Interaction of the UV-damaged DNA-binding protein with hepatitis B virus X protein is conserved among mammalian hepadnaviruses and restricted to transactivation-proficient X-insertion mutants
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Sitterlin, D
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机构:INST PASTEUR,UNITE RECOMBINAT & EXPRESS GENET,INSERM,U163,F-75724 PARIS 15,FRANCE
Sitterlin, D
Lee, TH
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Lee, TH
Prigent, S
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Prigent, S
Tiollais, P
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Tiollais, P
Butel, JS
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Butel, JS
Transy, C
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Transy, C
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[1] INST PASTEUR,UNITE RECOMBINAT & EXPRESS GENET,INSERM,U163,F-75724 PARIS 15,FRANCE
We carried out a comparative analysis of several proposed host protein partners of the human hepatitis B virus X protein (HBx) using both the GAL-4- and the LexA-based yeast two-hybrid system. We showed that the interaction of HBx with the UV-damaged DNA-binding protein (UVDDB) is positive in both yeast systems, detectable in cotransfected human cells, conserved by rodent hepadnavirus X proteins (known to transactivate in human cells), and tightly correlated with the transactivation proficiency of X-insertion mutants. Taken together, our results strongly suggest that UVDDB is involved in X-mediated transactivation.