Structural and functional insights into the regulation mechanism of CK2 by IP6 and the intrinsically disordered protein Nopp140

Authors
Lee, Won-KyuSon, Sang HyeonJin, Bong-SukNa, Jung-HyunKim, Soo-YoulKim, Kook-HanKim, Eunice EunKyeongYu, Yeon GyuLee, Hyung Ho
Issue Date
2013-11-26
Publisher
NATL ACAD SCIENCES
Citation
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, v.110, no.48, pp.19360 - 19365
Abstract
Protein kinase CK2 is a ubiquitous kinase that can phosphorylate hundreds of cellular proteins and plays important roles in cell growth and development. Deregulation of CK2 is related to a variety of human cancers, and CK2 is regarded as a suppressor of apoptosis; therefore, it is a target of anticancer therapy. Nucleolar phosphoprotein 140 (Nopp140), which is an intrinsically disordered protein, interacts with CK2 and inhibits the latter's catalytic activity in vitro. Interestingly, the catalytic activity of CK2 is recovered in the presence of D-myo-inositol 1,2,3,4,5,6-hexakisphosphate (IP6). IP6 is widely distributed in animal cells, but the molecular mechanisms that govern its cellular functions in animal cells have not been completely elucidated. In this study, the crystal structure of CK2 in complex with IP6 showed that the lysine-rich cluster of CK2 plays an important role in binding to IP6. The biochemical experiments revealed that a Nopp140 fragment (residues 568-596) and IP6 competitively bind to the catalytic subunit of CK2 (CK2 alpha), and phospho-Ser574 of Nopp140 significantly enhances its interaction with CK2 alpha. Substitutions of K74E, K76E, and K77E in CK2 alpha significantly reduced the interactions of CK2 alpha with both IP6 and the Nopp140-derived peptide. Our study gives an insight into the regulation of CK2. In particular, our work suggests that CK2 activity is inhibited by Nopp140 and reactivated by IP6 by competitive binding at the substrate recognition site of CK2.
Keywords
CASEIN KINASE-II; CELL-PROLIFERATION; CATALYTIC SUBUNIT; CK2-ALPHA; SURVIVAL; INOSITOL; PHOSPHORYLATION; SUPPRESSOR; EXPRESSION; DESIGN; CASEIN KINASE-II; CELL-PROLIFERATION; CATALYTIC SUBUNIT; CK2-ALPHA; SURVIVAL; INOSITOL; PHOSPHORYLATION; SUPPRESSOR; EXPRESSION; DESIGN; inositol hexakisphosphate; IDP; phosphorylation
ISSN
0027-8424
URI
https://pubs.kist.re.kr/handle/201004/127430
DOI
10.1073/pnas.1304670110
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KIST Article > 2013
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