tRNA elements mediate the assembly of an icosahedral RNA virus

Choi, Yoon Gi; Dreher, Theo W.; Rao, A. L. N.

doi:10.1073/pnas.022618199

Cited by 100 publications

(88 citation statements)

References 40 publications

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“…Bromovirus CP and RNA are amenable for assembly in vitro (2,5,8,37). Previous studies with BCP demonstrated that in vitro assembly is ideal for confirming the packaging defects observed in vivo (5).…”

Section: Fig 2 Electron Microscopy and Image Analysis Of Wt Ccmv Anmentioning

confidence: 99%

Deletion of Highly Conserved Arginine-Rich RNA Binding Motif in Cowpea Chlorotic Mottle Virus Capsid Protein Results in Virion Structural Alterations and RNA Packaging Constraints

Panneerselvam

Apte²,

Wilkens

et al. 2005

J Virol

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The N-proximal region of cowpea chlorotic mottle virus (CCMV) capsid protein (CP) contains an argininerich RNA binding motif (ARM) that is also found in the CPs of other members of Bromoviridae and in other RNA binding proteins such as the Tat and Rev proteins of human immunodeficiency virus. To assess the critical role played by this motif during encapsidation, a variant of CCMV RNA3 (C3) precisely lacking the ARM region (C3/⌬919) of its CP gene was constructed. The biology and the competence of the matured CP derived in vivo from C3/⌬919 to assemble and package progeny RNA was examined in whole plants. Image analysis and computer-assisted three-dimensional reconstruction of wild-type and mutant virions revealed that the CP subunits bearing the engineered deletion assembled into polymorphic virions with altered surface topology. Northern blot analysis of virion RNA from mutant progeny demonstrated that the engineered mutation down-regulated packaging of all four viral RNAs; however, the packaging effect was more pronounced on genomic RNA1 and RNA2 than genomic RNA3 and its CP mRNA. In vitro assembly assays with mutant CP subunits and RNA transcripts demonstrated that the mutant CP is inherently not defective in packaging genomic RNA1 (53%) and RNA2 (54%), but their incorporation into virions was competitively inhibited by the presence of other viral RNAs. Northern blot analysis of RNA encapsidation in vivo of two distinct bromovirus RNA3 chimeras, constructed by exchanging CPs having the ⌬919 deletion, demonstrated that the role of the conserved N-terminal ARM in recognizing and packaging specific RNA is distinct for each virus.The first 25 N-terminal amino acids of the capsid proteins (CPs) of the members of genera Bromovirus, brome mosaic virus (BMV) and cowpea chlorotic mottle virus (CCMVs), have a highly conserved arginine-rich motif (ARM) (26,32). In addition to the bromoviruses, this ARM, which recognizes specific regions in RNA, is also found in other plant virus genera, such as Cucumovirus, Sobemovirus, and Tombusvirus, and in human immunodeficiency virus Tat and Rev proteins, bacterial antiterminators, and ribosomal proteins of nonplant viruses (4,26,32).The genomes of BMV and CCMV are divided among three genomic RNAs. Viral RNA replication is dependent on efficient interaction between two nonstructural proteins, 1a and 2a, encoded by monocistronic RNA1 and RNA2, respectively (16). The two gene products encoded by the dicistronic RNA3 are dispensable for viral replication but are required for infection in plants (10,20,25,26,30). The genomic RNA3 encodes a nonstructural protein of 32 kDa, designated the movement protein (MP) (20,25,26), and a 19-kDa CP that is synthesized from a subgenomic RNA4 (CP mRNA) derived from progeny minus-strand RNA3 by internal initiation (19). The three genomic RNAs and a single subgenomic RNA4 are packaged into three physically and morphologically indistinguishable icosahedral virions (24). These virions having Tϭ3 symmetry are assembled from 180 identical subunits of a sin...

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Section: Fig 2 Electron Microscopy and Image Analysis Of Wt Ccmv Anmentioning

confidence: 99%

Deletion of Highly Conserved Arginine-Rich RNA Binding Motif in Cowpea Chlorotic Mottle Virus Capsid Protein Results in Virion Structural Alterations and RNA Packaging Constraints

Panneerselvam

Apte²,

Wilkens

et al. 2005

J Virol

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“…This suggests that the SL-II structure in BMV RNA3 functions as a cofactor for RNA packaging and also functions in concert with other cis-acting elements that may be present in BMV RNA3 regions other than the 3a ORF or within the 3a ORF. In BMV, the 3Ј-terminal TLS that is conserved in all BMV RNAs also plays a crucial role in RNA packaging in vitro (6). TLS and SL-II in B3PE may cooperate in RNA3 packaging in vivo through direct or indirect interactions between these regions.…”

Section: Discussionmentioning

confidence: 99%

“…RNA regions or elements involved in the packaging of BMV RNAs have been assigned to the coding region of BMV RNA1 by UV cross-linking and band-shift assays (11) as well as to the 3Ј-proximal region of the 3a open reading frame (ORF) in RNA3 (9). The tRNA-like structures (TLS) in the 3Ј-untranslated regions of BMV RNAs also play a crucial role in BMV RNA packaging in vitro (6). In the present study, we delimit a nucleotide sequence required for the efficient packaging of BMV RNA3 and show that 69 nucleotides (nt) in the 3Ј-proximal region of the BMV 3a ORF, especially a predicted stem-loop structure (30 nt), is essential for the efficient packaging of BMV RNA3.…”

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confidence: 99%

cis -Acting Elements Required for Efficient Packaging of Brome Mosaic Virus RNA3 in Barley Protoplasts

Damayanti

Tsukaguchi

Mise

et al. 2003

J Virol

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Viral RNAs are specifically selected for packaging during viral infection. Specific packaging occurs through an interaction between viral RNAs and structural coat proteins (CPs). The specific recognition of viral RNAs by CPs plays a crucial role in diverse facets of the viral life cycle and in the packaging event. The binding of CP to specific RNA elements is required for viral protein translation during infection initiation in alfalfa mosaic virus (28) and for the regulation of translation and the initiation of RNA packaging in the RNA phages (38). In retroviruses, nucleocapsid protein is thought to stimulate genomic RNA dimerization, which is required for efficient RNA packaging, reverse transcription, and recombination (14, 31). Many plant viruses require RNA packaging for systemic spread and for cell-to-cell movement (3, 10). Therefore, the CP-RNA interaction is a critical event in the viral life cycle. Compared with the characterization of trans-acting factors such as CP in RNA packaging, however, the RNA elements involved in specific packaging have not been well characterized for many viruses. One of the best-characterized RNA elements is "origin of assembly" of tobacco mosaic virus (36, 40). cis-acting sequences for RNA packaging have also been demonstrated in several icosahedral viruses, including flock house virus (39), Sindbis virus (37), hepatitis B virus (17), the human immunodeficiency viruses (2,14,22), and turnip crinkle virus (32).Brome mosaic virus (BMV) is an icosahedral plant RNA virus and is the type member of the genus Bromovirus in the family Bromoviridae in the alphavirus-like superfamily (18). The genome of BMV consists of three species of messenger sense single-stranded RNA (1). RNA1 (3.2 kb) and RNA2 (2.9 kb), which encode the 1a and 2a replicase proteins, respectively (1, 13, 19), are packaged separately into individual particles (21). RNA3 (2.1 kb), which encodes the 3a cell-to-cell movement protein (35), is packaged into a single particle together with subgenomic RNA4 (0.9 kb) (21). RNA4 is synthesized from the minus strand of RNA3 (25) and encodes CP. CP is required for packaging, cell-to-cell movement, and the systemic spread of the virus (29,33,34).A highly conserved N-terminal arginine-rich motif in BMV CP plays an important role in BMV RNA packaging through RNA-CP interactions (4,5,33,34). The crystallographic structure of BMV virions has been determined (23). RNA regions or elements involved in the packaging of BMV RNAs have been assigned to the coding region of BMV RNA1 by UV cross-linking and band-shift assays (11) as well as to the 3Ј-proximal region of the 3a open reading frame (ORF) in RNA3 (9). The tRNA-like structures (TLS) in the 3Ј-untranslated regions of BMV RNAs also play a crucial role in BMV RNA packaging in vitro (6). In the present study, we delimit a nucleotide sequence required for the efficient packaging of BMV RNA3 and show that 69 nucleotides (nt) in the 3Ј-proximal region of the BMV 3a ORF, especially a predicted stem-loop structure (30 nt), is essential fo...

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“…Moreover, BMV 1a protein must interact with the intercistronic region of BMV RNA 3 for efficient amplification of RNA 3 Sullivan & Ahlquist, 1999). Recent studies have identified sequences in the CP and viral RNAs that are required for bromovirus encapsidation (Choi et al, 2002;Damayanti et al, 2002). However, the interactions between bromovirus components required for movement have not been examined closely.…”

Section: Introductionmentioning

confidence: 99%

Use of Spring beauty latent virus to identify compatible interactions between bromovirus components required for virus infection

Fujisaki

Kaido

Mise

et al. 2003

Journal of General Virology

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Spring beauty latent virus (SBLV) is a member of the genus Bromovirus, and is closely related to Brome mosaic virus (BMV) and Cowpea chlorotic mottle virus (CCMV). Compatible interactions between viral components are required for successful infection of plants by BMV and CCMV. To further our understanding of interactions between bromovirus components, we used SBLV to produce reassortants among the three bromoviruses. We found that SBLV RNA 2 functioned with heterologous bromovirus RNA 1 in infections of whole plants and protoplasts of Nicotiana benthamiana, although SBLV RNA 1 did not function with heterologous bromovirus RNA 2. A DNA-based transient assay for 1a and 2a proteins, which are encoded by RNAs 1 and 2, respectively further suggested that SBLV 2a protein may function in combination with heterologous bromovirus 1a protein. Moreover, analysis of the ability of reassortants to spread locally revealed that an RNA 2-mediated interaction between viral components may be required for efficient cell-tocell movement of bromoviruses.

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tRNA elements mediate the assembly of an icosahedral RNA virus

Cited by 100 publications

References 40 publications

Deletion of Highly Conserved Arginine-Rich RNA Binding Motif in Cowpea Chlorotic Mottle Virus Capsid Protein Results in Virion Structural Alterations and RNA Packaging Constraints

Deletion of Highly Conserved Arginine-Rich RNA Binding Motif in Cowpea Chlorotic Mottle Virus Capsid Protein Results in Virion Structural Alterations and RNA Packaging Constraints

cis -Acting Elements Required for Efficient Packaging of Brome Mosaic Virus RNA3 in Barley Protoplasts

Use of Spring beauty latent virus to identify compatible interactions between bromovirus components required for virus infection

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