4.6 Article

Ditopic Aza-Scorpiand Ligands Interact Selectively with ds-RNA and Modulate the Interaction upon Formation of Zn2+ Complexes

期刊

MOLECULES
卷 26, 期 13, 页码 -

出版社

MDPI
DOI: 10.3390/molecules26133957

关键词

aza-macrocycle; DNA and RNA duplexes; zinc complex

资金

  1. Spanish MICINN
  2. Spanish MEC
  3. FEDER funds from the European Union [PID2019-110751RB-I00, PID2019-108643GA-I00, CTQ2017-90852-REDC, RED2018-102331-T]
  4. FEDER funds from the European Union (Unidad de Excelencia Maria de Maeztu) [CEX2019-000919, FIS PI16/00504]
  5. Conselleria de Innovacion, Universidades, Ciencia y Sociedad Digital of the Generalitat Valenciana [CIDEGENT/2018/015]
  6. Conselleria de Innovacion, Universidades, Ciencia y Sociedad Digital of the Generalitat Valenciana

向作者/读者索取更多资源

This study investigates the interaction between two aza-macrocycles and DNA/RNA, showing a high selectivity for ds-RNA. The interaction with these duplexes is blocked upon Zn2+ coordination, leading to a decrease in cytotoxicity of the metal complexes compared to free ligands.
Nucleic acids are essential biomolecules in living systems and represent one of the main targets of chemists, biophysics, biologists, and nanotechnologists. New small molecules are continuously developed to target the duplex (ds) structure of DNA and, most recently, RNA to be used as therapeutics and/or biological tools. Stimuli-triggered systems can promote and hamper the interaction to biomolecules through external stimuli such as light and metal coordination. In this work, we report on the interaction with ds-DNA and ds-RNA of two aza-macrocycles able to coordinate Zn2+ metal ions and form binuclear complexes. The interaction of the aza-macrocycles and the Zn2+ metal complexes with duplex DNA and RNA was studied using UV thermal and fluorescence indicator displacement assays in combination with theoretical studies. Both ligands show a high affinity for ds-DNA/RNA and selectivity for ds-RNA. The ability to interact with these duplexes is blocked upon Zn2+ coordination, which was confirmed by the low variation in the melting temperature and poor displacement of the fluorescent dye from the ds-DNA/RNA. Cell viability assays show a decrease in the cytotoxicity of the metal complexes in comparison with the free ligands, which can be associated with the observed binding to the nucleic acids.

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