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- Title
Tuning the Cell Uptake and Subcellular Distribution in BODIPY–Carboranyl Dyads: An Experimental and Theoretical Study.
- Authors
Labra‐Vázquez, Pablo; Flores‐Cruz, Ricardo; Galindo‐Hernández, Aylin; Cabrera‐González, Justo; Guzmán‐Cedillo, Cristian; Jiménez‐Sánchez, Arturo; Lacroix, Pascal G.; Santillan, Rosa; Farfán, Norberto; Núñez, Rosario
- Abstract
A set of BODIPY‐carboranyl dyads synthesized by a Sonogashira cross‐coupling reaction, where different C‐substituted ortho‐ and meta‐carboranyl fragments have been linked to a BODIPY fluorophore is described. Chemical, photophysical and physicochemical analyses are presented, including NMR and single XRD experiments, optical absorption/emission studies and partition coefficient (log P) measurements. These studies, supported by DFT computations (M06‐2X/6‐31G**), provide an explanation to the largely divergent cell income that these fluorescent carboranyl‐based fluorophores display, for which a structural or physicochemical explanation remains elusive. By studying the cell uptake efficiency and subcellular localization for our set of dyads on living HeLa cells, we tracked the origins of these differences to significant variations in their static dipole moments and partition coefficients, which tune their ability to interact with lipophilic microenvironments in cells. Remarkably, m‐carboranyl‐BODIPY derivatives with a higher lipophilicity are much better internalised by cells than their homologous with o‐carborane, suggesting that m‐isomers are potentially better theranostic agents for in vitro bioimaging and boron carriers for boron neutron capture therapy.
- Subjects
BORON-neutron capture therapy; PARTITION coefficient (Chemistry); DYADS; SONOGASHIRA reaction; DIPOLE moments; BIO-imaging sensors
- Publication
Chemistry - A European Journal, 2020, Vol 26, Issue 69, p16530
- ISSN
0947-6539
- Publication type
Academic Journal
- DOI
10.1002/chem.202002600