Our previous studies showed that UTL-5g, a novel anti-inflammatory TNF-α inhibitor, enhanced the chemotherapeutic efficacy of cisplatin against HCT-15 human colon cancer cells in an animal tumor model. To extend the study, we set out to investigate 3 newly synthesized analogs of UTL-5g (UTLOH-4a, -4b, and -4c) on whether they are associated with similar biological effects. Chemosensitizing effects of UTL-5g and its 3 analogs were investigated using HCT-15 cells in vitro with increasing doses of cisplatin, carboplatin, or oxaliplatin. IC 50 of each drug was determined from the dose-response surviving curves. The antiinflammatory effects were examined by their ability to inhibit PGE 2 production in mouse RAW cells stimulated with LPS. Myelotoxicity induced by cisplatin was examined with human CFU-GM clonogenic assay. All 4 compounds significantly potentiated the cytotoxic effect of cisplatin against HCT-15 cancer cells by lowering the IC 50 values. Among them, UTL-5g appeared to be the most promising sensitizer of cisplatin and UTLOH-4b was the most potent sensitizer of carboplatin. Anti-inflammatory study showed that UTL-5g, UTLOH-4a, and -4c inhibited PGE 2 production in LPS-stimulated RAW cells. In addition, UTL-5g and UTLOH-4a enhanced the survival of CFU-GM colony counts in cultures containing cisplatin, carboplatin and oxaliplatin respectively.
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