Red-Light Photocatalytic Activation of Pt(IV) Anticancer Prodrugs Using Methylene Blue

Catalysis-based approaches offer versatile strategies for activating anticancer prodrugs, potentially allowing precise control over drug release and localization within tumor tissues while reducing systemic toxicity. In this study, we explore the role of the phenothiazine dye methylene blue (MB+) as a photocatalyst in conjunction with biologically relevant electron donors to facilitate the red-light conversion of two Pt(IV) complexes, denoted as cis,cis,trans-[PtCl2 (NH 3 ) 2 (O2 CCH 2 CH 2 COOH)2 ] (1) andtrans-[Pt(O2 CCH 2 CH 2 COOH)21R,2R-(DACH)(ox)] (2), into cisplatin and oxaliplatin, respectively. Combining spectroscopic tech-niques (NMR, UV–vis, and flash photolysis) with computational methods, we reveal that the doubly reduced MB+ (becometh-lene blue, LMB) triggers the reductive elimination of axial ligands in the two Pt(IV) precursors, generating the corresponding Pt(II)anticancer drugs. In vitro experiments conducted on the human cervical cancer cell line CaSki, which harbors multiple copies sof the integrated HPV-16 genome, and on nontumoral cells(HaCat) demonstrate that coadministration with Pt(IV) prodrugs improves MB+’s antiproliferative efficacy in cancer cells, particularly under red light exposure. This enhancement could be attributed to the catalytic production of Pt(II) species within the cellular environment