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Reactive Pt(II) center as part of redox-active quinoline-based heterocyclic scaffolds toward new anticancer leads
Date Issued
15-11-2020
Author(s)
Kumbhakonam, Sateeshkumar
Saroj, Soumya
Venkatesan, Nalini
Devarajan, Karunagaran
Manheri, Muraleedharan K.
Abstract
New cisplatin analogs in which the diamminedichloro-Pt(II) unit is conjugated to dihydroquinoline- or tetrahydroquinoline frameworks were synthesized and subjected to biological evaluation in order to understand their effects on cellular redox homeostasis and cell viability. They exhibited better selectivity towards cancer cells (A549) compared to mice fibroblast NIH3T3 cells, with cytotoxicity in the same range as that of cisplatin. There was structure-dependent variation in the levels of ROS and were also able to induce cell death, as evidenced by accumulation of cells in sub-G1 phase.
Volume
30