Novel mechanism for reverse transcription in hepatitis B viruses.

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J Virol. 1993 November; 67(11): 6507-6512

Novel mechanism for reverse transcription in hepatitis B viruses.

G H Wang and C Seeger

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

ABSTRACT

Reverse transcription of all retroviruses and most retroid elementsrequires tRNA as a primer for DNA synthesis. However, in hepatitisB viruses the viral polymerase itself acts as a primer for reversetranscription (G.-H. Wang and C. Seeger, Cell 71:663-670, 1992).We have now demonstrated that in order to prime DNA synthesis,the polymerase binds to an RNA hairpin, which then serves asa template for the formation of a short DNA primer that is covalentlylinked to protein. Following its synthesis, the nascent DNAstrand apparently dissociates from its template and reannealswith complementary sequences at the 3' end of the RNA genome,where DNA synthesis continues. Since this RNA hairpin also functionsas a packaging signal for viral RNA, hepadnaviruses have adopteda replication strategy that relies on the same signal for twobiochemically distinct events, RNA packaging and reverse transcription.This mechanism is without precedent among all known retroidelements and among other viruses and bacteriophages that useprotein as a primer for RNA or DNA synthesis. It could providean effective target for antiviral therapy, which is requiredfor the treatment of more than 300 million carriers of hepatitisB virus.

J Virol. 1993 November; 67(11): 6507-6512

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