The cyclin box and C-terminus of cyclins A and E specify CDK activation and substrate specificity

被引：33

作者：

Horton, LE

Templeton, DJ

机构：

[1] CASE WESTERN RESERVE UNIV,SCH MED,INST PATHOL,CLEVELAND,OH 44106

[2] CASE WESTERN RESERVE UNIV,SCH MED,CELL BIOL PROGRAM,CLEVELAND,OH 44106

来源：

ONCOGENE | 1997年 / 14卷 / 04期

关键词：

cell cycle; cyclins; cyclin dependent kinase; lamin B;

D O I：

10.1038/sj.onc.1200851

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The cyclins and their catalytic partners, the Cyclin Dependent Kinases (CDKs), are essential for progression through the cell cycle. Cyclin/kinase complexes containing cyclins A or E are active primarily in Late G(1) to S phase and both have been shown to phosphorylate histone H1 and the retinoblastoma gene product (pRb) in vitro. Despite these similarities, cyclins A and E display differences in CDK activation and substrate specificity. We find that in vitro, cyclin E/CDK2 and cyclin A/CDK2 phosphorylate histone H1 similarly but only cyclin A/CDK2 phosphorylates lamin B. While both cyclin A and cyclin E bind CDK1 efficiently, only cyclin A activates CDK1 kinase activity. Using chimeric proteins between cyclins A and E we find that both the cyclin box and C-terminus of cyclins A and E are required for CDK binding, activation and targeting of substrate specificity.

引用

收藏

页码：491 / 498

页数：8

相关论文

共 47 条

[1] CRYSTAL-STRUCTURE OF CYCLIN-DEPENDENT KINASE-2 [J].

DEBONDT, HL ;

ROSENBLATT, J ;

JANCARIK, J ;

JONES, HD ;

MORGAN, DO ;

KIM, SH .

NATURE, 1993, 363 (6430) :595-602

[2] EFFECTS OF PHOSPHORYLATION BY CAK ON CYCLIN BINDING BY CDC2 AND CDK2 [J].

DESAI, D ;

WESSLING, HC ;

FISHER, RP ;

MORGAN, DO .

MOLECULAR AND CELLULAR BIOLOGY, 1995, 15 (01) :345-350

[3] CDC2 PHOSPHORYLATION IS REQUIRED FOR ITS INTERACTION WITH CYCLIN [J].

DUCOMMUN, B ;

BRAMBILLA, P ;

FELIX, MA ;

FRANZA, BR ;

KARSENTI, E ;

DRAETTA, G .

EMBO JOURNAL, 1991, 10 (11) :3311-3319

[4] ASSOCIATION OF HUMAN CYCLIN-E WITH A PERIODIC G(1)-S PHASE PROTEIN-KINASE [J].

DULIC, V ;

LEES, E ;

REED, SI .

SCIENCE, 1992, 257 (5078) :1958-1961

[5] DIFFERENTIAL REGULATION OF E2F TRANSACTIVATION BY CYCLIN CDK2 COMPLEXES [J].

DYNLACHT, BD ;

FLORES, O ;

LEES, JA ;

HARLOW, E .

GENES & DEVELOPMENT, 1994, 8 (15) :1772-1786

[6] A NEW HUMAN P34 PROTEIN-KINASE, CDK2, IDENTIFIED BY COMPLEMENTATION OF A CDC28 MUTATION IN SACCHAROMYCES-CEREVISIAE, IS A HOMOLOG OF XENOPUS-EG1 [J].

ELLEDGE, SJ ;

SPOTTSWOOD, MR .

EMBO JOURNAL, 1991, 10 (09) :2653-2659

[7] CDK2 ENCODES A 33-KDA CYCLIN-A-ASSOCIATED PROTEIN-KINASE AND IS EXPRESSED BEFORE CDC2 IN THE CELL-CYCLE [J].

ELLEDGE, SJ ;

RICHMAN, R ;

HALL, FL ;

WILLIAMS, RT ;

LODGSON, N ;

HARPER, JW .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (07) :2907-2911

[8] CAP-INDEPENDENT TRANSLATION OF MESSENGER-RNA CONFERRED BY ENCEPHALOMYOCARDITIS VIRUS 5' SEQUENCE IMPROVES THE PERFORMANCE OF THE VACCINIA VIRUS BACTERIOPHAGE-T7 HYBRID EXPRESSION SYSTEM [J].

ELROYSTEIN, O ;

FUERST, TR ;

MOSS, B .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (16) :6126-6130

[9] FUNCTIONAL INTERACTIONS OF THE RETINOBLASTOMA PROTEIN WITH MAMMALIAN D-TYPE CYCLINS [J].

EWEN, ME ;

SLUSS, HK ;

SHERR, CJ ;

MATSUSHIME, H ;

KATO, JY ;

LIVINGSTON, DM .

CELL, 1993, 73 (03) :487-497

[10] EVIDENCE THAT THE G1-S AND G2-M TRANSITIONS ARE CONTROLLED BY DIFFERENT CDC2 PROTEINS IN HIGHER EUKARYOTES [J].

FANG, F ;

NEWPORT, JW .

CELL, 1991, 66 (04) :731-742

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