Cytotoxicity of copper(I) complexes containing indole‐based thiosemicarbazones and triphenylphosphine

Author:

Arockia Doss Periyanayagam12,Haribabu Jebiti3,Balakrishnan Nithya1,Swaminathan Srividya4,Pino Jose A.5,Bhuvanesh Nattamai6,Karvembu Ramasamy1ORCID

Affiliation:

1. Department of Chemistry National Institute of Technology Tiruchirappalli 620015 India

2. Department of Chemistry St. Joseph's College (Autonomous) Tiruchirappalli 620002 India

3. Faculty of Medicine University of Atacama Copayapu 485 Copiapó Chile

4. Chennai Institute of Technology (CIT) Chennai 600069 India

5. Department of Medicine School of Medicine University of Atacama Copiapó Chile

6. Department of Chemistry Texas A & M University College Station Texas 77842 United States

Abstract

AbstractThe research and development department continues searching for effective and definite anticancer medications that would help eradicate cancer. The thiosemicarbazone ligands with indole fragment were utilized to create four new copper(I) complexes. Several spectral examinations and elemental analyses validated the formation of the complexes (14). Single crystal X‐ray diffraction (XRD) also proved that complex 4 had the expected tetrahedral structure. Complexes 14 were assessed for their cytotoxic property on different cell lines such as immortalized human vascular endothelial (EAhy.926), hepatocellular carcinoma (HepG‐2), and bladder cancer (T24), and kidney epithelial normal cells extracted from an African green monkey (Vero). The complexes showed reduced toxicity towards healthy Vero cells while being active in cancer cell lines. While the standard cisplatin revealed IC50 values of 26.60 and 49.90 μM, the N‐phenyl substituted complex 3 displayed a superior cytotoxic effect with IC50 values of 13.82 and 24.93 μM towards EAhy.926 and HepG‐2 cells, respectively.

Publisher

Wiley

Subject

General Chemistry

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