Walter Reiser scite author profile

To study the replication strategy of the human hepatitis B virus, the 5' end of the RNA pregenome and the initiation sites of DNA plus and minus strands have been mapped. The RNA pregenome was found to be terminally redundant by 120 nucleotides; it is initiated within the pre-C region and may also function as mRNA for synthesis of the major core protein and the hepatitis B virus reverse transcriptase. The hepatitis B virus DNA minus strand is initiated within the direct repeat sequence DR1, it contains a terminal redundancy of up to eight nucleotides, and its synthesis does not require any template switch. The DNA plus strand is primed by a short oligoribonucleotide probably derived from the 5' end of the RNA pregenome, and its synthesis is initiated close to the direct repeat sequence DR2. For its elongation to pass the discontinuity in the DNA minus strand an intramolecular template switch occurs using the terminal redundancy of this template. Thus, the route of reverse transcription and DNA replication of hepatitis B viruses is fundamentally different from that of retroviruses.

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Transcripts and the putative RNA pregenome of duck hepatitis B virus: Implications for reverse transcription

Büscher¹,

Reiser²,

Will³

et al. 1985

Cell

140

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Structure of the carbohydrate moiety of human interferon-beta secreted by a recombinant Chinese hamster ovary cell line.

Conradt¹,

Egge²,

Peter‐Katalinić³

et al. 1987

Journal of Biological Chemistry

104

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Structure and function of mutants in the P gene of bacteriophage λ leading to the π phenotype

1983

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The location of 14 independently isolated spontaneous pi A and pi B point mutants in the lambda P gene and their base exchanges were determined. It was found that the pi B mutation is one unique type mapping close to other pi A mutants. The number of possible pi A mutation sites could be estimated. The mutation sites are distributed asymmetrically in the gene. The N-terminal half of the protein is unchanged. It is assumed to be required for the interaction with the lambda O protein. The P protein can be changed by substitution of a limited number of amino acids at the C-terminus. All functional proteins of this type have pi character. pi proteins do not appear to have altered intracellular levels or stabilities as compared to wild-type P protein. The plating characteristics of our mutants on two groP- mutants located in the dnaJ and dnaK genes, respectively, are strikingly different.

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Cloning of the replication gene O of E. coli bacteriophage lambda and its expression under the control of the lac promoter

Kuypers

Reiser

Klein

1980

Gene

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Walter Reiser

Replication strategy of human hepatitis B virus

Transcripts and the putative RNA pregenome of duck hepatitis B virus: Implications for reverse transcription

Structure of the carbohydrate moiety of human interferon-beta secreted by a recombinant Chinese hamster ovary cell line.

Structure and function of mutants in the P gene of bacteriophage λ leading to the π phenotype

Cloning of the replication gene O of E. coli bacteriophage lambda and its expression under the control of the lac promoter

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