Open AccessGene Transcription Through Myc Family Members in Eukaryotic Cells
Author(s) -
Nobuyuki Kuramoto,
Kiyokazu Ogita,
Yukio Yoneda
Publication year - 1999
Publication title -
japanese journal of pharmacology/japanese journal of pharmacology
Language(s) - English
Resource type - Journals
eISSN - 1347-3506
pISSN - 0021-5198
DOI - 10.1254/jjp.80.103
Subject(s) - enhancer , dna , gene , transcription (linguistics) , biology , transcription factor , transition (genetics) , promoter , regulatory sequence , nuclear protein , dna binding protein , genetics , scaffold/matrix attachment region , microbiology and biotechnology , response element , gene expression , linguistics , philosophy , chromatin remodeling
c-Myc family proteins, encoded by c-myc family proto-oncogenes, play critical roles in mechanisms associated with proliferation, differentiation and apoptotic death in eukaryotic cells. These functions are mediated by transcriptional activity of these proteins through binding to the E-box core sequence CACGTG referred to as a Myc core element located at a promoter or enhancer region of the individual target genes in the nucleus. Recent studies have demonstrated the presence of novel nuclear proteins that specifically recognize a Myc core element, in addition to c-Myc, Max, Mad and Mxi1. On the other hand, a Myc core element has alternating purine/pyrimidine repeats which could undergo a conformational transition from right-handed (B-DNA) to left-handed (Z-DNA) forms in the presence of a high concentration of salts such as Mg2+ and polyamines. Similarly, a Myc element has a homopurine-homopyrimidine site that may take a triplex configuration in particular situations. We have searched for nuclear proteins that can specifically recognize a Myc core element in different topological variations in murine brain.