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Identification of a BET family bromodomain/casein kinase II/TAF-containing complex as a regulator of mitotic condensin function.

Authors :
Kim, Hyun-Soo
Kim, Hyun-Soo
Mukhopadhyay, Rituparna
Rothbart, Scott B
Silva, Andrea C
Vanoosthuyse, Vincent
Radovani, Ernest
Kislinger, Thomas
Roguev, Assen
Ryan, Colm J
Xu, Jiewei
Jahari, Harlizawati
Hardwick, Kevin G
Greenblatt, Jack F
Krogan, Nevan J
Fillingham, Jeffrey S
Strahl, Brian D
Bouhassira, Eric E
Edelmann, Winfried
Keogh, Michael-Christopher
Kim, Hyun-Soo
Kim, Hyun-Soo
Mukhopadhyay, Rituparna
Rothbart, Scott B
Silva, Andrea C
Vanoosthuyse, Vincent
Radovani, Ernest
Kislinger, Thomas
Roguev, Assen
Ryan, Colm J
Xu, Jiewei
Jahari, Harlizawati
Hardwick, Kevin G
Greenblatt, Jack F
Krogan, Nevan J
Fillingham, Jeffrey S
Strahl, Brian D
Bouhassira, Eric E
Edelmann, Winfried
Keogh, Michael-Christopher
Source :
Cell reports; vol 6, iss 5, 892-905; 2211-1247
Publication Year :
2014

Abstract

Condensin is a central regulator of mitotic genome structure with mutants showing poorly condensed chromosomes and profound segregation defects. Here, we identify NCT, a complex comprising the Nrc1 BET-family tandem bromodomain protein (SPAC631.02), casein kinase II (CKII), and several TAFs, as a regulator of condensin function. We show that NCT and condensin bind similar genomic regions but only briefly colocalize during the periods of chromosome condensation and decondensation. This pattern of NCT binding at the core centromere, the region of maximal condensin enrichment, tracks the abundance of acetylated histone H4, as regulated by the Hat1-Mis16 acetyltransferase complex and recognized by the first Nrc1 bromodomain. Strikingly, mutants in NCT or Hat1-Mis16 restore the formation of segregation-competent chromosomes in cells containing defective condensin. These results are consistent with a model where NCT targets CKII to chromatin in a cell-cycle-directed manner in order to modulate the activity of condensin during chromosome condensation and decondensation.

Details

Database :
OAIster
Journal :
Cell reports; vol 6, iss 5, 892-905; 2211-1247
Notes :
application/pdf, Cell reports vol 6, iss 5, 892-905 2211-1247
Publication Type :
Electronic Resource
Accession number :
edsoai.on1377980092
Document Type :
Electronic Resource