Structural heterogeneity in the intrinsically disordered RNA polymerase II C-terminal domain

被引:0
作者
Bede Portz
Feiyue Lu
Eric B. Gibbs
Joshua E. Mayfield
M. Rachel Mehaffey
Yan Jessie Zhang
Jennifer S. Brodbelt
Scott A. Showalter
David S. Gilmour
机构
[1] Center for Eukaryotic Gene Regulation,Department of Biochemistry and Molecular Biology
[2] The Pennsylvania State University,Department of Chemistry
[3] University Park,Department of Molecular Biosciences
[4] The Huck Institutes of Life Sciences. The Pennsylvania State University,Department of Chemistry
[5] University Park,undefined
[6] The Pennsylvania State University,undefined
[7] University of Texas,undefined
[8] University of Texas,undefined
[9] Institute for Cellular and Molecular Biology,undefined
[10] University of Texas,undefined
来源
Nature Communications | / 8卷
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摘要
RNA polymerase II contains a repetitive, intrinsically disordered, C-terminal domain (CTD) composed of heptads of the consensus sequence YSPTSPS. The CTD is heavily phosphorylated and serves as a scaffold, interacting with factors involved in transcription initiation, elongation and termination, RNA processing and chromatin modification. Despite being a nexus of eukaryotic gene regulation, the structure of the CTD and the structural implications of phosphorylation are poorly understood. Here we present a biophysical and biochemical interrogation of the structure of the full length CTD of Drosophila melanogaster, which we conclude is a compact random coil. Surprisingly, we find that the repetitive CTD is structurally heterogeneous. Phosphorylation causes increases in radius, protein accessibility and stiffness, without disrupting local structural heterogeneity. Additionally, we show the human CTD is also structurally heterogeneous and able to substitute for the D. melanogaster CTD in supporting fly development to adulthood. This finding implicates conserved structural organization, not a precise array of heptad motifs, as important to CTD function.
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