The cover image, by Masood Fereidoonnezhad et al., is based on the Full Paper (Benzyl isocyanide)gold(I) pyrimidine‐2‐thiolate complex: Synthesis and biological activity, DOI: . Design Credit: Eric Pipkin.
The reaction of [(Me2S)AuCl] with an equimolar amount of benzyl isocyanide (PhCH2NC) ligand led to the formation of complex [(PhCH2NC)AuCl] (1). The solid‐state structure of 1 was determined using the X‐ray diffraction method. Through a salt metathesis reaction, the chloride ligand in 1 was replaced by pyrimidine‐2‐thiolate (SpyN−) to afford the complex [(PhCH2NC)Au(η1‐S‐Spy)] (2), which was characterized spectroscopically. The cytotoxic activities of 1 and 2 were evaluated against three human cancer cell lines: ovarian carcinoma (SKOV3), lung carcinoma (A549) and breast carcinoma (MCF‐7). Complex 2 showed higher cytotoxicity than cisplatin against SKOV3 and MCF‐7 cancer cell lines. It showed a strong anti‐proliferative activity with IC50 of 7.80, 6.26 and 6.14 μM, compared with that measured for cisplatin which was 7.62, 12.36 and 11.47 μM, against A549, SKOV3 and MCF‐7 cell lines, respectively. The induction of cellular apoptosis by 2 was also studied on MCF‐7 cell line. Our results indicated that 2 could induce apoptosis in cancerous cells in a dose‐dependent manner.
Gold complexes as a new class of non-platinum antitumor drugs with prominent cytotoxic activities are presently being evaluated as potential anticancer agents.It was observed that the gold anticancer mechanism of action are through different pathways su ch as inhibition of the thioredoxinreductase (TrxR), selenium-glutathione peroxidase and gluthationereductase (GR) enzymes as well as intercalation with the DNA base pairs. Here, Molecular docking studies of Alkynyl(triphenylphosphine)gold(I) complexes, as novel anticancer gold(I) compounds were performed on three targets including TrxR, GR and DNA by means of AutoDock 4.2 to acquire the detailed molecular binding modes and binding sites for these compounds tothe above targets. The docking results indicated that the important amino acids inside the active site of the cavity that are responsible for essential interactions are Ile A52, Glu A54 and Arg B25 for TrxR andArg37, and Asn117 for GR receptors. A5, G4, G10 and C11 are among the most base pairs that involved in the interaction of these compounds to the DNA.
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