Double-stranded flanking ends affect the folding kinetics and conformational equilibrium of G-quadruplexes forming sequences within the promoter of KIT oncogene

Author:

Vesco Guglielmo1,Lamperti Marco2ORCID,Salerno Domenico3,Marrano Claudia Adriana3,Cassina Valeria3,Rigo Riccardo4,Buglione Enrico3,Bondani Maria5,Nicoletto Giulia4,Mantegazza Francesco3ORCID,Sissi Claudia46ORCID,Nardo Luca3ORCID

Affiliation:

1. Department of Science and High Technology, University of Insubria, 22100 Como, Italy

2. Department of Physics, Polytechnic of Milan, 23900 Lecco, Italy

3. School of Medicine and Surgery, BioNanoMedicine Center NANOMIB, University of Milano-Bicocca, 20854 Vedano al Lambro (MB), Italy

4. Department of Pharmaceutical and Pharmacological Sciences, University of Padova, 35131 Padova, Italy

5. Institute for Photonics and Nanotechnology, IFN-CNR, 22100 Como, Italy

6. CRIBI Biotechnology Center, University of Padova, 35131 Padova, Italy

Abstract

Abstract G-quadruplexes embedded within promoters play a crucial role in regulating the gene expression. KIT is a widely studied oncogene, whose promoter contains three G-quadruplex forming sequences, c-kit1, c-kit2 and c-kit*. For these sequences available studies cover ensemble and single-molecule analyses, although for kit* the latter were limited to a study on a promoter domain comprising all of them. Recently, c-kit2 has been reported to fold according to a multi-step process involving folding intermediates. Here, by exploiting fluorescence resonance energy transfer, both in ensemble and at the single molecule level, we investigated the folding of expressly designed constructs in which, alike in the physiological context, either c-kit2 or c-kit* are flanked by double stranded DNA segments. To assess whether the presence of flanking ends at the borders of the G-quadruplex affects the folding, we studied under the same protocols oligonucleotides corresponding to the minimal G-quadruplex forming sequences. Data suggest that addition of flanking ends results in biasing both the final equilibrium state and the folding kinetics. A previously unconsidered aspect is thereby unravelled, which ought to be taken into account to achieve a deeper insight of the complex relationships underlying the fine tuning of the gene-regulatory properties of these fascinating DNA structures.

Funder

University of Padova

Italian Ministry of University and Research

University of Milan

Publisher

Oxford University Press (OUP)

Subject

Genetics

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