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Open AccessJournal ArticleDOI

Role of an adenovirus E2 promoter binding factor in E1A-mediated coordinate gene control

Imre Kovesdi, +2 more
- 01 Apr 1987 - 
- Vol. 84, Iss: 8, pp 2180-2184
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TLDR
It is concluded that E2F is likely to be responsible for the E1A-mediated stimulation of the E 1A gene as well as the E2 gene but is not involved in the activation of the other E1a-inducible promoters.
Abstract
A product of the adenovirus gene E1A is responsible for the stimulation of transcription from six viral promoters as well as at least two cellular promoters. We have detected a HeLa cell factor, termed E2 promoter binding factor (E2F), that appears to mediate the transcriptional stimulation of the viral E2 promoter. Competition experiments revealed that E2F did not recognize and bind to the E1B, E3, E4, or major late promoter sequences. Furthermore, three additional promoters stimulated by E1A, heat shock protein 70, beta-globin, and early simian virus 40, do not bind E2F. In contrast, the factor does recognize sequences in the E1A enhancer, and within the E1A enhancer are duplicated binding sites for E2F. Finally, a single E2F binding site from the E1A enhancer can confer increased transcription to a mouse beta-globin promoter, dependent on the action of the E1A gene product. This stimulation requires binding of E2F since methylation of the binding site, which blocks binding in vitro, reduces transcription stimulation in vivo. We, therefore, conclude that E2F is likely to be responsible for the E1A-mediated stimulation of the E1A gene as well as the E2 gene but is not involved in the activation of the other E1A-inducible promoters.

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Citations
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Journal ArticleDOI

A genomic sequencing protocol that yields a positive display of 5-methylcytosine residues in individual DNA strands.

TL;DR: A genomic sequencing method is reported that provides positive identification of 5-methylcytosine residues and yields strand-specific sequences of individual molecules in genomic DNA, which suggests that the high methylation level of single-copy sequences in sperm may be locally modulated by binding of protein factors in germ-line cells.
Journal ArticleDOI

Transcriptional regulation in mammalian cells by sequence-specific DNA binding proteins

TL;DR: This review summarizes recent studies that define structural domains for DNA binding and transcriptional activation functions in sequence-specific transcription factors in mammalian DNA binding transcription factors.
Journal ArticleDOI

The regulation of E2F by pRB-family proteins

TL;DR: The rapid growth in the size of the E2F literature hides the fact that several fundamental questions have not been fully answered, and the second section of this review details five unresolved issues that have been highlighted by recent publications.
Journal ArticleDOI

E2F: a link between the Rb tumor suppressor protein and viral oncoproteins

TL;DR: The cellular transcription factor E2F, previously identified as a component of early adenovirus transcription, has been shown to be important in cell proliferation control and appears to be a functional target for the action of the tumor suppressor protein Rb that is encoded by the retinoblastoma susceptibility gene.
References
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Journal ArticleDOI

Accurate transcription initiation by RNA polymerase II in a soluble extract from isolated mammalian nuclei

TL;DR: A procedure for preparing extracts from nuclei of human tissue culture cells that directs accurate transcription initiation in vitro from class II promoters, including tRNA and Ad 2 VA, is developed.
Journal ArticleDOI

DNA tumor viruses

John Tooze, +1 more
- 08 Feb 1982 - 
Journal ArticleDOI

Definition of essential sequences and functional equivalence of elements downstream of the adenovirus E2A and the early simian virus 40 polyadenylation sites.

TL;DR: The construction and assay of bidirectional deletion mutants in the adenovirus E2A poly(A) site indicates that there may be redundant multiple sequence elements that affect poly( A) site usage and that normal cleavage and polyadenylation could be restored at the early SV40 poly( a) site by the addition of downstream sequences from the adanov virus E2 a poly(a) site to the SV40 +5 mutant.
Journal ArticleDOI

Cellular promoters incorporated into the adenovirus genome: cell specificity of albumin and immunoglobulin expression.

TL;DR: Recombinant adenoviruses were constructed in which the viral E1A gene was deleted and the E1B promoter was replaced by the rat albumin, mouse beta-major globin, or mouse immunoglobulin heavy-chain promoter, and expression of the albumin promoter in the virus paralleled that of the cellular albumin gene.

Cellular Promoters Incorporated into theAdenovirus Genome:Cell Specificity ofAlbumin andImmunoglobulin Expression

TL;DR: For example, this paper found that cell-specific expression of albumin depends on the presence of issue-specific trans-acting factors, but thepresence of such factors alone does not suffice for amaximal rate of transcription, aconclusion that requires direct comparison within a differentiated cell of a newly introduced and pre-existing active cellgene.
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