The ability of a ternary complex to form over the serum response element correlates with serum inducibility of the human c-fos promoter.

Shaw PE; Schröter H; Nordheim A

doi:10.1016/0092-8674(89)90579-5

The ability of a ternary complex to form over the serum response element correlates with serum inducibility of the human c-fos promoter.

Shaw PE ¹,

Schröter H ,

Nordheim A

Affiliations

1. Zentrum für Molekulare Biologie, Universität Heidelberg, Federal Republic of Germany.
Authors
Shaw PE¹
(1 author)

ORCIDs linked to this article

Shaw PE | 0000-0002-2598-4283

Cell, 01 Feb 1989, 56(4):563-572
https://doi.org/10.1016/0092-8674(89)90579-5 PMID: 2492906

Abstract

Rapid induction of c-fos transcription by serum and phorbol esters requires the serum response element (SRE). The SRE contains a 20 bp element of interrupted dyad symmetry (DSE) that is bound by p67/SRF. We have identified a hitherto unrecognized protein with an apparent size of 62 kd. This novel component, p62, is shown to be an integral but physically separable part of a ternary complex formed with p67/SRF and the SRE. Alone, p62 fails to bind the SRE but requires DSE-bound p67/SRF and sequences both within and outside the DSE for its interaction with DNA. In vivo, the response of the c-fos promoter to serum is severely impaired by mutations that abolish ternary complex formation in vitro.

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References

Articles referenced by this article (41)

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The ability of a ternary complex to form over the serum response element correlates with serum inducibility of the human c-fos promoter.

Affiliations

Authors

ORCIDs linked to this article

Abstract

Full text links

References

Complexity of the early genetic response to growth factors in mouse fibroblasts.

Functional cooperativity between transcription factors UBF1 and SL1 mediates human ribosomal RNA synthesis.

MAT alpha 1 protein, a yeast transcription activator, binds synergistically with a second protein to a set of cell-type-specific genes.

Activation of the c-fos gene by UV and phorbol ester: different signal transduction pathways converge to the same enhancer element.

The c-Fos protein interacts with c-Jun/AP-1 to stimulate transcription of AP-1 responsive genes.

The structure and function of the fos proto-oncogene

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

Equilibria and kinetics of lac repressor-operator interactions by polyacrylamide gel electrophoresis.

A gel electrophoresis method for quantifying the binding of proteins to specific DNA regions: application to components of the Escherichia coli lactose operon regulatory system.

The c-fos serum response element responds to protein kinase C-dependent and -independent signals but not to cyclic AMP.

Citations & impact

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Citations of article over time

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Smart citations by scite.ai
Explore citation contexts and check if this article has been supported or disputed.
https://scite.ai/reports/10.1016/0092-8674(89)90579-5

Article citations

Regulating Androgen Receptor Function in Prostate Cancer: Exploring the Diversity of Post-Translational Modifications.

Gas6-Axl Signaling Induces SRF/MRTF-A Gene Transcription via MICAL2.

Differential regulation of hair cell actin cytoskeleton mediated by SRF and MRTFB.

HTLV-1 intragenic viral enhancer influences immortalization phenotype in vitro, but is dispensable for persistence and disease development in animal models.

SRF: a seriously responsible factor in cardiac development and disease.

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The ability of a ternary complex to form over the serum response element correlates with serum inducibility of the human c-fos promoter.

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Affiliations

Authors

ORCIDs linked to this article

Abstract

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References

The structure and function of the fos proto-oncogene

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