A single point mutation in TFIIA suppresses NC2 requirement in vivo
AUTOR(ES)
Xie, Jun
FONTE
Oxford University Press
RESUMO
Negative cofactor 2 (NC2) is a dimeric histone-fold complex that represses RNA polymerase II transcription through binding to TATA-box-binding protein (TBP) and inhibition of the general transcription factors TFIIA and TFIIB. Here we study molecular mechanisms of repression by human NC2 in vivo in yeast. Yeast NC2 genes are essential and can be exchanged with human NC2. The physiologically rele– vant regions of NC2 have been determined and shown to match the histone-fold dimerization motif. A suppressor screen based upon limiting concentrations of NC2β yielded a cold-sensitive mutant in the yeast TFIIA subunit Toa1. The single point mutation in Toa1 alleviates the requirement for both subunits of NC2. Biochemical characterization indicated that mutant (mt)-Toa1 dimerizes well with Toa2; it supports specific recognition of the TATA box by TBP but forms less stable TBP–TFIIA–DNA complexes. Wild-type but not the mt-Toa1 can relieve NC2 effects in purified trans– cription systems. These data provide evidence for a dimeric NC2 complex that is in an equilibrium with TFIIA after the initial binding of TBP to promoter TATA boxes.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=305605Documentos Relacionados
- The NC2 α and β subunits play different roles in vivo
- Functional antagonism between RNA polymerase II holoenzyme and global negative regulator NC2 in vivo
- Transport of β-Galactosides in Lactobacillus plantarum NC2 †
- Yeast NC2 Associates with the RNA Polymerase II Preinitiation Complex and Selectively Affects Transcription In Vivo
- Characterization of the basal inhibitor of class II transcription NC2 from Saccharomyces cerevisiae.
