Transcription activator structure reveals redox control of a replication initiation reaction†

نویسندگان

  • Cyril M. Sanders
  • Dmytro Sizov
  • Philippa R. Seavers
  • Miguel Ortiz-Lombardía
  • Alfred A. Antson
چکیده

Redox changes are one of the factors that influence cell-cycle progression and that control the processes of cellular proliferation, differentiation, senescence and apoptosis. Proteins regulated through redox-sensitive cysteines have been characterized but specific 'sulphydryl switches' in replication proteins remain to be identified. In bovine papillomavirus type-1, DNA replication begins when the viral transcription factor E2 recruits the viral initiator protein E1 to the origin of DNA replication (ori). Here we show that a novel dimerization interface in the E2 transcription activation domain is stabilized by a disulphide bond. Oxidative cross-linking via Cys57 sequesters the interaction surface between E1 and E2, preventing pre-initiation and replication initiation complex formation. Our data demonstrate that as well as a mechanism for regulating DNA binding, redox reactions can control replication by modulating the tertiary structure of critical protein factors using a specific redox sensor.

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عنوان ژورنال:

دوره 35  شماره 

صفحات  -

تاریخ انتشار 2007