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SERINE-173 OF THE EPSTEIN-BARR-VIRUS ZEBRA PROTEIN IS REQUIRED FOR DNA-BINDING AND IS A TARGET FOR CASEIN KINASE-II PHOSPHORYLATION

被引:45
作者
KOLMAN, JL
TAYLOR, N
MARSHAK, DR
MILLER, G
机构
[1] YALE UNIV,DEPT MOLEC BIOPHYS & BIOCHEM,NEW HAVEN,CT 06510
[2] COLD SPRING HARBOR LAB,WM KECK STRUCT BIOL LAB,COLD SPRING HARBOR,NY 11724
[3] YALE UNIV,DEPT PEDIAT,NEW HAVEN,CT 06510
[4] YALE UNIV,DEPT EPIDEMIOL & PUBL HLTH,NEW HAVEN,CT 06510
来源
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1993年 / 90卷 / 21期
关键词
D O I
10.1073/pnas.90.21.10115
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
An Epstein-Barr virus-encoded protein, ZEBRA, mediates the switch from latency to the viral lytic life cycle. ZEBRA's domain structure and DNA binding specificity resemble that of cellular transcriptional activators such as c-Fos/c-Jun. We show that ZEBRA, like c-Jun, is phosphorylated by casein kinase II (CKII). The principal site of phosphorylation is serine-173 (S173), five amino acids upstream of the basic DNA recognition domain. CKII phosphorylation abrogated ZEBRA's capacity to bind its target DNA sequences. S173 is a functional component of ZEBRA's DNA binding domain, since mutation of S173 to alanine (S173A) reduced DNA binding in vitro to 10% of wild-type levels. Transcriptional activation of a native viral promoter in vivo by mutant S173A was also reduced markedly. Reversible phosphorylation of S173 is likely to be an important means of regulating ZEBRA's activity in vivo.
引用
收藏
页码:10115 / 10119
页数:5
相关论文
共 45 条
[1]  
ABATE C, 1991, ONCOGENE, V6, P2179
[2]  
Ausubel FM., 1995, MOL REPROD DEV, V3rd edn, DOI DOI 10.1002/MRD.1080010210
[3]   JUN IS PHOSPHORYLATED BY SEVERAL PROTEIN-KINASES AT THE SAME SITES THAT ARE MODIFIED IN SERUM-STIMULATED FIBROBLASTS [J].
BAKER, SJ ;
KERPPOLA, TK ;
LUK, D ;
VANDENBERG, MT ;
MARSHAK, DR ;
CURRAN, T ;
ABATE, C .
MOLECULAR AND CELLULAR BIOLOGY, 1992, 12 (10) :4694-4705
[4]   CHANGING EPSTEIN-BARR VIRAL ZEBRA PROTEIN INTO A MORE POWERFUL ACTIVATOR ENHANCES ITS CAPACITY TO DISRUPT LATENCY [J].
BAUMANN, R ;
GROGAN, E ;
PTASHNE, M ;
MILLER, G .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (10) :4436-4440
[5]   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
[6]   MYC AND MAX ASSOCIATE INVIVO [J].
BLACKWOOD, EM ;
LUSCHER, B ;
EISENMAN, RN .
GENES & DEVELOPMENT, 1992, 6 (01) :71-80
[7]   TRANSCRIPTIONAL SYNERGY BY THE EPSTEIN-BARR-VIRUS TRANSACTIVATOR ZEBRA [J].
CAREY, M ;
KOLMAN, J ;
KATZ, DA ;
GRADOVILLE, L ;
BARBERIS, L ;
MILLER, G .
JOURNAL OF VIROLOGY, 1992, 66 (08) :4803-4813
[8]  
CARROLL D, 1989, J BIOL CHEM, V264, P7345
[9]   REGULATING CELL-GROWTH - CASEIN-KINASE-II-DEPENDENT PHOSPHORYLATION OF NUCLEAR ONCOPROTEINS [J].
CARROLL, D ;
SANTORO, N ;
MARSHAK, DR .
COLD SPRING HARBOR SYMPOSIA ON QUANTITATIVE BIOLOGY, 1988, 53 :91-95
[10]   BOTH EPSTEIN-BARR-VIRUS (EBV)-ENCODED TRANS-ACTING FACTORS, EB1 AND EB2, ARE REQUIRED TO ACTIVATE TRANSCRIPTION FROM AN EBV EARLY PROMOTER [J].
CHEVALLIERGRECO, A ;
MANET, E ;
CHAVRIER, P ;
MOSNIER, C ;
DAILLIE, J ;
SERGEANT, A .
EMBO JOURNAL, 1986, 5 (12) :3243-3249
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