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Small Maf proteins heterodimerize with Fos and may act as competitive repressors of the NF-E2 transcription factor.

机译:小黑手党蛋白与Fos异源二聚体,并可能充当NF-E2转录因子的竞争性阻遏物。

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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-E2 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-E2 p45, and Ech for small Maf proteins and for binding sites.
机译:maf癌基因编码一个bZip核蛋白,该蛋白识别与AP-1位点相关的序列(与Fos和Jun成为同二聚体或异二聚体)。在此我们描述了一个与maf相关的新基因mafG,该基因与另外两个maf具有广泛的同源性相关基因,mafK和mafF。这三个与maf相关的基因编码缺少v-Maf的反式激活域的小的基本亮氨酸拉链蛋白。细菌表达的小Maf蛋白以同二聚体形式与DNA结合,其序列识别谱与v-Maf几乎相同。如我们先前所述,这三个小Maf蛋白也与NF-E2的大亚基(p45)二聚形成一个类红细胞特异性转录因子NF-E2,它具有独特的DNA结合特异性。这项研究表明,小的Maf蛋白也可以在它们之间以及与Fos和新鉴定的与p45相关的分子(Ech)形成二聚体,但不能与v-Maf或Jun形成二聚体。尽管小的Maf蛋白优先识别共有的NF-E2序列为具有NF-E2 p45,Ech或Fos的异二聚体,这些异二聚体的反式激活潜能似乎不同。 Fos和小黑手党的共表达不能激活与NF-E2位点串联重复的启动子。这些结果增加了通过Fos,NF-E2 p45和Ech之间竞争小Maf蛋白和结合位点来调节红系细胞组织特异性基因表达和分化的可能性。

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