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Literature DB >> 2778874

A system for studying the selective encapsidation of hepadnavirus RNA.

Abstract

All hepadnaviruses produce multiple genome-length RNA species, only one of which is encapsidated into subviral core particles prior to reverse transcription. To study the encapsidation mechanism, we developed a system in which the packaging of genetically marked target genomes of duck hepatitis B virus is mediated by factors supplied from a separate (helper) plasmid that encodes encapsidation functions. In the helper plasmid, the synthesis of the viral core and polymerase proteins was driven by a simian virus 40 promoter; the RNA produced by this construct was itself inefficiently packaged and was not active as a template for reverse transcription. Cotransfection of this construct with mutant genomes bearing frameshift lesions in either core or polymerase cistrons resulted in the successful packaging and reverse transcription of the mutant genomes. This system should allow definition of both the cis- and trans-acting elements of the encapsidation pathway.

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Year: 1989 PMID： 2778874 PMCID： PMC251040 DOI： 10.1128/JVI.63.10.4257-4263.1989

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

24 in total

1. Biosynthesis of the reverse transcriptase of hepatitis B viruses involves de novo translational initiation not ribosomal frameshifting.

Authors: L J Chang; P Pryciak; D Ganem; H E Varmus
Journal: Nature Date: 1989-01-26 Impact factor: 49.962

2. Cleavage of structural proteins during the assembly of the head of bacteriophage T4.

Authors: U K Laemmli
Journal: Nature Date: 1970-08-15 Impact factor: 49.962

3. Varying the position of a retrovirus packaging sequence results in the encapsidation of both unspliced and spliced RNAs.

Authors: R Mann; D Baltimore
Journal: J Virol Date: 1985-05 Impact factor: 5.103

4. Construction of a retrovirus packaging mutant and its use to produce helper-free defective retrovirus.

Authors: R Mann; R C Mulligan; D Baltimore
Journal: Cell Date: 1983-05 Impact factor: 41.582

5. Replication of the genome of a hepatitis B--like virus by reverse transcription of an RNA intermediate.

Authors: J Summers; W S Mason
Journal: Cell Date: 1982-06 Impact factor: 41.582

Review 6. Transcription and RNA processing by the DNA tumour viruses.

Authors: E B Ziff
Journal: Nature Date: 1980-10-09 Impact factor: 49.962

7. Mapping the major transcripts of ground squirrel hepatitis virus: the presumptive template for reverse transcriptase is terminally redundant.

Authors: G H Enders; D Ganem; H Varmus
Journal: Cell Date: 1985-08 Impact factor: 41.582

8. Comparative sequence analysis of duck and human hepatitis B virus genomes.

Authors: R Sprengel; C Kuhn; H Will; H Schaller
Journal: J Med Virol Date: 1985-04 Impact factor: 2.327

9. Transcripts and the putative RNA pregenome of duck hepatitis B virus: implications for reverse transcription.

Authors: M Büscher; W Reiser; H Will; H Schaller
Journal: Cell Date: 1985-03 Impact factor: 41.582

10. Simian virus 40 early mRNA's contain multiple 5' termini upstream and downstream from a Hogness-Goldberg sequence; a shift in 5' termini during the lytic cycle is mediated by large T antigen.

Authors: P K Ghosh; P Lebowitz
Journal: J Virol Date: 1981-10 Impact factor: 5.103

18 in total

Review 1. An advance in liver-specific gene delivery.

Authors: D Ganem
Journal: Proc Natl Acad Sci U S A Date: 1999-10-12 Impact factor: 11.205

2. cis-acting sequences required for encapsidation of duck hepatitis B virus pregenomic RNA.

Authors: R C Hirsch; D D Loeb; J R Pollack; D Ganem
Journal: J Virol Date: 1991-06 Impact factor: 5.103

3. Mutations affecting hepadnavirus plus-strand DNA synthesis dissociate primer cleavage from translocation and reveal the origin of linear viral DNA.

Authors: S Staprans; D D Loeb; D Ganem
Journal: J Virol Date: 1991-03 Impact factor: 5.103

A system for studying the selective encapsidation of hepadnavirus RNA.

1. Biosynthesis of the reverse transcriptase of hepatitis B viruses involves de novo translational initiation not ribosomal frameshifting.

2. Cleavage of structural proteins during the assembly of the head of bacteriophage T4.

3. Varying the position of a retrovirus packaging sequence results in the encapsidation of both unspliced and spliced RNAs.

4. Construction of a retrovirus packaging mutant and its use to produce helper-free defective retrovirus.

5. Replication of the genome of a hepatitis B--like virus by reverse transcription of an RNA intermediate.

Review 6. Transcription and RNA processing by the DNA tumour viruses.

7. Mapping the major transcripts of ground squirrel hepatitis virus: the presumptive template for reverse transcriptase is terminally redundant.

8. Comparative sequence analysis of duck and human hepatitis B virus genomes.

9. Transcripts and the putative RNA pregenome of duck hepatitis B virus: implications for reverse transcription.

10. Simian virus 40 early mRNA's contain multiple 5' termini upstream and downstream from a Hogness-Goldberg sequence; a shift in 5' termini during the lytic cycle is mediated by large T antigen.

Review 1. An advance in liver-specific gene delivery.

2. cis-acting sequences required for encapsidation of duck hepatitis B virus pregenomic RNA.

3. Mutations affecting hepadnavirus plus-strand DNA synthesis dissociate primer cleavage from translocation and reveal the origin of linear viral DNA.

4. Pregenomic RNA encapsidation analysis of eleven missense and nonsense polymerase mutants of human hepatitis B virus.

5. Infection initiated by the RNA pregenome of a DNA virus.

6. Hsp90 is required for the activity of a hepatitis B virus reverse transcriptase.

7. An RNA stem-loop structure directs hepatitis B virus genomic RNA encapsidation.

8. Efficient duck hepatitis B virus production by an avian liver tumor cell line.

9. Enhanced replication of a hepatitis B virus mutant associated with an epidemic of fulminant hepatitis.

10. Suppression of hepatitis B virus expression and replication by hepatitis C virus core protein in HuH-7 cells.