SMALL MAF PROTEINS HETERODIMERIZE WITH FOS AND MAY ACT AS COMPETITIVE REPRESSORS OF THE NF-E2 TRANSCRIPTION FACTOR

被引:0
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作者
KATAOKA, K
IGARASHI, K
ITOH, K
FUJIWARA, KT
NODA, M
YAMAMOTO, M
NISHIZAWA, M
机构
[1] JAPANESE FDN CANC RES,INST CANC,DEPT VIRAL ONCOL,TOSHIMA KU,TOKYO 170,JAPAN
[2] TOHOKU UNIV,SCH MED,AOBA KU,SENDAI,MIYAGI 98077,JAPAN
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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 maf oncogene encodes a bZip nuclear protein which recognizes sequences related to an AP-1 site either as a homodimer or as heterodimers with Fos and Jun. We describe here a novel maf-related gene, mafG, which shows extensive homology with two other maf-related genes, mafK and mafF. These three maf-related genes encode small basic-leucine zipper proteins lacking the trans-activator domain of v-Maf. Bacterially expressed small Maf proteins bind to DNA as homodimers with a sequence recognition profile that is virtually identical to that of v-Maf. As we have previously described, the three small Maf proteins also dimerize with the large subunit of NF-E2 (p45) to form an erythroid cell-specific transcription factor, NF-E2, which has distinct DNA-binding specificity. This study shows that the small Maf proteins can also dimerize among themselves and with Fos and a newly identified p45-related molecule (Ech) but not with v-Maf or Jun. Although the small Maf proteins preferentially recognize the consensus NF-E2 sequence as heterodimers with either NF-EZ p45, Ech, or Fos, these heterodimers seemed to be different in their transactivation potentials. Coexpression of Fos and small Mafs could not activate a promoter with tandem repeats of the NF-E2 site. These results raise the possibility that tissue specific gene expression and differentiation of erythroid cells are regulated by competition among Fos, NF-EZ p45, and Ech for small Maf proteins and for binding sites.
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页码:2180 / 2190
页数:11
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