Abstract
BackgroundIrinotecan (SN38) and oxaliplatin are chemotherapeutic agents used in the treatment of colorectal cancer. However, the frequent development of resistance to these drugs represents a considerable challenge in the clinic. Alus as retrotransposons comprise 11% of the human genome. Genomic toxicity induced by carcinogens or drugs can reactivate Alus by altering DNA methylation. Whether or not reactivation of Alus occurs in SN38 and oxaliplatin resistance remains unknown.ResultsWe applied reduced representation bisulfite sequencing (RRBS) to investigate the DNA methylome in SN38 or oxaliplatin resistant colorectal cancer cell line models. Moreover, we extended the RRBS analysis to tumor tissue from 14 patients with colorectal cancer who either did or did not benefit from capecitabine + oxaliplatin treatment. For the clinical samples, we applied a concept of ‘DNA methylation entropy’ to estimate the diversity of DNA methylation states of the identified resistance phenotype-associated methylation loci observed in the cell line models. We identified different loci being characteristic for the different resistant cell lines. Interestingly, 53% of the identified loci were Alu sequences- especially the Alu Y subfamily. Furthermore, we identified an enrichment of Alu Y sequences that likely results from increased integration of new copies of Alu Y sequence in the drug-resistant cell lines. In the clinical samples, SOX1 and other SOX gene family members were shown to display variable DNA methylation states in their gene regions. The Alu Y sequences showed remarkable variation in DNA methylation states across the clinical samples.ConclusionOur findings imply a crucial role of Alu Y in colorectal cancer drug resistance. Our study underscores the complexity of colorectal cancer aggravated by mobility of Alu elements and stresses the importance of personalized strategies, using a systematic and dynamic view, for effective cancer therapy.Electronic supplementary materialThe online version of this article (doi:10.1186/s12864-015-1552-y) contains supplementary material, which is available to authorized users.
Highlights
Irinotecan (SN38) and oxaliplatin are chemotherapeutic agents used in the treatment of colorectal cancer
All cell lines merged in a big cluster separated from the clinical samples in unsupervised clustering, suggesting that the colorectal cancer cell lines might show similar features of DNA methylome, whereas sporadic clinical samples show high diversity between individual methylomes
We found that sets P, O and S are highly enriched in Alu elements, which accounted for 48.8%, 60.1% and 53.3% of all identified cytosine loci, respectively
Summary
Irinotecan (SN38) and oxaliplatin are chemotherapeutic agents used in the treatment of colorectal cancer. Genomic toxicity induced by carcinogens or drugs can reactivate Alus by altering DNA methylation. Whether or not reactivation of Alus occurs in SN38 and oxaliplatin resistance remains unknown. FOLFIRI (folinic acid, 5-fluorouracil and irinotecan) [2], FOLFOX (folinic acid, 5-fluorouracil and oxaliplatin) [3] and XELOX (capecitabine and oxaliplatin) [4] are commonly used chemotherapeutic combinations used to treat colorectal cancer. A considerable subpopulation of patients will experience disease recurrence due to acquired resistance to treatment. The molecular mechanisms underlying acquired resistance to these drugs remain elusive. DNA methylation is a long-term stable epigenetic mechanism. DNA methylation represses the activity of mobile genetic elements and maintains genome integrity
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