Ruthenium-arene complexes bearing naphthyl-substituted 1,3-dioxoindan-2-carboxamides ligands for G-quadruplex DNA recognition.

6533b829fe1ef96bd128a347

RESEARCH PRODUCT

Ruthenium-arene complexes bearing naphthyl-substituted 1,3-dioxoindan-2-carboxamides ligands for G-quadruplex DNA recognition.

Claudia Kieler Silvia Alonso-de Castro Wolfgang Kandioller Dina Baier Luca Salassa Luca Salassa Alessio Terenzi Alessio Terenzi Stephan Mokesch Alexander Roller Bernhard K. Keppler Walter Berger Laura A. Hager

subject

Guanine Stereochemistry Cell Survival chemistry.chemical_element Antineoplastic Agents 010402 general chemistry G-quadruplex Ligands 01 natural sciences Ruthenium Inorganic Chemistry chemistry.chemical_compound Structure-Activity Relationship Coordination Complexes Pyridine Tumor Cells Cultured Humans Ruthenium Quadruplex G-quadruplex G4 DNA Cancer Metal Complexes heterocyclic compounds Cell Proliferation Dose-Response Relationship Drug Molecular Structure 010405 organic chemistry Ligand RNA Small molecule 3. Good health 0104 chemical sciences Ruthenium G-Quadruplexes chemistry Settore CHIM/03 - Chimica Generale E Inorganica Calixarenes Drug Screening Assays Antitumor DNA

description

Quadruplex nucleic acids – DNA/RNA secondary structures formed in guanine rich sequences – proved to have key roles in the biology of cancers and, as such, in recent years they emerged as promising targets for small molecules. Many reports demonstrated that metal complexes can effectively stabilize quadruplex structures, promoting telomerase inhibition, downregulation of the expression of cancer-related genes and ultimately cancer cell death. Although extensively explored as anticancer agents, studies on the ability of ruthenium arene complexes to interact with quadruplex nucleic acids are surprisingly almost unknown. Herein, we report on the synthesis and characterization of four novel Ru(II) arene complexes with 1,3-dioxoindan-2-carboxamides ligands bearing pendant naphthyl-groups designed to bind quadruplexes by both stacking and coordinating interactions. We show how improvements on the hydrolytic stability of such complexes, by substituting the chlorido leaving ligand with pyridine, have a dramatic impact on their interaction with quadruplexes and on their cytotoxicity against ovarian cancer cells.

year	journal	country	edition	language
2019-07-12	Dalton transactions (Cambridge, England : 2003)

10.1039/c9dt02078k https://pubmed.ncbi.nlm.nih.gov/31292575