Bimetallic titanocene-gold phosphane complexes inhibit invasion, metastasis, and angiogenesis-associated signaling molecules in renal cancer

Elie, Benelita T.; Fernández-Gallardo, Jacob; Curado, Natalia; Cornejo, Mike; Ramos, Joe W.; Contel, Marı́a

doi:10.1016/j.ejmech.2018.10.034

Cited by 50 publications

(74 citation statements)

References 83 publications

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“…An intriguing approach to exploit the distinct cytotoxic mechanism of action of Ti(IV) and Au(I) is synergizing their activity in the form of heterometallic compounds [115][116][117][118][119][120][121][122]. These compounds build off of the titanocene structure.…”

Section: Fusing the Auranofin And Titanocene Moieties To Create A Bimmentioning

confidence: 99%

Evaluating Ligand Modifications of the Titanocene and Auranofin Moieties for the Development of More Potent Anticancer Drugs

et al. 2020

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Over time platinum-based anticancer drugs have dominated the market, but their side effects significantly impact the quality of life of patients. Alternative treatments are being developed all over the world. The titanocene and auranofin families of compounds, discovered through an empirical search for other metal-based therapeutics, hold tremendous promise to improve the outcomes of cancer treatment. Herein we present a historical perspective of these compounds and review current efforts focused on the evolution of their ligands to improve their physiological solution stability, cancer selectivity, and antiproliferative performance, guided by a clear understanding of the coordination chemistry and aqueous speciation of the metal ions, of the cytotoxic mechanism of action of the compounds, and the external factors that limit their therapeutic potential. Newer members of these families of compounds and their combination in novel bimetallic complexes are the result of years of scientific research. We believe that this review can have a positive impact in the development and understanding of the metal-based drugs of gold, titanium, and beyond.

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Section: Fusing the Auranofin And Titanocene Moieties To Create A Bimmentioning

confidence: 99%

Evaluating Ligand Modifications of the Titanocene and Auranofin Moieties for the Development of More Potent Anticancer Drugs

et al. 2020

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“…Unexpectedly, NAMI‐A yielded less antimetastatic activity than Ru8 , suppressing the gap closure with 19.0 % at 32 μ m , which was comparable with the activity of Ru8 at 4 μ m (Figure 4 B). To eliminate the influence of cytotoxicity, the wound‐healing assay was further performed at low drug concentrations (e.g., IC 10 and IC 20 , Table S4) [31] . Encouragingly, Ru8 remained active against migration as compared to untreated cells.…”

Section: Resultsmentioning

confidence: 99%

“…To eliminate the influence of cytotoxicity,the wound-healing assayw as further performed at low drug concentrations (e.g.,I C 10 and IC 20 ,T able S4). [31] En- couragingly, Ru8 remained active against migration as compared to untreated cells. However, at the concentrations of IC 10 or IC 20 ,N AMI-A failed to inhibit the gap closure in the cells (Figure S30).…”

Section: In Vitro Antimetastatic Activitymentioning

confidence: 93%

New Organometallic Ruthenium(II) Compounds Synergistically Show Cytotoxic, Antimetastatic and Antiangiogenic Activities for the Treatment of Metastatic Cancer

Wang

Jin

Shu

et al. 2020

Chemistry A European J

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In this study,w en ewly designed ands ynthesized as mall library of ten structurally relatedC ,N-cyclometalated ruthenium(II) complexes containing various pyridine-functionalized NHC ligand and chelating bipyridyl ligands(e.g., 2,2'-bipyridine, 5,5'-dimethyl-2,2'-bipyridine, and 1,10-phenanthroline(phen)). The complexes were well characterized by NMR, electrosprayi onization-mass spectrometry,a nd single-crystal X-ray structurea nalyses. Among the new ruthenium(II) derivatives, we identified that the complex Ru8 bearing bulky moieties(i.e.,phen and pentamethyl benzene) had the most potent cytotoxicity against all tested cancer cell lines, generating dose-and cell line-dependent IC 50 values at the range of 3.3-15.0 mm.M ore significantly, Ru8 not only efficiently inhibited the metastasis process against invasiona nd migration of tumor cells but also exhibited potent antivascular effects by suppressing HUVECc ellsm igration andt ube formationi nv itro and blockingv essel generation in vivo (chicken chorioallantoic membrane model). In am etastatic A2780 tumor xenograft-bearing mouse model, administration of Ru8 outperformed antimetastatic agent NAMI-Aa nd clinically approved cisplatin in terms of antitumor efficacy and inhibition of metastases to other organs. Overall,t hese data provided compellinge vidence that the new cyclometalated ruthenium complex Ru8 is an attractive agent because of synergistically suppressing bulky tumors and metastasized tumor nudes. Therefore, the complex Ru8 deserves furtherinvestigations.

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“…The incorporation of the PEt 3 auxiliary ligand was motivated by the activity observed for the Au‐PEt 3 fragment of Auranofin. Extensive in vitro studies revealed that both 98 and 104 (Figure ), inhibit cell migration, proliferation and angiogenesis, as well as the inhibition of TrxR and VEGF (vascular endothelial growth factor) …”

Section: Goldmentioning

confidence: 99%

Heterometallic Multinuclear Complexes as Anti‐Cancer Agents‐An Overview of Recent Developments

2019

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This review provides a critical assessment of the advances made in the development of heterometallic multinuclear complexes as potential chemotherapeutic agents, with the aim of providing a starting point for future investigators. The combination of the classical transition metals (Pt, Ru and Au) with other metal moieties has the potential to result in complexes with improved pharmacokinetic and pharmacodynamic properties. This enables selective targeting of the bio- [a] 3434 Figure 2. The Pt II -Ru III complexes, IT127 and AH-197, [35] and the macrocyclic rectangles investigated by Chi and colleagues. [36] The IC 50 (μM) values reported are shown below the chemical structures.

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Bimetallic titanocene-gold phosphane complexes inhibit invasion, metastasis, and angiogenesis-associated signaling molecules in renal cancer

Cited by 50 publications

References 83 publications

Evaluating Ligand Modifications of the Titanocene and Auranofin Moieties for the Development of More Potent Anticancer Drugs

Evaluating Ligand Modifications of the Titanocene and Auranofin Moieties for the Development of More Potent Anticancer Drugs

New Organometallic Ruthenium(II) Compounds Synergistically Show Cytotoxic, Antimetastatic and Antiangiogenic Activities for the Treatment of Metastatic Cancer

Heterometallic Multinuclear Complexes as Anti‐Cancer Agents‐An Overview of Recent Developments

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