Diastereomeric Separation of Chiral fac -Tricarbonyl(iminopyridine) Rhenium(I) Complexes and Their Cytotoxicity Studies: Approach toward an Action Mechanism against Glioblastoma

Artigo Revisado por pares

Diastereomeric Separation of Chiral fac -Tricarbonyl(iminopyridine) Rhenium(I) Complexes and Their Cytotoxicity Studies: Approach toward an Action Mechanism against Glioblastoma

2022; American Chemical Society; Volume: 65; Issue: 13 Linguagem: Inglês

10.1021/acs.jmedchem.2c00561

ISSN

1520-4804

Autores

Gloria A. Suárez-Ortiz, Rodrigo Hernández-Correa, Melissa D. Morales-Moreno, Rubén A. Toscano, María Teresa Ramírez‐Apán, Armando Hernández-García, Manuel Amézquita‐Valencia, Daniela Araiza‐Olivera,

Tópico(s)

Metal-Organic Frameworks: Synthesis and Applications

Resumo

A series of new (tricarbonyl)rhenium(I) complexes were synthesized using chiral bidentate ligands (+)/(−)-iminopyridines (LR/LS). The reaction yielded a mixture of mononuclear Re(I) diastereoisomers, formulated as fac-[Br(CO)3Re(S/R)L(S/R)]. Each single diastereoisomer was isolated and fully characterized. X-ray crystallography and circular dichroism spectra verified their enantiomeric nature. The cytotoxicity of each complex was evaluated against six cancer cell lines. The effect of the two complexes on viability, proliferation, and migration was analyzed on glioblastoma cell lines (U251 and LN229). Changes in the expression of histones, apoptotic, and key signaling proteins, as well as alterations in DNA structure, were also observed. These experiments showed that the chirality associated with both metal and ligand has a strong influence on cytotoxicity.

Ver no editor

Altmetric

PlumX

Entrar

Lembrar minha senha

Receber meu e-mail de confirmação

Diastereomeric Separation of Chiral fac -Tricarbonyl(iminopyridine) Rhenium(I) Complexes and Their Cytotoxicity Studies: Approach toward an Action Mechanism against Glioblastoma