Hereditary Cancer in Clinical Practice (Oct 2012)

Absence of the RET+3:T allele in the MTC patients

  • Borun Pawel,
  • Jerzy Sowinski,
  • Ziemnicka Katarzyna,
  • Kubaszewski Lukasz,
  • Lipinski Daniel,
  • Plawski Andrzej

DOI
https://doi.org/10.1186/1897-4287-10-14
Journal volume & issue
Vol. 10, no. 1
p. 14

Abstract

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Abstract The mutations of the RET proto-oncogene contributes to the development of MTC by increasing the activity of the receptor encoded by this gene. Variant T of polymorphism rs2435357 located in the enhancer of the RET gene reduces the enhancer’s activity. The opposite effects of rs2435357 and the mutations causing medullary thyroid carcinoma resulted in the investigation of the status of this polymorphism in patients with MTC. In our study, we compared the frequency of polymorphism rs2435357 in the group of 48 MTC patients with its frequency in Polish population. The frequency of heterozygotes C/T at rs2435357 reached almost 12% (18/152) for the Polish population, in contrast to the group of MTC patients where not even a single T allele was found. The frequency difference is statistically significant. This observation might indicate that the presence of the heterozygous T allele at rs2435357 may be associated with the inhibition of medullary thyroid carcinoma development.