posted on 2016-01-19, 21:05authored byAdriana Grozav, Ovidiu Balacescu, Loredana Balacescu, Thomas Cheminel, Ioana Berindan-Neagoe, Bruno Therrien
Sixteen
hydrazinyl-thiazolo arene ruthenium complexes of the general
formula [(η6-p-cymene)Ru(N,N′-hydrazinyl-thiazolo)Cl]Cl were synthesized.
All complexes were tested in vitro for their antiproliferative
activity on three tumor cell lines (HeLa, A2780, and A2780cisR) and
on a noncancerous cell line (HFL-1). A superior cytotoxic activity
of the ruthenium complexes as compared to cisplatin and oxaliplatin,
on both cisplatin-sensitive and cisplatin resistant ovarian cancer
cells, was observed. In addition, the biological activity of two selected
derivatives was evaluated using microarray gene expression assay and
ingenuity pathway analysis. p53 signaling was identified as an important
pathway modulated by both arene ruthenium compounds. New activated
molecules such as FAS, ZMAT3, PRMT2, BBC3/PUMA, and PDCD4, whose overexpressions
are correlated with overcoming resistance to cisplatin therapy, were
also identified as potential targets. Moreover, the arene ruthenium
complexes can be used in association with cisplatin to prevent cisplatin
resistance development and synergistically to induce cell death in
ovarian cancer cells.