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Construction and analysis of yeast RNA polymerase II CTD deletion and substitution mutations.

M L West and J L Corden
Genetics August 1, 1995 vol. 140 no. 4 1223-1233
M L West
Howard Hughes Medical Institute, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205-2185, USA.
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J L Corden
Howard Hughes Medical Institute, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205-2185, USA.
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Abstract

The carboxyl-terminal domain (CTD) of the RNA polymerase II largest subunit plays an essential but poorly understood role in transcription. The CTD is highly phosphorylated in vivo and this modification may be important in the transition from transcription initiation to elongation. We report here the development of a strategy for creating novel yeast CTDs. We have used this approach to show that the minimum viable CTD in yeast contains eight consensus (Tyr1Ser2Pro3Thr4Ser5Pro6Ser7) heptapeptide repeats. Substitution of alanine or glutamate for serines in positions two or five is lethal. In addition, changing tyrosine in position one to phenylalanine is lethal. The effects of mutations that alter potential phosphorylation sites are consistent with a requirement for CTD phosphorylation in vivo.

  • Copyright © 1995 by the Genetics Society of America
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Volume 140 Issue 4, August 1995

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Construction and analysis of yeast RNA polymerase II CTD deletion and substitution mutations.

M L West and J L Corden
Genetics August 1, 1995 vol. 140 no. 4 1223-1233
M L West
Howard Hughes Medical Institute, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205-2185, USA.
  • Find this author on Google Scholar
  • Find this author on PubMed
  • Search for this author on this site
J L Corden
Howard Hughes Medical Institute, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205-2185, USA.
  • Find this author on Google Scholar
  • Find this author on PubMed
  • Search for this author on this site
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Citation

Construction and analysis of yeast RNA polymerase II CTD deletion and substitution mutations.

M L West and J L Corden
Genetics August 1, 1995 vol. 140 no. 4 1223-1233
M L West
Howard Hughes Medical Institute, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205-2185, USA.
  • Find this author on Google Scholar
  • Find this author on PubMed
  • Search for this author on this site
J L Corden
Howard Hughes Medical Institute, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205-2185, USA.
  • Find this author on Google Scholar
  • Find this author on PubMed
  • Search for this author on this site

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