PLoS ONE (Jan 2013)

Correlation of chromosomal instability, telomere length and telomere maintenance in microsatellite stable rectal cancer: a molecular subclass of rectal cancer.

  • Lisa A Boardman,
  • Ruth A Johnson,
  • Kimberly B Viker,
  • Kari A Hafner,
  • Robert B Jenkins,
  • Douglas L Riegert-Johnson,
  • Thomas C Smyrk,
  • Kristin Litzelman,
  • Songwon Seo,
  • Ronald E Gangnon,
  • Corinne D Engelman,
  • David N Rider,
  • Russell J Vanderboom,
  • Stephen N Thibodeau,
  • Gloria M Petersen,
  • Halcyon G Skinner

DOI
https://doi.org/10.1371/journal.pone.0080015
Journal volume & issue
Vol. 8, no. 11
p. e80015

Abstract

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IntroductionColorectal cancer (CRC) tumor DNA is characterized by chromosomal damage termed chromosomal instability (CIN) and excessively shortened telomeres. Up to 80% of CRC is microsatellite stable (MSS) and is historically considered to be chromosomally unstable (CIN+). However, tumor phenotyping depicts some MSS CRC with little or no genetic changes, thus being chromosomally stable (CIN-). MSS CIN- tumors have not been assessed for telomere attrition.Experimental designMSS rectal cancers from patients ≤50 years old with Stage II (B2 or higher) or Stage III disease were assessed for CIN, telomere length and telomere maintenance mechanism (telomerase activation [TA]; alternative lengthening of telomeres [ALT]). Relative telomere length was measured by qPCR in somatic epithelial and cancer DNA. TA was measured with the TRAPeze assay, and tumors were evaluated for the presence of C-circles indicative of ALT. p53 mutation status was assessed in all available samples. DNA copy number changes were evaluated with Spectral Genomics aCGH.ResultsTumors were classified as chromosomally stable (CIN-) and chromosomally instable (CIN+) by degree of DNA copy number changes. CIN- tumors (35%; n=6) had fewer copy number changes (ConclusionsMSS rectal cancer appears to represent a heterogeneous group of tumors that may be categorized both on the basis of CIN status and telomere maintenance mechanism. MSS CIN- rectal cancers appear to have longer telomeres than those of MSS CIN+ rectal cancers and to utilize ALT rather than activation of telomerase.