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BCL-6 is phosphorylated at multiple sites in its serine- and proline-clustered region by mitogen-activated protein kinase (MAPK) in vivo

被引:36
作者
Moriyama, M
Yamochi, T
Semba, K
Akiyama, T
Mori, S
机构
[1] UNIV TOKYO, INST MED SCI, DEPT CELLULAR & MOL BIOL, TOKYO 108, JAPAN
[2] OSAKA UNIV, INST MICROBIAL DIS, DEPT ONCOGENE RES, OSAKA 565, JAPAN
来源
ONCOGENE | 1997年 / 14卷 / 20期
关键词
BCL-6; MAP kinase; transcription factor; zinc finger; BTB/POZ; phosphorylation;
D O I
10.1038/sj.onc.1201084
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
BCL-6 gene alterations have been observed in 27-45% of diffuse large B-cell lymphomas (DLBs) with chromosomal translocations at 3q27. The deregulated expression of normal BCL-6 protein caused by this chromosomal translocation is believed to be responsible for lymphomagenesis. Recently, we demonstrated that BCL-6 is expressed at high levels in germinal center B-cells as a 92-98 kDa nuclear protein in a constitutively phosphorylated form. In this study, we show that BCL-6 is phosphorylated by mitogen-activated protein kinase (MAPK) in vitro at the sites phosphorylated in vivo. These numerous phosphorylation sites were found to be located in its serine- and proline-clustered (SPC) region (amino acids-250-483). BCL-6 phosphorylation significantly increased in Ramos cells following stimulation with 12-o-tetradecanoylphorbol-13-acetate (TPA) or BCL-6- and erk1-transfected COS-7 cells stimulated with epidermal growth factor (EGF), and the increase of phosphorylation was inhibited by MEK1 inhibitor, PD98059. Furthermore, we observed that BCL-6 was associated with MAPK in vivo and its SPC region was important for this association. These results suggest that the functions of BCL-6 are regulated by phosphorylation mediated by the MAPK signaling pathway.
引用
收藏
页码:2465 / 2474
页数:10
相关论文
共 55 条
[1]   PHOSPHORYLATION OF THE RETINOBLASTOMA PROTEIN BY CDK2 [J].
AKIYAMA, T ;
OHUCHI, T ;
SUMIDA, S ;
MATSUMOTO, K ;
TOYOSHIMA, K .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (17) :7900-7904
[2]  
ALVAREZ E, 1991, J BIOL CHEM, V266, P15277
[3]   THE POZ DOMAIN - A CONSERVED PROTEIN-PROTEIN INTERACTION MOTIF [J].
BARDWELL, VJ ;
TREISMAN, R .
GENES & DEVELOPMENT, 1994, 8 (14) :1664-1677
[4]   BCL6 ENCODES A SEQUENCE-SPECIFIC DNA-BINDING PROTEIN [J].
BARON, BW ;
STANGER, RR ;
HUME, E ;
SADHU, A ;
MICK, R ;
KERCKAERT, JP ;
DEWEINDT, C ;
BASTARD, C ;
NUCIFORA, G ;
ZELEZNIKLE, N ;
MCKEITHAN, TW .
GENES CHROMOSOMES & CANCER, 1995, 13 (03) :221-224
[5]  
BASTARD C, 1994, BLOOD, V83, P2423
[6]   CASEIN KINASE-II INHIBITS THE DNA-BINDING ACTIVITY OF MAX HOMODIMERS BUT NOT MYC MAX HETERODIMERS [J].
BERBERICH, SJ ;
COLE, MD .
GENES & DEVELOPMENT, 1992, 6 (02) :166-176
[7]  
BERNSTEIN LR, 1994, J BIOL CHEM, V269, P9401
[8]   ERKS - A FAMILY OF PROTEIN-SERINE THREONINE KINASES THAT ARE ACTIVATED AND TYROSINE PHOSPHORYLATED IN RESPONSE TO INSULIN AND NGF [J].
BOULTON, TG ;
NYE, SH ;
ROBBINS, DJ ;
IP, NY ;
RADZIEJEWSKA, E ;
MORGENBESSER, SD ;
DEPINHO, RA ;
PANAYOTATOS, N ;
COBB, MH ;
YANCOPOULOS, GD .
CELL, 1991, 65 (04) :663-675
[9]  
BOYLE WJ, 1991, METHOD ENZYMOL, V201, P110
[10]   BCL-6 PROTEIN IS EXPRESSED IN GERMINAL-CENTER B-CELLS [J].
CATTORETTI, G ;
CHANG, CC ;
CECHOVA, K ;
ZHANG, JD ;
YE, BH ;
FALINI, B ;
LOUIE, DC ;
OFFIT, K ;
CHAGANTI, RSK ;
DALLAFAVERA, R .
BLOOD, 1995, 86 (01) :45-53
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