High-affinity DNA Binding by the C-terminal Domain of the Transcriptional Coactivator PC4 Requires Simultaneous Interaction with Two Opposing Unpaired Strands and Results in Helix Destabilization

Overview

Journal J Mol Biol

Publisher Elsevier

Specialties Microbiology
Molecular Biology

Date 1998 Mar 26

PMID 9512709

Citations 23

Authors

S Werten

F W Langen

R van Schaik

H T Timmers

M Meisterernst

P C van der Vliet

Affiliations

Soon will be listed here.

Abstract

The general transcriptional cofactor PC4 enhances transcription from various promoters and functions with a wide range of transcriptional activators. Earlier studies have suggested that this enhancement originates mostly from stabilization of the TATA-box/TFIID/TFIIA complex by simultaneous interaction of PC4 with transactivation domains of upstream-binding factors and the basal factor TFIIA. However, the C-terminal half of the protein also has been shown to exhibit substantial ssDNA binding properties, to which as yet no clear function has been assigned. We have investigated the interaction of this domain with various DNA structures and report that high-affinity binding, characterized by an equilibrium dissociation constant in the nanomolar range, requires either a heteroduplex containing a minimum of about eight mismatches, or alternatively a single-stranded DNA molecule consisting of 16 to 20 nucleotides. Furthermore, both juxtaposed single strands of a heteroduplex are protected by the C-terminal domain of PC4 in DNase I footprinting experiments, whereas the double-stranded regions do not appear to be contacted. We conclude from these observations that the role of PC4 ssDNA binding is likely to involve simultaneous interaction with opposing strands in internally melted duplexes, or the induction of a pronounced distortion in the local structure of ssDNA that results in a similar juxtaposed arrangement of single strands. In addition, we have observed that both the PC4 C-terminal domain and the intact PC4 destabilize dsDNA and we discuss the possible involvement of PC4 in promoter opening and other strand displacement events.

Citing Articles

Human PC4 supports telomere stability and viability in cells utilizing the alternative lengthening of telomeres mechanism.

Salgado S, Abreu P, Moleirinho B, Guedes D, Larcombe L, Azzalin C EMBO Rep. 2024; 25(12):5294-5315.

PMID: 39468351 PMC: 11624207. DOI: 10.1038/s44319-024-00295-3.

An extrinsic motor directs chromatin loop formation by cohesin.

Guerin T, Barrington C, Pobegalov G, Molodtsov M, Uhlmann F EMBO J. 2024; 43(19):4173-4196.

PMID: 39160275 PMC: 11445435. DOI: 10.1038/s44318-024-00202-5.

The novel anti-CRISPR AcrIIA22 relieves DNA torsion in target plasmids and impairs SpyCas9 activity.

Forsberg K, Schmidtke D, Werther R, Uribe R, Hausman D, Sommer M PLoS Biol. 2021; 19(10):e3001428.

PMID: 34644300 PMC: 8545432. DOI: 10.1371/journal.pbio.3001428.

Antisense technology: A review.

Crooke S, Liang X, Baker B, Crooke R J Biol Chem. 2021; 296:100416.

PMID: 33600796 PMC: 8005817. DOI: 10.1016/j.jbc.2021.100416.

The large family of PC4-like domains - similar folds and functions throughout all kingdoms of life.

Janowski R, Niessing D RNA Biol. 2020; 17(9):1228-1238.

PMID: 32476604 PMC: 7549692. DOI: 10.1080/15476286.2020.1761639.