Synthesis of New Thiourea-Metal Complexes with Promising Anticancer Properties

In this work, two thiourea ligands bearing a phosphine group in one arm and in the other a phenyl group (T2) or 3,5-di-CF3 substituted phenyl ring (T1) have been prepared and their coordination to Au and Ag has been studied. A different behavior is observed for gold complexes, a linear geometry with coordination only to the phosphorus atom or an equilibrium between the linear and three-coordinated species is present, whereas for silver complexes the coordination of the ligand as P^S chelate is found. The thiourea ligands and their complexes were explored against different cancer cell lines (HeLa, A549, and Jurkat). The thiourea ligands do not exhibit relevant cytotoxicity in the tested cell lines and the coordination of a metal triggers excellent cytotoxic values in all cases. In general, data showed that gold complexes are more cytotoxic than the silver compounds with T1, in particular the complexes [AuT1(PPh3)]OTf, the bis(thiourea) [Au(T1)2]OTf and the gold-thiolate species [Au(SR)T1]. In contrast, with T2 better results are obtained with silver species [AgT1(PPh3)]OTf and the [Ag(T1)2]OTf. The role played by the ancillary ligand bound to the metal is important since it strongly affects the cytotoxic activity, being the bis(thiourea) complex the most active species. This study demonstrates that metal complexes derived from thiourea can be biologically active and these compounds are promising leads for further development as potential anticancer agents.

Significant differences between solid state and solution photochemistry and photophysics of mesogenic organometallic gold complexes

Five new gold complexes 4-ROC6H4C≡CAuN≡CC6H4-4-OR′ (R/R′ = CH3/C9H19 (C1N9 ), C15H31/C9H19 (C15N9 ), C6H13/C15H31 (C6N15 ), C9H19/C15H31 (C9N15 ), C12H25/C15H31 (C12N15 )) were synthesized and characterized (1H and 13C NMR, IR, Raman spectroscopy, and high resolution mass spectrometry). Their organized smectic phases were investigated by TGA, DSC, powder XRD, and polarized light optical microscopy, and the solids are found to have crystalline and amorphous domains. No evidence for Au•••Au interactions was observed. The steady state and time-resolved absorption and emission properties at 298 and 77 K were examined, and surprisingly, the excited lifetime of the triplet excited state in the solid state is extremely short-lived (<100 ps) in comparison with the microsecond time scale recorded for the solution and at 77 K. The photosensitization of 1O2 was observed in solution but not in the solid state. The nature of the singlet (ligand-to-ligand charge transfer) and triplet (ethynyl/intraligand ππ*) excited states were assessed using DFT and TD-DFT computations. The thermal and UV-photochemical formation of gold nanoparticles were performed in solution (slow) and in the solid state (faster). The thermally generated nanoparticles are found to be larger (2–20 nm; TEM) and exhibit well-defined shapes, whereas the photochemically generated ones are smaller (1–10 nm) and show ill-defined shapes.

An Efficient Synthesis of [n]Cycloparaphenylenes (n = 9, 12, 15) via the Self-Assembly into Macrocyclic Gold(I)-Oligophenylene Complexes Based on Dynamic Au–C σ-Bonds

The transmetalation of the digold(I) complex [Au2Cl2(Cy2PCH2PCy2)] with oligophenylene diboronic acids gave the triangu-lar macrocyclic complexes [Au2(C6H4)x(Cy2PCH2PCy2)]3 (x = 3, 4, 5) with yields of over 70%. A series of [n]cycloparaphenylenes (n = 9, 12, 15) was isolated in 78–88% yield via the oxidative chlorination of the macrocyclic gold complexes. A kinetics study employing two acyclic dinuclear gold(I) complexes, [Au2R2(Cy2PCH2PCy2)] (R = Ph and/or C6H4-4-F), revealed that an intermolecular Au(I)–C σ-bond-exchange reaction proceeded. These results indicate that the trian-gular complexes were obtained selectively via reversible intermolecular Au(I)–C σ-bond exchanges. By reacting two different oligophenylene diboronic acids with the digold(I) complex, a mixture of macrocyclic complexes incorporating different oli-gophenylene linkers was formed. The oxidative chlorination of this mixture gave [n]cycloparaphenylenes with various num-bers of phenylene units.

Gold Clusters: From the Dispute on a Gold Chair to the Golden Future of Nanostructures

The present work opens with an acknowledgement to the research activity performed by Luciana Naldini while affiliated at the Università degli Studi di Sassari (Italy), in particular towards gold complexes and clusters, as a tribute to her outstanding figure in a time and a society where being a woman in science was rather difficult, hoping her achievements could be of inspiration to young female chemists in pursuing their careers against the many hurdles they may encounter. Naldini’s findings will be a key to introduce the most recent results in this field, showing how the chemistry of gold compounds has changed throughout the years, to reach levels of complexity and elegance that were once unimagined. The study of gold complexes and clusters with various phosphine ligands was Naldini’s main field of research because of the potential application of these species in diverse research areas including electronics, catalysis, and medicine. As the conclusion of a vital period of study, here we report Naldini’s last results on a hexanuclear cationic gold cluster, [(PPh3)6Au6(OH)2]2+, having a chair conformation, and on the assumption, supported by experimental data, that it comprises two hydroxyl groups. This contribution, within the fascinating field of inorganic chemistry, provides the intuition of how a simple electron counting may lead to predictable species of yet unknown molecular architectures and formulation, nowadays suggesting interesting opportunities to tune the electronic structures of similar and higher nuclearity species thanks to new spectroscopic and analytical approaches and software facilities. After several decades since Naldini’s exceptional work, the chemistry of the gold cluster has reached a considerable degree of complexity, dealing with new, single-atom precise, materials possessing interesting physico-chemical properties, such as luminescence, chirality, or paramagnetic behavior. Here we will describe some of the most significant contributions.

N-Heterocyclic Carbene-Gold(I) Complexes Targeting Actin Polymerization

Transition metal complexes are attracting attention because of their various chemical and biological properties. In particular, the NHC-gold complexes represent a productive field of research in medicinal chemistry, mostly as anticancer tools, displaying a broad range of targets. In addition to the already known biological targets, recently, an important activity in the organization of the cell cytoskeleton was discovered. In this paper, we demonstrated that two NHC-gold complexes (namely AuL4 and AuL7) possessing good anticancer activity and multi-target properties, as stated in our previous studies, play a major role in regulating the actin polymerization, by the means of in silico and in vitro assays. Using immunofluorescence and direct enzymatic assays, we proved that both the complexes inhibited the actin polymerization reaction without promoting the depolymerization of actin filaments. Our outcomes may contribute toward deepening the knowledge of NHC-gold complexes, with the objective of producing more effective and safer drugs for treating cancer diseases.

Emerging Molecular Receptors for the Specific-Target Delivery of Ruthenium and Gold Complexes into Cancer Cells

Cisplatin and derivatives are highly effective in the treatment of a wide range of cancer types; however, these metallodrugs display low selectivity, leading to severe side effects. Additionally, their administration often results in the development of chemoresistance, which ultimately results in therapeutic failure. This scenario triggered the study of other transition metals with innovative pharmacological profiles as alternatives to platinum, ruthenium- (e.g., KP1339 and NAMI-A) and gold-based (e.g., Auranofin) complexes being among the most advanced in terms of clinical evaluation. Concerning the importance of improving the in vivo selectivity of metal complexes and the current relevance of ruthenium and gold metals, this review article aims to survey the main research efforts made in the past few years toward the design and biological evaluation of target-specific ruthenium and gold complexes. Herein, we give an overview of the inorganic and organometallic molecules conjugated to different biomolecules for targeting membrane proteins, namely cell adhesion molecules, G-protein coupled receptors, and growth factor receptors. Complexes that recognize the progesterone receptors or other targets involved in metabolic pathways such as glucose transporters are discussed as well. Finally, we describe some complexes aimed at recognizing cell organelles or compartments, mitochondria being the most explored. The few complexes addressing targeted gene therapy are also presented and discussed.