A complete protocol for the synthesis of new palladacyclopentadienyl complexes with purine‐ based carbenes as supporting ligands is described. The new organometallic compounds were exhaustively characterized using NMR and infrared spectroscopies and elemental analysis. The single‐ crystal X‐ ray structure of complex 2b coordinating also a triphenylphosphine was resolved. Some of these complexes showed an antiproliferative activity comparable to or better than that of cisplatin on two human ovarian cancer lines: A2780 (cisplatin‐ sensitive) and A2780cis (cisplatin‐ resistant). Moreover, for complexes 2 and 3 (coordinating one purine‐ based N‐ heterocyclic carbene ligand and one phosphine) the cytotoxicity is associated with an evident induction of apoptosis. Finally, complexes 3 , bearing one purine‐ based N‐ heterocyclic carbene ligand and one 1,3,5‐ triaza‐ 7‐ phosphaadamantane, proved practically inactive on non‐ tumour fibroblast cells (MRC‐ 5).

Palladacyclopentadienyl complexes bearing purine-based N-heterocyclic carbenes: A new class of promising antiproliferative agents against human ovarian cancer

Scattolin T.;Bergamini P.;Canovese L.;Rizzolio F.;Visentin F.
2019-01-01

Abstract

A complete protocol for the synthesis of new palladacyclopentadienyl complexes with purine‐ based carbenes as supporting ligands is described. The new organometallic compounds were exhaustively characterized using NMR and infrared spectroscopies and elemental analysis. The single‐ crystal X‐ ray structure of complex 2b coordinating also a triphenylphosphine was resolved. Some of these complexes showed an antiproliferative activity comparable to or better than that of cisplatin on two human ovarian cancer lines: A2780 (cisplatin‐ sensitive) and A2780cis (cisplatin‐ resistant). Moreover, for complexes 2 and 3 (coordinating one purine‐ based N‐ heterocyclic carbene ligand and one phosphine) the cytotoxicity is associated with an evident induction of apoptosis. Finally, complexes 3 , bearing one purine‐ based N‐ heterocyclic carbene ligand and one 1,3,5‐ triaza‐ 7‐ phosphaadamantane, proved practically inactive on non‐ tumour fibroblast cells (MRC‐ 5).
2019
33
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10278/3718649
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