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(Received for publication, July 8, 1994; and in revised form, October 12, 1994) The role of nucleotides in activated RNA polymerase II
transcription was studied. Permanganate footprinting confirmed that
there is a strict nucleotide requirement for forming open promoter
complexes that cannot be overcome by the addition of a dinucleotide
primer corresponding to the start site sequence. However, higher
concentrations of other nucleoside triphosphates can substitute for ATP
in catalyzing open complex formation. Opening catalyzed by these
nucleotides is inhibited by the ATP analogue adenosine
5`-O-(thiotriphosphate), suggesting that they may function
through cross-binding to the ATP site. The K
Volume 270,
Number 3,
Issue of January 20, 1995 pp. 1277-1281
©1995 by The American Society for Biochemistry and Molecular Biology, Inc.
for ATP for opening and the involvement of other nucleotides
in opening differs from the characteristics reported for TFIIH helicase
and C-terminal domain kinase activities. This raises the possibility
that opening does not involve these activities. The results alleviate
very significantly the considerable current uncertainty concerning the
role of ATP in the mammalian mRNA transcription initiation pathway.
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