Combination of polymorphisms within 5' and 3' untranslated regions of thymidylate synthase gene modulates survival in 5 fluorouracil-treated colorectal cancer patients

  • Authors:
    • María-Encarnación Fernández-Contreras
    • José Javier Sánchez-Hernández
    • Enrique González
    • Belén Herráez
    • Irene Domínguez
    • María Lozano
    • María-Luisa García De Paredes
    • Alberto Muñoz
    • Carlos Gamallo
  • View Affiliations

  • Published online on: January 1, 2009     https://doi.org/10.3892/ijo_00000144
  • Pages: 219-229
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Abstract

In the present study we explored the effect of three polymorphisms of the TS gene on overall and progression- free survival of colorectal cancer (CRC) patients subjected to 5FU chemotherapy. A 28 bp variable number of tandem repeats (VNTR), a G/C single nucleotide polymorphism (SNP), and a deletion of 6 bp at position 1494 were studied. The possible combined effect of these DNA polymorphisms on the clinical outcome of patients was also evaluated. A retrospective study was carried out on paraffin-embedded sections from 113 patients diagnosed of advanced CRC. TS genotyping methods were polymerase chain reaction (PCR) for VNTR and PCR, followed by restriction length fragment polymorphism (PCR-RFLP) for SNP and ins/del 6 bp. To study the combined effect of TS polymorphisms, four categories were defined accordingly to the level of expression attributed to SNP and ins/del 6 bp genotypes: C&allele 6−, C&6+/6+, G&allele6− and G&6+/6+. VNTR and ins/del 6 bp genotypes varied with tumour anatomical site: 2R/2R genotype was rare in left-sided tumours (7.0% vs. 26.3% of right-sided and 24.1% of rectal cancers; P<0.01), where the variant allele 6− was very frequent (69.0%). Instead, most patients with right-sided tumours were wild-type homozygous 6+/6+ (63.9%) (P<0.01). Heterozygous 6+/6− genotype was more frequent among tumours classified as C (50.0%) and D (76.5%) Dukes stages (P=0.05). None of the studied polymorphisms alone affected overall or progression-free survival (PFS). C&6+/6+ and G&6+/6+ combined genotypes were respectively associated to the best and worst PFS (P=0.03 when compared with each other), while combinations carrying the allele 6− determined an intermediate evolution that might be indicative of a variable response to chemotherapy. The rate of Dukes B stage tumours was unexpectedly high (59.1%) among patients with the unfavourable G&6+/6+ combination. In our study the combination of high TS expression genotypes G&6+/6+ identifies a group of high risk within CRC patients treated with 5FU.

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January 2009
Volume 34 Issue 1

Print ISSN: 1019-6439
Online ISSN:1791-2423

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Spandidos Publications style
Fernández-Contreras M, Sánchez-Hernández JJ, González E, Herráez B, Domínguez I, Lozano M, García De Paredes M, Muñoz A and Gamallo C: Combination of polymorphisms within 5' and 3' untranslated regions of thymidylate synthase gene modulates survival in 5 fluorouracil-treated colorectal cancer patients. Int J Oncol 34: 219-229, 2009
APA
Fernández-Contreras, M., Sánchez-Hernández, J.J., González, E., Herráez, B., Domínguez, I., Lozano, M. ... Gamallo, C. (2009). Combination of polymorphisms within 5' and 3' untranslated regions of thymidylate synthase gene modulates survival in 5 fluorouracil-treated colorectal cancer patients. International Journal of Oncology, 34, 219-229. https://doi.org/10.3892/ijo_00000144
MLA
Fernández-Contreras, M., Sánchez-Hernández, J. J., González, E., Herráez, B., Domínguez, I., Lozano, M., García De Paredes, M., Muñoz, A., Gamallo, C."Combination of polymorphisms within 5' and 3' untranslated regions of thymidylate synthase gene modulates survival in 5 fluorouracil-treated colorectal cancer patients". International Journal of Oncology 34.1 (2009): 219-229.
Chicago
Fernández-Contreras, M., Sánchez-Hernández, J. J., González, E., Herráez, B., Domínguez, I., Lozano, M., García De Paredes, M., Muñoz, A., Gamallo, C."Combination of polymorphisms within 5' and 3' untranslated regions of thymidylate synthase gene modulates survival in 5 fluorouracil-treated colorectal cancer patients". International Journal of Oncology 34, no. 1 (2009): 219-229. https://doi.org/10.3892/ijo_00000144