The compound (4b) with 6-chloro substitution was found to be active and showed selective influence on non-small cell lung cancer, renal cancer and leukemia cancer cell lines with % growth of −44.72%, 43.03, 44.81 and % GI of 141.68%, 54.68, 52.87 respectively, and compound (4h), (4i), (4j) exhibited excellent anti-inflammatory activity with % inhibition 94%, 89%, 89% respectively. From newly synthesized heterocyclic compounds (4b), (4c), (4f) were selected and tested by in vitro
anticancer activity in the NCI Developmental Therapeutics Program against panel of sixty human cancer cell lines, among CX-5461 this the 6-chloro substitution (4b) revealed selective influence on non-small cell lung cancer (NCI-H522) as well as showed potent in-vitro anti-inflammatory activity results. It was observed that chloro substituted amino benzothiazoles were found to have encouraging sensitivity to cancer cell lines compared to others. Benzothiazole ring containing electron withdrawing groups Cl, F, OCH3 INCB024360 nmr and heterocyclic rings like piperazine, pyrimidine, exhibit promising anticancer, anti-inflammatory activity. Among all the compounds
tested, 6-nitro substitution on benzothiazole showed excellent in-vitro anti-inflammatory activity while 6-chloro, 5-chloro, 6-fluoro and 6-bromo substitution showed moderate anti-inflammatory activity compared to the standard Diclofenac, hence anti-inflammatory inhibitors proved as promising anticancer agents. Present work can be a rich source for exploitation as anticancer
and anti-inflammatory agents. All authors have none to declare. The authors would like to thank USA National Cancer Institute (Harold Varmus, MD NCI; Bethesda) for screening anticancer activity, S.A.I.F. Punjab University Chandigarh for providing MASS and 1H NMR Spectrophotometer Facility And JPR Solutions for partial funding to publish this article. “
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