Combination of SNX-2112 with 5-FU exhibits antagonistic effect in esophageal cancer cells.

[esophageal squamous cell carcinoma]

The low efficacy of single -drug chemotherapy forms the basis for combination therapy in esophageal squamous cell carcinoma . SNX-2112 , a selective heat shock protein 90 (Hsp 90 ) inhibitor , was recently reported as being effective in combination with cisplatin and paclitaxel . In this study , we investigated the effect of SNX-2112 in combination with 5 -fluorouracil (5 -FU ), another first -line anticancer drug , in esophageal cancer . Unexpectedly , tetrazolium assay revealed that the combination of SNX-2112 with 5 -FU exhibited antagonistic effect . Flow cytometry revealed that the SNX-2112 and 5 -FU combination greatly decreased the number of G 2 /M cells compared to SNX-2112 -only treatment in Eca‑109 cells . This effect might be related to the altered mRNA level of cyclin-related genes including cyclin D 1 , Chk 2 and Cdk 4 . Further , 5 -FU attenuated SNX-2112 -induced apoptosis by decreasing poly (ADP-ribose ) polymerase (PARP ) cleavage and inactivating caspase-3 , -8 and -9 . Additionally , 5 -FU suppressed the SNX-2112 -induced decrease of mitochondrial membrane potential . Moreover , 5 -FU partly recovered Hsp 90 client proteins , including Akt , p -Akt , inhibitor of κB kinase (IKK )α , extracellular signal-regulated kinase (ERK )1 /2 , and glycogen synthase kinase (GSK )-3 β , which SNX-2112 had downregulated . Taken together , this is the first report that the combination of SNX-2112 with 5 -FU exhibited antagonistic effect in esophageal cancer cells by affecting growth inhibition , cell cycle , apoptosis , and Hsp 90 client proteins , suggesting that care is required in the clinical application of combined SNX-2112 and 5 -FU .