Reverse transcription in hepatitis B viruses is primed by a tyrosine residue of the polymerase.

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J Virol. 1994 January; 68(1): 6-13

Reverse transcription in hepatitis B viruses is primed by a tyrosine residue of the polymerase.

F Zoulim and C Seeger

Institute for Cancer Research, Fox Chase Cancer Center, Philadelphia, Pennsylvania 19111.

ABSTRACT

All known DNA polymerases require primers for the initiationof DNA synthesis. While cellular polymerases and reverse transcriptasesuse free hydroxyl groups of RNA or DNA, the DNA polymerasesof certain animal viruses and bacteriophages depend upon hydroxylgroups of amino acid residues within proteins as primers forDNA synthesis. Recently, the reverse transcriptase of a hepadnavirushas been shown to prime RNA-directed DNA synthesis from an internalsite of the polypeptide (G.H. Wang and C. Seeger, Cell 71:663-670,1992). In this report we demonstrate that a tyrosine residueof the polymerase polypeptide is the site of a phosphodiesterlinkage with the first nucleotide of minus-strand DNA. Thistyrosine residue is located within an amino-terminal domainof the polymerase polypeptide and is indispensable for the primingof reverse transcription. Our results demonstrate that the hepatitisB virus reverse transcriptase can initiate DNA synthesis withoutthe requirement for tRNA as a primer.

J Virol. 1994 January; 68(1): 6-13

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