Publication | Open Access
Luminescent ruffled iridium(<scp>iii</scp>) porphyrin complexes containing N-heterocyclic carbene ligands: structures, spectroscopies and potent antitumor activities under dark and light irradiation conditions
61
Citations
86
References
2018
Year
A panel of iridium(iii) porphyrin complexes containing axial N-heterocyclic carbene (NHC) ligand(s) were synthesized and characterized. X-ray crystal structures of the bis-NHC complexes [Ir<sup>III</sup>(ttp)(IMe)<sub>2</sub>]<sup>+</sup> (<b>2a</b>), [Ir<sup>III</sup>(oep)(BIMe)<sub>2</sub>]<sup>+</sup> (<b>2d</b>), [Ir<sup>III</sup>(oep)(I <sup><i>i</i></sup> Pr)<sub>2</sub>]<sup>+</sup> (<b>2e</b>) and [Ir<sup>III</sup>(F<sub>20</sub>tpp)(IMe)<sub>2</sub>]<sup>+</sup> (<b>2f</b>) display ruffled porphyrin rings with mesocarbon displacements of 0.483-0.594 Å and long Ir-C<sub>NHC</sub> bonds of 2.100-2.152 Å. Variable-temperature <sup>1</sup>H NMR analysis of <b>2a</b> reveals that the macrocycle porphyrin ring inversion takes place in solution with an activation barrier of 40 ± 1 kJ mol<sup>-1</sup>. The UV-vis absorption spectra of Ir<sup>III</sup>(por)-NHC complexes display split Soret bands. TD-DFT calculations and resonance Raman experiments show that the higher-energy Soret band is derived from the <sup>1</sup>MLCT dπ(Ir) → π*(por) transition. The near-infrared phosphorescence of Ir<sup>III</sup>(por)-NHC complexes from the porphyrin-based <sup>3</sup>(π, π*) state features broad emission bands at 701-754 nm with low emission quantum yields and short lifetimes (<i>Φ</i> <sub>em</sub> < 0.01; <i>τ</i> < 4 μs). [Ir<sup>III</sup>(por)(IMe)<sub>2</sub>]<sup>+</sup> complexes (por = ttp and oep) are efficient photosensitizers for <sup>1</sup>O<sub>2</sub> generation (<i>Φ</i> <sub>so</sub> = 0.64 and 0.88) and are catalytically active in the light-induced aerobic oxidation of secondary amines and arylboronic acid. The bis-NHC complexes exhibit potent dark cytotoxicity towards a panel of cancer cells with IC<sub>50</sub> values at submicromolar levels. The cytotoxicity of these complexes could be further enhanced upon light irradiation with IC<sub>50</sub> values as low as nanomolar levels in association with the light-induced generation of reactive oxygen species (ROS). Bioimaging of [Ir<sup>III</sup>(oep)(IMe)<sub>2</sub>]<sup>+</sup> (<b>2c</b>) treated cells indicates that this Ir complex mainly targets the endoplasmic reticulum. [Ir<sup>III</sup>(oep)(IMe)<sub>2</sub>]<sup>+</sup> catalyzes the photoinduced generation of singlet oxygen and triggers protein oxidation, cell cycle arrest, apoptosis and the inhibition of angiogenesis. It also causes pronounced photoinduced inhibition of tumor growth in a mouse model of human cancer.
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