6533b826fe1ef96bd12842f5

RESEARCH PRODUCT

BODIPY - phosphane - gold complexes : towards the elaboration of optical theranostics

subject

description

This work describes new anticancer agents that could be detected by optical imaging, namely optical theranostics.After a first chapter describing the context of cancer imaging and therapy, a second chapter describes a first series of BODIPY-phosphine-gold theranostics, the synthesis of which has been optimized (less steps, shortening the reaction time, scale up). Their conjugation with biomolecules (glucose, peptide) has been achieved by developing a simple and efficient method that leads to the coupling between the gold atom of the probe and the thiol of the biomolecule (modified or not), leading to a gold sulfur bound. Hence, it makes the biovectorization of the probes possible in order to get selectivity against tumor cells compared with healthy cells. Subsequent photophysical and biological studies demonstrated the potential of such theranostics, such as in vitro monitoring, and the impact of a chosen biomolecule (vector).A third chapter presents two additional series of theranostics and precursors with two distinct objectives aimed at making the probe more suitable for in vivo optical imaging. A first structural modification of the BODIPY platform was achieved upon introducing chemical groups allowing an extention of the π conjugation. It leads to BODIPYs that absorb and emit in the « therapeutic window » (650 900 nm, NIR). Preliminary in vivo studies and preliminary photoacoustic imaging studies with such compounds led to promising results. A second structural modification upon introducing bulky groups on each face of the probe was aimed at preventing stacking of BODIPYs platforms in biological media (a phenomenon known to affect their optical properties). Hence, a porphyrin « Picket Fence » approach was successfully transposed to BODIPY together with the concept of atropisomery and atropisomer interconversion.