HBV C promoter Sp1 binding sequence functionally substitutes for the yeast ARS1 ABF1 binding site

Transcriptional factors have been implicated in eukaryotic DNA replication. We have studied the potential function of a viral promoter sequence in DNA replication. The hepatitis B virus (HBV) pregenomic promoter is regulated by two enhancers and cis-elements. The G-C rich region between 1734-1754 nt...

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Veröffentlicht in:DNA and cell biology 2002-10, Vol.21 (10), p.737-742
Hauptverfasser: Yan, Peijun, Mao, Xicheng, Wang, Lei, Zha, Xiliang, Lu, Changde
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Sprache:eng
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Zusammenfassung:Transcriptional factors have been implicated in eukaryotic DNA replication. We have studied the potential function of a viral promoter sequence in DNA replication. The hepatitis B virus (HBV) pregenomic promoter is regulated by two enhancers and cis-elements. The G-C rich region between 1734-1754 nt, which contains two SP1 binding sites, is necessary for transcription origin and HBV replication. We found that the Abf1-binding B3 element in yeast ARS1 can be functionally replaced by the viral Sp1-binding DNA sequence, which activates transcription from the HBV C promoter. Further, yeast RAP1 bound to the viral Sp1 binding sites in vitro. These results suggest that RAP1 binds to the Sp1 binding sites and stimulates yeast DNA replication.
ISSN:1044-5498
1557-7430
DOI:10.1089/104454902760599717