Potentiating Effect of UVA Irradiation on Anticancer Activity of <i>Carboplatin</i> Derivatives Involving 7-Azaindoles

<div><p>The moderate-to-high <i>in vitro</i> cytotoxicity against ovarian A2780 (IC₅₀ = 4.7–14.4 μM), prostate LNCaP (IC₅₀ = 18.7–30.8 μM) and prostate PC-3 (IC₅₀ = 17.6–42.3 μM) human cancer cell lines of the platinum(II) cyclobutane-1,1'-dicarboxylato complexes [Pt(cbdc)(<i>n</i>aza)2] (<b>1–6</b>; cbdc = cyclobutane-1,1'-dicarboxylate(2-); <i>n</i>aza = halogeno-substituted 7-azaindoles), derived from the anticancer metallodrug <i>carboplatin</i>, are reported. The complexes containing the chloro- and bromo-substituted 7-azaindoles (<b>1</b>, <b>2</b>, and <b>4–6</b>) showed a significantly higher (p < 0.05) cytotoxicity against A2780 cell line as compared to <i>cisplatin</i> used as a reference drug. Addition of the non-toxic concentration (5.0 μM) of L-buthionine sulfoximine (L-BSO, an effective inhibitor of γ-glutamylcysteine synthase) markedly increases the <i>in vitro</i> cytotoxicity of the selected complex <b>3</b> against A2780 cancer cell line by a factor of about 4.4. The cytotoxicity against A2780 and LNCaP cells, as well as the DNA platination, were effectively enhanced by UVA light irradiation (λ_max = 365 nm) of the complexes, with the highest phototoxicity determined for compound <b>3</b>, resulting in a 4-fold decline in the A2780 cells viability from 25.1% to 6.1%. The ¹H NMR and ESI-MS experiments suggested that the complexes did not interact with glutathione as well as their ability to interact with guanosine monophosphate. The studies also confirmed UVA light induced the formation of the <i>cis</i> [Pt(H₂O)₂(cbdc`)(<i>n</i>aza)] intermediate, where cbdc` represents monodentate-coordinated cbdc ligand, which is thought to be responsible for the enhanced cytotoxicity. This is further supported by the results of transcription mapping experiments showing that the studied complexes preferentially form the bifunctional adducts with DNA under UVA irradiation, in contrast to the formation of the less effective monofunctional adducts in dark.</p>