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pH-driven conformational switch between non-canonical DNA structures in a C-rich domain of EGFR promoter

Academic Article
Publication Date:
2019
abstract:
EGFR is an oncogene that encodes for a trans-membrane tyrosine kinase receptor. Its mis-regulation is associated to several human cancers that, consistently, can be treated by selective tyrosine kinase inhibitors. The proximal promoter of EGFR contains a G-rich domain located at 272 bases upstream the transcription start site. We previously proved it folds into two main interchanging G-quadruplex structures, one of parallel and one of hybrid topology. Here we present the first evidences supporting the ability of the complementary C-rich strand (EGFR-272_C) to assume an intramolecular i-Motif (iM) structure that, according to the experimental conditions (pH, presence of co-solvent and salts), can coexist with a different arrangement we referred to as a hairpin. The herein identified iM efficiently competes with the canonical pairing of the two complementary strands, indicating it as a potential novel target for anticancer therapies. A preliminary screening for potential binders identified some phenanthroline derivatives as able to target EGFR-272_C at multiple binding sites when it is folded into an iM.
Iris type:
01.01 - Articolo in rivista
Keywords:
Multidisciplinary
List of contributors:
Cristofari, Camilla; Rigo, Riccardo; Greco, Maria Laura; Ghezzo, Michele; Sissi, Claudia
Authors of the University:
RIGO RICCARDO
SISSI CLAUDIA
Handle:
https://www.research.unipd.it/handle/11577/3300870
Full Text:
https://www.research.unipd.it//retrieve/handle/11577/3300870/1128501/unpaywall-bitstream-178548403.pdf
Published in:
SCIENTIFIC REPORTS
Journal
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URL

www.nature.com/srep/index.html
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