Survival of colorectal cancer cell lines treated with paclitaxel, radiation, and 5‐FU: Effect of TP53 or hMLH1 deficiency

Abstract Clonogenic survival and early cell death during treatment of human colon carcinoma cells were investigated following X‐irradiation (IR) alone, IR followed by 5‐FU for 24 h, and Taxol administered 24 h before IR and 5F‐U. The investigated cell lines were: HCT116, 40‐16 clonally derived from HCT116, and two HCT116 variants: N6CHR3 expressing hMLH1 , and TP53 null cells denoted HCT116 p53‐/‐. The objective was to determine efficacy of the combined treatment and to correlate response with constitutive levels of TP53, WAF1, and hMLH1 proteins, as well as with mRNA levels of the apoptosis‐related genes survivin, BNIP3 , and MYC . At the end of treatment with 5‐FU, the proportion of viable cells was between 0.65 and 0.70 for all cell lines. Additional cell loss occurred in 40‐16 and HCT116 p53‐/‐ cells following administration of Taxol before IR and 5‐FU. Radiation sensitivity was unaffected by combined treatments, except for Taxol, irradiation, and 5‐FU sequence in the HCT116 p53‐/‐ and 40‐16 cell lines, where radiation sensitivity determined by clonogenic survival curve slopes was doubled or quadrupled, respectively. Under our present experimental conditions, treatment response did not correlate with TP53 or hMLH1 status, but was associated with apoptosis‐related genes, most notably BNIP3 . Int. J. Cancer (Radiat. Oncol. Invest.) 90, 175–185 (2000). © 2000 Wiley‐Liss, Inc.