Proteomics

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Tousled-like kinases phosphorylate Asf1 to promote histone supply during DNA replication


ABSTRACT: During DNA replication, nucleosomes are rapidly assembled on newly synthesized DNA to restore chromatin organization. Asf1, a key histone H3-H4 chaperone required for this process, is phosphorylated by Tousled-Like Kinases (TLKs). Here, we identify TLK phosphorylation sites by mass spectrometry and dissect how phosphorylation impacts on human Asf1 function. The divergent C-terminal tail of Asf1a is phosphorylated at several sites and this is required for timely progression through S phase. Consistent with this, biochemical analysis of wild-type and phospho-mimetic Asf1a shows that phosphorylation enhances binding to histones and the downstream chaperones CAF-1 and HIRA. Moreover, we find that TLK phosphorylation of Asf1a is induced in cells experiencing deficiency of new histones and that TLK interaction with Asf1a involves its histone-binding pocket. We thus propose that TLK signaling promotes histone supply in S phase by targeting histone-free Asf1 and stimulating its ability to shuttle histones to sites of chromatin assembly.

INSTRUMENT(S): LTQ Orbitrap

ORGANISM(S): Homo Sapiens (human)

SUBMITTER: Clifford Young  

LAB HEAD: Ole Nørregaard Jensen

PROVIDER: PXD000686 | Pride | 2014-03-06

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
Ob003244.RAW Raw
Ob003244.msf Msf
Ob003244.pep.xml Pepxml
Ob02496.RAW Raw
Ob02496.msf Msf
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Publications

Tousled-like kinases phosphorylate Asf1 to promote histone supply during DNA replication.

Klimovskaia Ilnaz M IM   Young Clifford C   Strømme Caroline B CB   Menard Patrice P   Jasencakova Zuzana Z   Mejlvang Jakob J   Ask Katrine K   Ploug Michael M   Nielsen Michael L ML   Jensen Ole N ON   Groth Anja A  

Nature communications 20140306


During DNA replication, nucleosomes are rapidly assembled on newly synthesized DNA to restore chromatin organization. Asf1, a key histone H3-H4 chaperone required for this process, is phosphorylated by Tousled-like kinases (TLKs). Here, we identify TLK phosphorylation sites by mass spectrometry and dissect how phosphorylation has an impact on human Asf1 function. The divergent C-terminal tail of Asf1a is phosphorylated at several sites, and this is required for timely progression through S phase  ...[more]

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