Role of the SUMO-interacting motif in HIPK2 targeting to the PML nuclear bodies and regulation of p53
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- 作者:Ki Sa Sunga ; Yun-Ah Leea ; Eui Tae Kimb ; Seung-Rock Leec ; Jin-Hyun Ahnb ; Cheol Yong Choia ; choicy@skku.ac.kr
- 关键词:HIPK2 ; PML ; SUMO-interaction motif ; p53 phosphorylation
- 刊名:Experimental Cell Research
- 出版年:2011
- 出版时间:15 April 2011
- 年:2011
- 卷:317
- 期:7
- 页码:1060-1070
- 全文大小:1615 K
文摘
Homeodomain-interacting protein kinase 2 (HIPK2) is a key regulator of various transcription factors including p53 and CtBP in the DNA damage signaling pathway. PML-nuclear body (NB) is required for HIPK2-mediated p53 phosphorylation at Ser46 and induction of apoptosis. Although PML-NB targeting of HIPK2 has been shown, much is not clear about the molecular mechanism of HIPK2 recruitment to PML-NBs. Here we show that HIPK2 colocalizes specifically with PML-I and PML-IV. Mutational analysis showed that HIPK2 recruitment to PML-IV-NBs is mediated by the SUMO-interaction motifs (SIMs) of both PML-IV and HIPK2. Wild-type HIPK2 associated with SUMO-conjugated PML-IV at a higher affinity than with un-conjugated PML-IV, while the association of a HIPK2 SIM mutant with SUMO-modified PML-IV was impaired. In colony formation assays, HIPK2 strongly suppressed cell proliferation, but HIPK2 SIM mutants did not. In addition, activation and phosphorylation of p53 at the Ser46 residue were impaired by HIPK2 SIM mutants. These results suggest that SIM-mediated HIPK2 targeting to PML-NBs is crucial for HIPK2-mediated p53 activation and induction of apoptosis.