Abstract
G-quadruplex (G4) sites in the human genome frequently colocalize with CCCTC-binding factor (CTCF)-bound sites in CpG islands (CGIs). We aimed to clarify the role of G4s in CTCF positioning. Molecular modeling data suggested direct interactions, so we performed in vitro binding assays with quadruplex-forming sequences from CGIs in the human genome. G4s bound CTCF with Kd values similar to that of the control duplex, while respective i-motifs exhibited no affinity for CTCF. Using ChIP-qPCR assays, we showed that G4-stabilizing ligands enhance CTCF occupancy at a G4-prone site in STAT3 gene. In view of the reportedly increased CTCF affinity for hypomethylated DNA, we next questioned whether G4s also facilitate CTCF recruitment to CGIs via protecting CpG sites from methylation. Bioinformatics analysis of previously published data argued against such a possibility. Finally, we questioned whether G4s facilitate CTCF recruitment by affecting chromatin structure. We showed that three architectural chromatin proteins of the high mobility group colocalize with G4s in the genome and recognize parallel-stranded or mixed-topology G4s in vitro. One of such proteins, HMGN3, contributes to the association between G4s and CTCF according to our bioinformatics analysis. These findings support both direct and indirect roles of G4s in CTCF recruitment.
Highlights
The guanine quadruplex (G4) structures play a role in DNA replication, transcription, recombination, and DNA repair [1]
We showed that CCCTC-binding factor (CTCF) binds folded G4s and consensus duplexes with comparable affinities (Figure 4)
We argue that direct contacts only partially account for CTCF recruitment to G4-prone sites
Summary
The guanine quadruplex (G4) structures play a role in DNA replication, transcription, recombination, and DNA repair [1]. G4s may contribute to epigenetic regulation [2,3] by shaping the DNA methylome [4] and by promoting Yin Yang 1-mediated [5] or CCCTC-binding factor (CTCF)-mediated [6] chromatin looping. G4-chromatin immunoprecipitation sequencing (G4-ChIP-seq) peaks show statistically significant colocalization with CTCF-bound sites [6]. The role of G4s in CTCF recruitment has not been explained so far. To other zinc-finger (ZF) transcription factors, CTCF binds DNA in a sequencespecific manner, but its cognate sites are rather diverse [7]. A motif that best distinguishes core CCGCGNGGNGGCAG [8].
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