Illuminating cytochrome P450 binding: Ru(<scp>ii</scp>)-caged inhibitors of CYP17A1

Li, Ao; Yadav, Rahul; White, Jessica K.; Herroon, Mackenzie K.; Callahan, Brian P.; Podgorski, Izabela; Turró, Claudia; Scott, Emily E.; Kodanko, Jeremy J.

doi:10.1039/c7cc01459g

Cited by 68 publications

(71 citation statements)

References 38 publications

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“…Two sterically hindered ruthenium photocaging scaffolds were chosen based upon earlier work by the group of Turro and Kodanko: [Ru(tpy)(dmbpy)(L)] 2+ (tpy=2,2′;6′‐2′′‐terpyridine; dmbpy=6,6′‐dimethyl‐2,2′‐bipyridine) and [Ru(tpy)(biq)(L)] 2+ (biq=2,2′‐biquinoline). Both types of complexes have an absorption band that extends into the red region of the spectrum, and they photodissociate when the monodentate ligand (L) is a thioether or a pyridine moiety . These scaffolds were conjugated to 4‐[({[4‐(2‐methyl‐2‐propanyl)phenyl]sulfonyl}amino)methyl]‐ N ‐(3‐pyridinyl)benzamide (STF‐31), a known cytotoxic organic compound containing a pyridine moiety that can coordinate to ruthenium.…”

Section: Methodsmentioning

confidence: 87%

“…The almost identical EC 50 found for [ 1 ]Cl 2 in the dark and after light irradiation, and its high NAMPT inhibition in the dark, suggest that [ 1 ]Cl is thermally unstable: When followed for 48 hours at 37 °C in the dark in OptiMEM medium (Figure S8), [ 1 ] 2+ slowly decomposed to [Ru(tpy)(dmbpy)(OH 2 )] 2+ while [ 2 ] 2+ remained stable (Figure and Figure S9). This result is in contrast to Kodanko et al., who used [Ru(tpy)(dmbpy)] 2+ to cage a steroidal CYP17A1 inhibitor . According to our results, [Ru(tpy)(NN)(L)] 2+ complexes are only stable enough for PACT when NN=biq, while complexes with NN=dmbpy are more photoreactive and are also unstable in the dark …”

Section: Methodsmentioning

confidence: 99%

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A Red‐Light‐Activated Ruthenium‐Caged NAMPT Inhibitor Remains Phototoxic in Hypoxic Cancer Cells

et al. 2017

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We describe two water‐soluble ruthenium complexes, [1]Cl2 and [2]Cl2, that photodissociate to release a cytotoxic nicotinamide phosphoribosyltransferase (NAMPT) inhibitor with a low dose (21 J cm−2) of red light in an oxygen‐independent manner. Using a specific NAMPT activity assay, up to an 18‐fold increase in inhibition potency was measured upon red‐light activation of [2]Cl2, while [1]Cl2 was thermally unstable. For the first time, the dark and red‐light‐induced cytotoxicity of these photocaged compounds could be tested under hypoxia (1 % O2). In skin (A431) and lung (A549) cancer cells, a 3‐ to 4‐fold increase in cytotoxicity was found upon red‐light irradiation for [2]Cl2, whether the cells were cultured and irradiated with 1 % or 21 % O2. These results demonstrate the potential of photoactivated chemotherapy for hypoxic cancer cells, in which classical photodynamic therapy, which relies on oxygen activation, is poorly efficient.

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Section: Methodsmentioning

confidence: 87%

Section: Methodsmentioning

confidence: 99%

A Red‐Light‐Activated Ruthenium‐Caged NAMPT Inhibitor Remains Phototoxic in Hypoxic Cancer Cells

et al. 2017

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“…41 Similar PIs for PCT agents that release cytotoxic ligands and/or metal complexes have been reported. 27,29,50,56 These ndings inspired us to consider other ways of instilling hypoxic activity in Ru(II) complexes that are photostable and exploit photocatalytic pathways/mechanisms for cytotoxic effects. Our approach is to create metal complex PSs that combine powerful 1 O 2 sensitization, such that some activity can be maintained even in hypoxia, with the possibility of light-induced electron transfer reactions via triplet intraligand charge transfer ( 3 ILCT) excited states.…”

Section: Introductionmentioning

confidence: 99%

Breaking the barrier: an osmium photosensitizer with unprecedented hypoxic phototoxicity for real world photodynamic therapy

et al. 2020

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“…1–4 More recently, RPCs are being explored as light-responsive agents for photobiological applications such as photodynamic therapy (PDT)/photoactivated cancer therapy (PACT) and photochemotherapy (PCT), 5–7 and as photocaging units for precise delivery of enzyme inhibitors. 8,9 Our RPC TLD1433 is currently in a clinical trial for treating bladder cancer with PDT (ClinicalTrials.gov Identifier: NCT03053635), which is the first example of a Ru(II)-based photosensitizer that has advanced to human studies.…”

Section: Introductionmentioning

confidence: 99%

Cyclometalated Ruthenium(II) Complexes Derived from α-Oligothiophenes as Highly Selective Cytotoxic or Photocytotoxic Agents

et al. 2018

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The photophysical and photobiological properties of a new class of cyclometalated ruthenium(II) compounds incorporating π-extended benzo[ h]imidazo[4,5- f]quinoline (IBQ) cyclometalating ligands (C^N) bearing thienyl rings ( n = 1-4, compounds 1-4) were investigated. Their octanol-water partition coefficients (log P) were positive and increased with n. Their absorption and emission energies were red-shifted substantially compared to the analogous Ru(II) diimine (N^N) complexes. They displayed C^N-based intraligand (IL) fluorescence and triplet excited-state absorption that shifted to longer wavelengths with increasing n and N^N-based metal-to-ligand charge transfer (MLCT) phosphorescence that was independent of n. Their photoluminescence lifetimes (τ) ranged from 4-10 ns for IL states and 12-18 ns forMLCT states. Transient absorption lifetimes (τ) were 5-8 μs with 355 nm excitation, ascribed to IL states that became inaccessible for 1-3 with 532 nm excitation (1-3, τ = 16-17 ns); the IL of 4 only was accessible by lower energy excitation, τ = 3.8 μs. Complex 4 was nontoxic (EC > 300 μM) to SK-MEL-28 melanoma cells and CCD1064-Sk normal skin fibroblasts in the dark, while 3 was selectively cytotoxic to melanoma (EC= 5.1 μM) only. Compounds 1 and 2 were selective for melanoma cells in the dark, with submicromolar potencies (EC = 350-500 nM) and selectivity factors (SFs) around 50. The photocytotoxicities of compounds 1-4 toward melanoma cells were similar, but only compounds 3 and 4 displayed significant phototherapeutic indices (PIs; 3, 43; 4, >1100). The larger cytotoxicities for compounds 1 and 2 were attributed to increased cellular uptake and nuclear accumulation, and possibly related to the DNA-aggregating properties of all four compounds as demonstrated by cell-free gel mobility-shift assays. Together, these results demonstrate a new class of thiophene-containing Ru(II) cyclometalated compounds that contain both highly selective chemotherapeutic agents and extremely potent photocytotoxic agents.

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Illuminating cytochrome P450 binding: Ru(ii)-caged inhibitors of CYP17A1

Cited by 68 publications

References 38 publications

A Red‐Light‐Activated Ruthenium‐Caged NAMPT Inhibitor Remains Phototoxic in Hypoxic Cancer Cells

A Red‐Light‐Activated Ruthenium‐Caged NAMPT Inhibitor Remains Phototoxic in Hypoxic Cancer Cells

Breaking the barrier: an osmium photosensitizer with unprecedented hypoxic phototoxicity for real world photodynamic therapy

Cyclometalated Ruthenium(II) Complexes Derived from α-Oligothiophenes as Highly Selective Cytotoxic or Photocytotoxic Agents

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