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Virology 5.1, 2014. RNA Virus Gene Expression and Replication Issues, Problems, Strategies for ss + RNA Viruses. Terms and definitions. Replication Replicase (old name) RdRp Transcriptase (old name) Initiation/termination codons Cistron ORF Cis and trans RF and RI (see cartoon). -.
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Virology 5.1, 2014 RNA Virus Gene Expression and Replication Issues, Problems, Strategies for ss+ RNA Viruses
Terms and definitions Replication Replicase (old name) RdRp Transcriptase (old name) Initiation/termination codons Cistron ORF Cis and trans RF and RI (see cartoon)
- + A Cartoon of the Replication of + Viral RNA - - + + + * * Synthesis of Minus-Strand Intermediates By RDRP Synthesis of Plus-Strand Progeny RNAs Synthesis of Minus-Strand By RDRP * * * or * * - - + * + - + + Genomic RNA (+ssRNA) Replicative Form RF Replicative Intermediate Replicative Intermediate RI Intermediates are double-stranded RNAs; Asymmetrical copying of RNA intermediates occurs.
Plus-Strand RNA Viruses • Viruses with this genome strategy have been found in both prokaryotes and eukaryotes. They are among the most abundant plant and animal viruses. • Three different supergroups of plus strand viruses have been identified based on the phylogeny of their RNA dependent RNA polymerases (RdRP). • Supergroup 1: include picornaviruses and comoviruses that express their genomes as polyproteins that are cleaved into individual functional viral proteins. • Supergroup 2 viruses include flavi and tombus viruses whose RNAs are not capped and 3’ encoded ORFs are expressed from subgenomic mRNAs. • Supergroup 3 viruses are monopartite, bipartite and tripartite viruses whose RNAs are capped and 3’ encoded ORFs expressed from sg RNAs.
General challenges for these viruses RNA viruses must encode many of their own enzymes but Genetic Economy is still in force. Viruses must accommodate the realities of the host cell environment. Nonconventional methods for gene expression and regulation. More specific challenges Preferential initiation of translation Expression of internal genes Regulation: timing and fine tuning
Studies of TMV Provide Some Answers Strains of TMV infect tomato and cause poor yield, distorted fruits, delayed fruit ripening and various fruit discoloration problems that affect market values.
Diagram of TMV RNA Suggests Some Strategies The TMV genome is a messenger-sense RNA that produces 4 proteins during virus infection. The RNA possesses a 7mG cap structure at the 5’-end and a tRNA-like structure charged with the amino acid histidine (His) at the 3’-end. Two polymerase-related proteins are produced. One protein possesses methyltransferase (MET, capping enzyme) and RNA helicase (HEL) domains. A second protein also contains an RNA-dependent RNA polymerase (RdRp) domain. Two other proteins, movement protein (MP) and capsid protein (CP), are produced from the viral RNA
Initiation of Translation-TMV RNA • Initiation complex assembles at 5’ end • Ribosome strips away capsid proteins as it translates • Cotranslational disassembly
Cap and UTRs Boost Translation of TMV RNAdRP • The Omega () sequence in the 5’ untranslated region (UTR) of TMV RNA consists of 68 NT with 8 CAA repeats. 35S Promoter-driven plasmid • Both the 5’ sequence and a pseudoknot in the 3' UTR region increase the stabilty of synthetic mRNAs and translation of GUS or LUC reporter genes in plant and animal cells. • The sequence, the 3’ UTR and the p102 host protein interact synergistically to enhance translation. • These results fit a model for translation of circular mRNAs.
MP 183K CCA CP 126K Expression of 5’ TMV Genes AUG UAG UAG • The 126K and 183K RDRP protein subunits are expressed by direct translation of the infecting genomic RNA. • Most of the ribosomes expressing the 126K subunit fall off of the mRNA when they reach the (UAG) termination codon. • A small proportion (~5%) of the ribosomes continue synthesis of protein to produce the 183K translational readthrough protein. The stop codon is “leaky” due to a suppressor tRNA for Tyrosine • The 183K protein contains the 126K protein but also has a C- terminal extension. • Both proteins must be translated before viral RNA replication can begin-and the amounts of each protein must be regulated.
The TMV Replicase is a Multifunctional Protein Methyl- transferase domain 3’-tRNA-like binding Polymerase domain Helicase UAG MP 183K CCA CP 126K • The TMV 126/183K protein is a multifunctional enzyme with several domains. • The RdRP binds very strongly to the 3’ tRNA-like structure on the plus strand genomic RNA • The RdRP also binds to an ordered structure at the 3’ end of the minus strand of the replicating RNA. • The 126K & 183K subunits interact as heterodimers to form RdRP complexes. • 126K also has VSR activity
The MP and CP ORFs at the 3’ end of TMV RNA are expressed from subgenomic mRNAs MP TMV gRNA 183K CCA CP 126K • The 3’ ORFs on the TMV genes are not expressed from the genomic RNA. • Three subgenomic mRNAs (I1, I2 & LMC) are copied from the full length minus strand • The I1 sgRNA is present in very low amounts and no protein has been detected. • The 30K MP is translated from the I2 sgRNA but the CP ORF is not translated. • The 17K CP is translated from the LMC sgRNA. I1 RNA Function is unknown MP 54K CCA I1-RNA CP MP CCA I2-RNA CP sg-mRNAs CCA LMC RNA CP
What Strategies Does TMV Use? Initiation: 126 K, 183K, MP, CP Internal cistrons: 183 K, MP, CP Fine tuning: 126 K, 183K, MP, CP Genetic Economy?
RNA 1 RNA 2 RNA 3 + 4 BROME MOSAIC VIRUS • • BMV particles are Icosahedra consisting of 180 coat protein subunits. • • Type member of the Bromovirus genus, family Bromoviridae. • • Virions are nonenveloped icosahedral (T=3), 26 nm in diameter, contain 22% nucleic acid and 78% protein. • • The BMV genome consists of three positive sense RNAs. RNA1 (3.2 kb) & RNA2 (2.9 kb), are encapsidated in separate particles. RNA3 (2.1 kb) & RNA4 (0.9 kb) are located in a third spherical particle.
tRNA-like Helicase Subunit 5’ m7G 3.2 kB 3’ Polymerase Subunit 2.9 kB 5’ m7G 3’ Movement Coat 5’ m7G 2.1 kB 3’ Coat Brome Mosaic Virus RNAs 0.9 kB 5’ m7G 3’ P Divided RNA Genome of Brome Mosaic Virus Viruses with divided genomes can efficiently express genes needed early in infection & can regulate the timing and amounts of late genes by synthesis of sgRNAs. Brome mosaic virus is a tripartite RNA virus. Four proteins are expressed from three genomic RNAs RNA 1 encodes the helicase subunit of the RDRP. RNA 2 encodes the polymerase subunit of the RDRP. RNA 3 is bicistronic and encodes the movement protein and the coat protein. Ribosomes initiate at the 5’ m7G Cap of RNAs 1, 2 and 3 but can not initiate internally on RNA 3. RNA 4 is a sg mRNA translated from an internal promoter on the minus strand of RNA 3.
5’ Leader Sequence Genomic length (-) RNA (+) Viral RNA Jump Coronaviruses Use Another Mechanism for sg mRNA Synthesis Subgenomic mRNAs
TMV and Similar Viruses of Eukaryotes Provide Examples of Important Themes 1) UTR’s contain regulatory elements. 2) Viral mRNAs usually have some resemblance to cellular mRNAs. 3) Viruses often have overlapping genes and readthrough. 4) Subgenomic mRNAs are strategies for expression of “internal” genes. 5) Replication and expression are linked! 6) Multifunctional proteins save space!