BÖSKEN, Christian A., Lucas FARNUNG, Corinna HINTERMAIR, Miriam Merzel SCHACHTER, Karin VOGEL- BACHMAYR, Dalibor BLAŽEK, Kanchan ANAND, Robert P. FISHER, Dirk EICK a Matthias GEYER. The structure and substrate specificity of human Cdk12/Cyclin K. NATURE COMMUNICATIONS. London: Nature Publishing Group, 2014, roč. 5, č. 3505, s. "nestránkováno", 14 s. ISSN 2041-1723. Dostupné z: https://dx.doi.org/10.1038/ncomms4505. |
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@article{1186174, author = {Bösken, Christian A. and Farnung, Lucas and Hintermair, Corinna and Schachter, Miriam Merzel and Vogeland Bachmayr, Karin and Blažek, Dalibor and Anand, Kanchan and Fisher, Robert P. and Eick, Dirk and Geyer, Matthias}, article_location = {London}, article_number = {3505}, doi = {http://dx.doi.org/10.1038/ncomms4505}, keywords = {RNA-POLYMERASE-II; C-TERMINAL DOMAIN; CAPPING ENZYME RECRUITMENT; CYCLIN-DEPENDENT KINASE-9; CTD CODE; P-TEFB; PROTEIN-KINASES; FISSION YEAST; CRYSTAL-STRUCTURE; IN-VIVO}, language = {eng}, issn = {2041-1723}, journal = {NATURE COMMUNICATIONS}, title = {The structure and substrate specificity of human Cdk12/Cyclin K}, url = {http://www.nature.com/ncomms/2014/140324/ncomms4505/pdf/ncomms4505.pdf}, volume = {5}, year = {2014} }
TY - JOUR ID - 1186174 AU - Bösken, Christian A. - Farnung, Lucas - Hintermair, Corinna - Schachter, Miriam Merzel - Vogel- Bachmayr, Karin - Blažek, Dalibor - Anand, Kanchan - Fisher, Robert P. - Eick, Dirk - Geyer, Matthias PY - 2014 TI - The structure and substrate specificity of human Cdk12/Cyclin K JF - NATURE COMMUNICATIONS VL - 5 IS - 3505 SP - "nestránkováno" EP - "nestránkováno" PB - Nature Publishing Group SN - 20411723 KW - RNA-POLYMERASE-II KW - C-TERMINAL DOMAIN KW - CAPPING ENZYME RECRUITMENT KW - CYCLIN-DEPENDENT KINASE-9 KW - CTD CODE KW - P-TEFB KW - PROTEIN-KINASES KW - FISSION YEAST KW - CRYSTAL-STRUCTURE KW - IN-VIVO UR - http://www.nature.com/ncomms/2014/140324/ncomms4505/pdf/ncomms4505.pdf L2 - http://www.nature.com/ncomms/2014/140324/ncomms4505/pdf/ncomms4505.pdf N2 - Phosphorylation of the RNA polymerase II C-terminal domain (CTD) by cyclin-dependent kinases is important for productive transcription. Here we determine the crystal structure of Cdk12/CycK and analyse its requirements for substrate recognition. Active Cdk12/CycK is arranged in an open conformation similar to that of Cdk9/CycT but different from those of cell cycle kinases. Cdk12 contains a C-terminal extension that folds onto the N- and C-terminal lobes thereby contacting the ATP ribose. The interaction is mediated by an HE motif followed by a polybasic cluster that is conserved in transcriptional CDKs. Cdk12/CycK showed the highest activity on a CTD substrate prephosphorylated at position Ser7, whereas the common Lys7 substitution was not recognized. Flavopiridol is most potent towards Cdk12 but was still 10-fold more potent towards Cdk9. T-loop phosphorylation of Cdk12 required coexpression with a Cdk-activating kinase. These results suggest the regulation of Pol II elongation by a relay of transcriptionally active CTD kinases. ER -
BÖSKEN, Christian A., Lucas FARNUNG, Corinna HINTERMAIR, Miriam Merzel SCHACHTER, Karin VOGEL- BACHMAYR, Dalibor BLAŽEK, Kanchan ANAND, Robert P. FISHER, Dirk EICK a Matthias GEYER. The structure and substrate specificity of human Cdk12/Cyclin K. \textit{NATURE COMMUNICATIONS}. London: Nature Publishing Group, 2014, roč.~5, č.~3505, s.~''nestránkováno'', 14 s. ISSN~2041-1723. Dostupné z: https://dx.doi.org/10.1038/ncomms4505.
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