FUNCTIONAL DOMAINS AND PHOSPHORYLATION OF THE ORPHAN RECEPTOR NUR77

被引：118

作者：

DAVIS, IJ

HAZEL, TG

CHEN, RH

BLENIS, J

LAU, LF

机构：

[1] HARVARD UNIV, SCH MED, DEPT CELLULAR & MOLEC BIOL, BOSTON, MA 02115 USA

[2] UNIV ILLINOIS, COLL MED, DEPT GENET, M-C 669, 808 S WOOD ST, CHICAGO, IL 60612 USA

来源：

MOLECULAR ENDOCRINOLOGY | 1993年 / 7卷 / 08期

关键词：

D O I：

10.1210/me.7.8.953

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Nur77 represents a unique class within the steroid receptor superfamily since its synthesis is tightly regulated by extracellular signals and it is capable of potent transactivation activity in the absence of an exogenously added ligand. In this study, we sought to dissect the functional domains regulating the activities of Nur77 by deletion mapping. We demonstrate that whereas the transactivation activity of Nur77 resides in the amino-terminal domain, the carboxy-terminal domain regulates this activity. A short deletion from the carboxy terminus eliminates transactivation activity while a further deletion restores the activity. Deletion of the domain immediately carboxyl to the zinc fingers motif eliminates both DNA binding activity and nuclear localization, thus abolishing transactivation. Nur77 is posttranslationally modified predominantly by phosphorylation, which occurs primarily at the N-terminal domain. The growth-related kinase pp90rsk, but neither the pp44mapk nor the pp70s6k, can phosphorylate recombinant Nur77 in vitro. Furthermore, we have identified a site within the region required for sequence-specific DNA binding, Ser-354, that is phosphorylated by pp90rsk in vitro; this site is also phosphorylated in vivo. The possibility that phosphorylation might affect DNA binding is discussed.

引用

页码：953 / 964

页数：12

共 44 条

[1] CLONING AND EXPRESSION OF THE MOUSE PGK-1 GENE AND THE NUCLEOTIDE-SEQUENCE OF ITS PROMOTER
ADRA, CN
BOER, PH
MCBURNEY, MW
[J]. GENE, 1987, 60 (01) : 65 - 74
[2] GROWTH-FACTORS AND MEMBRANE DEPOLARIZATION ACTIVATE DISTINCT PROGRAMS OF EARLY RESPONSE GENE-EXPRESSION - DISSOCIATION OF FOS AND JUN INDUCTION
BARTEL, DP
SHENG, M
LAU, LF
GREENBERG, ME
[J]. GENES & DEVELOPMENT, 1989, 3 (03) : 304 - 313
[3] GENE-REGULATION BY STEROID-HORMONES
BEATO, M
[J]. CELL, 1989, 56 (03) : 335 - 344
[4] BLENIS J, 1991, CANCER CELL-MON REV, V3, P445
[5] BOYLE WJ, 1991, METHOD ENZYMOL, V201, P110
[6] STEROID-RECEPTOR FAMILY - STRUCTURE AND FUNCTIONS
CARSONJURICA, MA
SCHRADER, WT
OMALLEY, BW
[J]. ENDOCRINE REVIEWS, 1990, 11 (02) : 201 - 220
[7] NUCLEAR-LOCALIZATION AND REGULATION OF ERK-ENCODED AND RSK-ENCODED PROTEIN-KINASES
CHEN, RH
SARNECKI, C
BLENIS, J
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1992, 12 (03) : 915 - 927
[8] REGULATION OF PP90RSK PHOSPHORYLATION AND S6 PHOSPHOTRANSFERASE ACTIVITY IN SWISS 3T3 CELLS BY GROWTH FACTOR-MEDIATED, PHORBOL ESTER-MEDIATED, AND CYCLIC AMP-MEDIATED SIGNAL TRANSDUCTION
CHEN, RH
CHUNG, JK
BLENIS, J
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1991, 11 (04) : 1861 - 1867
[9] RAPAMYCIN FKBP SPECIFICALLY BLOCKS GROWTH-DEPENDENT ACTIVATION OF AND SIGNALING BY THE 70 KD S6 PROTEIN-KINASES
CHUNG, J
KUO, CJ
CRABTREE, GR
BLENIS, J
[J]. CELL, 1992, 69 (07) : 1227 - 1236
[10] TRANSCRIPTIONAL ACTIVATION BY NUR77, A GROWTH FACTOR-INDUCIBLE MEMBER OF THE STEROID-HORMONE RECEPTOR SUPERFAMILY
DAVIS, IJ
HAZEL, TG
LAU, LF
[J]. MOLECULAR ENDOCRINOLOGY, 1991, 5 (06) : 854 - 859

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