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Journal of Virology, June 2000, p. 5562-5568, Vol. 74, No. 12
Department of Gene Research, The Cancer
Institute (JFCR), Toshima-ku, Tokyo 170-8455, Japan
Received 13 December 1999/Accepted 21 March 2000
Accumulated findings have indicated that hepatitis B virus (HBV)
DNA integrates into the cellular DNA of HBV-infected chronic hepatitis
tissues. The integrated sequence (IS) of HBV DNA at the virus-cell
junction is conserved in a 25-bp region which is adjacent to direct
repeat 1. A cellular protein which we purified from the nuclear extract
of HepG2 cells binds to the IS and was designated IS binding protein 3 (ISBP3). The amino acid sequence of ISBP3 was determined and found to
be identical to that of transcription initiation factor Yin and Yang 1 (YY1). An antibody against C-terminal amino acids of YY1 recognized
ISBP3 in a Western blot analysis and an electrophoretic mobility shift
assay. Furthermore, ISBP3 also interacted with Y3, which corresponds to
the YY1 binding sequence, to enhance intramolecular recombination of
polyomavirus DNA. Although YY1 is known as a transcription factor, the
IS did not exhibit any effect on the transcription of precore and
pregenome RNAs. The possible involvement of YY1 in the intramolecular
recombination of linear replicative HBV DNA has been examined (Y. Hayashi et al., unpublished data). Data suggest that YY1 is involved in
the joining reaction between HBV DNA and cellular DNA to form the virus-cell junction.
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Integrated Hepatitis B Virus DNA Preserves the
Binding Sequence of Transcription Factor Yin and Yang 1 at the
Virus-Cell Junction
*
Corresponding author. Mailing address: Department of
Gene Research, The Cancer Institute (JFCR), Kami-Ikebukuro, Toshima-ku, Tokyo 170-8455, Japan. Phone: (81) 3-5394-3813. Fax: (81) 3-5394-3902. E-mail: kkoike{at}jfcr.or.jp.
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