Author:
Ginsberg D,Vairo G,Chittenden T,Xiao Z X,Xu G,Wydner K L,DeCaprio J A,Lawrence J B,Livingston D M
Abstract
The E2F family of transcription factors has been implicated in the regulation of cell proliferation, and E2F-binding sites are present in the promoters of several growth-regulating genes. E2F family members are functionally regulated, in part, by complex formation with one or more members of the nuclear pocket protein family, RB, p107, and p130. Pocket protein regulation of E2F likely contributes to normal cellular growth control. While the three cloned species of E2F, E2F-1, E2F-2, and E2F-3, are known to be targets of RB interaction, no E2F species has yet been shown to be a specific p107 or p130 target. Here, we describe the cloning of a new member of the E2F family, E2F-4, which forms heterodimers with a member(s) of the DP family and, unlike some family members, is present throughout the cell cycle and appears to be a differentially phosphorylated p107-binding partner. p107 binding not only can be linked to the regulation of E2F-4 transcriptional activity, but also to suppression of the ability of E2F-4 to transform an immortalized rodent cell line.
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
Reference64 articles.
1. Ausubel, F.M., R. Brent, R.E. Kingston, D.D. Moore, J.G. Seidman, J.A. Smith, and K. Struhl. 1987. Current protocols in molecular biology. John Wiley/Greene, New York.
2. The retinoblastoma protein copurifies with E2F-I, an E1A-regulated inhibitor of the transcription factor E2F
3. Functional synergy between DP-1 and E2F-1 in the cell cycle regulating transcription factor DRTF1/E2F.;EMBO J.,1993
4. Functional antagonism between c-Jun and MyoD proteins: A direct physical association
5. Transcription factor E2F is required for efficient expression of the hamster dihydrofolate reductase gene in vitro and in vivo.;Mol. Cell. Biol.,1989
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