiratory Syndrome Virus

Templated Self‐Replication in Biomimetic Systems

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