Abstract
The activity of a novel thymidylate synthase inhibitor, 1843U89, against WiDr human colon carcinoma multicellular tumor spheroids was investigated. Continuous exposure of the spheroids to 3 nM 1843U89 for 10 days resulted in spheroid disruption, whereas 100 nM methotrexate (MTX) was required for similar effects. Short-term treatment experiments demonstrated that a 3-day exposure to 100 nM 1843U89 caused spheroid disruption 9 days after drug removal. A 4-day exposure to 10 nM 1843U89 caused spheroid disruption 8 days after drug removal. In contrast, treatment with 10 or 100 nM 1843U89 for 6–48 h or treatment with 1 nM 1843U89 for up to 5 days caused only growth delay. Continuous exposure of spheroids to 30 nM 1843U89 in the presence of 0.05–0.3 μM thymidine was as effective in causing spheroid disruption as treatment in the absence of thymidine, but treatment in the presence of 0.7–3.0 μM thymidine caused partial reversal of spheroid disruption. The results of these experiments suggest that 1843U89 should have potent solid tumor activity in humans but should be less effective in mice due to differences in circulating thymidine levels (0.1 vs 1 μM, respectively).
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References
Sutherland RM (1988) Cell and environment interactions in tumor microregions: the multicell spheroid model. Science 240: 177–184
Petrelli N, Herrera L, Rustum Y, Burke P, Creaven P, Stulc J, Emrich LJ, Mittelman A (1987) A prospective randomized trial of 5-fluorouracil versus 5-fluorouracil and high-dose leucovorin versus 5-fluorouracil and methotrexate in previously untreated patients with advanced colorectal carcinoma. J Clin Oncol 5: 1559–1565
Newell DR, Alison DL, Calvert AH, Harrap KR, Jarman M, Jones TR, Manteuffel-Cymborowska M, O'Connor P (1986) Pharmacokinetics of the thymidylate synthase inhibitorN 10-propargyl-5,8-dideazafolic acid (CB3717) in the mouse. Cancer Treat Rep 70: 971–979
Alison DL, Newell DR, Sessa C, Harland SJ, Hart LI, Harrap KR, Calvert AH (1985) The clinical pharmacokinetics of the novel antifolateN 10-propargyl-5,8-dideazafolic acid (CB3717). Cancer Chemother Pharmacol 14: 265–271
Judson I, Clarke S, Ward J, Sutcliffe F, Planting A, Spiers J, Smith R, Verweij J (1992) Pharmacokinetics of ICI D1694 following a 15-min infusion in patients with advanced cancer. Proc 28th Annu Meet Am Soc Clin Oncol 11: 117
Pendergast W, Dickerson S, Dev I, Ferone R, Duch D, Smith G (1992) Benzoquinazoline inhibitors of thymidylate synthase: effect on cytotoxicity and thymidylate synthase activity of variation of side chain structure and C3 substitution. Proc 83rd Annu Meet Am Assoc Cancer Res 33: 407
Duch D, Banks S, Dev IK, Dickerson SH, Ferone R, Heath LS, Humphreys J, Knick V, Pendergast W, Singer S, Smith GK, Waters K, Wilson HR (1993) Biochemical and cellular pharmacology of 1843U89 a novel benzoquinazoline inhibitor of thymidylate synthase. Cancer Res 53: 810–818
Nottebrock H, Then R (1977) Thymidine concentrations in serum and urine of different animal species and man. Biochem Pharmacol 26: 2175–2179
Jackman AL, Taylor GA, Calvert AH, Harrap KR (1984) Modulation of anti-metabolite effects. Biochem Pharmacol 33: 3269–3275
Wilson HR, Heath LS, Knick VC, Koszalka GW, Ferone R (1992) In vivo antitumor activity of 1843U89, a new antifolate thymidylate synthase inhibitor. Proc 83rd Annu Meet Am Assoc Cancer Res 33: 407
Cook WJ, Koszalka GW, Hall WW, Burns CL, Ealick SE (1987) Crystallization and preliminary X-ray investigation of thymidine phosphorylase fromEscherichia coli. J Biol Chem 262: 3788–3789
Nair MG, Murthy BR, Patil SD, Kisliuk RL, Thorndike J, Gaumont Y, Ferone R, Duch DS, Edelstein MP (1989) Folate analogues. 31. Synthesis of the reduced derivatives of 11-deazahomofolic acid, 10-methyl-11-deazahomofolic acid, and their evaluation as inhibitors of glycinamide ribonucleotide formyltransferase. J Med Chem 32: 1277–1283
Sutherland RM, Durand RE (1976) Radiation effects on mammalian cells grown as an in vitro tumor model. Curr Top Radiat Res 11: 87–139
Sutherland RM, Durand RE (1984) Growth and cellular characteristics of multicell spheroids. In: Acker H, Carlsson J, Durand R, Sutherland RM (eds) Spheroids in cancer research. Springer, Berlin Heidelberg New York, pp 24–29
Jansen M, Dykstra M, Lee J, Stables J, Topley P, Knick V, Mullin RJ, Duch DS, Smith GK (1994) Effect of purine synthesis inhibition on WiDr spheroids in vitro or on WiDr or colon 38 tumors in vivo: complete growth inhibition but not regression. Biochem Pharmacol (in press)
Howell SB, Herbst K, Boss GR, Frei E III (1980) Thymidine requirements for the rescue of patients treated with high-dose methotrexate. Cancer Res 40: 1824–1829
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Banks, S.D., Waters, K.A., Barrett, L.L. et al. Destruction of WiDr multicellular tumor spheroids with the novel thymidylate synthase inhibitor 1843U89 at physiological thymidine concentrations. Cancer Chemother. Pharmacol. 33, 455–459 (1994). https://doi.org/10.1007/BF00686500
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DOI: https://doi.org/10.1007/BF00686500