Exploiting the 4-Phenylquinazoline Scaffold for the Development of High Affinity Fluorescent Probes for the Translocator Protein (TSPO).
Ciro MiliteElisabetta BarresiEleonora Da PozzoBarbara CostaMonica VivianoAmalia PortaAnna MessereGianluca SbardellaFederico Da SettimoEttore NovellinoSandro CosconatiSabrina CastellanoSabrina TalianiClaudia MartiniPublished in: Journal of medicinal chemistry (2017)
The quinazoline class was exploited to search for a new translocator protein (TSPO) fluorescent probe endowed with improved affinity and residence time (RT). Computational studies on an "in-house" collection of quinazoline derivatives, featuring highly steric demanding groups at the amide nitrogen, suggested that, despite their molecular extension, these ligands are still easily lodged in the TSPO binding site. Binding assays supported this hypothesis, highlighting a low nanomolar/subnanomolar affinity of these ligands, together with a higher RT of the representative compound 11 with respect to our previously reported indole-based fluorescent probe. Thanks to the amenability of the amide nitrogen atom to be substituted with bulky groups, we developed quinazoline-based imaging tools by fluorescently labeling the scaffold at this position. Probes with relevant TSPO affinity, favorable spectroscopic properties, and improved RT were identified. The results from fluorescence microscopy showed that these probes specifically labeled the TSPO at the mitochondrial level in the U343 cell line.
Keyphrases
- living cells
- fluorescent probe
- pet imaging
- single molecule
- high resolution
- molecular docking
- positron emission tomography
- high throughput
- protein protein
- binding protein
- oxidative stress
- amino acid
- small molecule
- tissue engineering
- fluorescence imaging
- capillary electrophoresis
- molecular dynamics
- mass spectrometry
- quantum dots