Scientific Reports (May 2021)

A genetic variant in telomerase reverse transcriptase (TERT) modifies cancer risk in Lynch syndrome patients harbouring pathogenic MSH2 variants

  • Mariann Unhjem Wiik,
  • Tiffany-Jane Evans,
  • Sami Belhadj,
  • Katherine A. Bolton,
  • Dagmara Dymerska,
  • Shantie Jagmohan-Changur,
  • Gabriel Capellá,
  • Grzegorz Kurzawski,
  • Juul T. Wijnen,
  • Laura Valle,
  • Hans F. A. Vasen,
  • Jan Lubinski,
  • Rodney J. Scott,
  • Bente A. Talseth-Palmer

DOI
https://doi.org/10.1038/s41598-021-90501-2
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 9

Abstract

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Abstract Individuals with Lynch syndrome (LS), have an increased risk of developing cancer. Common genetic variants of telomerase reverse transcriptase (TERT) have been associated with a wide range of cancers, including colorectal cancer (CRC) in LS. We combined genotype data from 1881 LS patients, carrying pathogenic variants in MLH1, MSH2 or MSH6, for rs2075786 (G>A, intronic variant), 1207 LS patients for rs2736108 (C>T, upstream variant) and 1201 LS patients for rs7705526 (C>A, intronic variant). The risk of cancer was estimated by heterozygous/homozygous odds ratio (OR) with mixed-effects logistic regression to adjust for gene/gender/country of sample origin considering family identity. The AA genotype of SNP rs2075786 is associated with 85% higher odds at developing cancer compared to GG genotype in MSH2 pathogenic variant carriers (p = 0.0160). Kaplan–Meier analysis also shows an association for rs2075786; the AA allele for MSH2 variant carriers confers risk for earlier diagnosis of LS cancer (log-rank p = 0.0011). We report a polymorphism in TERT to be a possible modifier of disease risk in MSH2 pathogenic variant carriers. The rs2075786 SNP in TERT is associated with a differential risk of developing cancer for MSH2 pathogenic variant carriers. Use of this information has the potential to personalise screening protocols for LS patients.