Leukocyte-adjusted epigenome-wide association studies of blood from solid tumor patients

Scott M. Langevin, E. Andres Houseman, William P. Accomando, Devin C. Koestler, Brock C. Christensen, Heather H. Nelson, Margaret R. Karagas, Carmen J. Marsit, John K. Wiencke, Karl T. Kelsey

Research output: Contribution to journalArticlepeer-review

32 Scopus citations

Abstract

Epigenome-wide studies of DNA methylation using blood-derived DNA from cancer patients are complicated by the heterogeneity of cell types within blood and the associated cell lineage specification of DNA methylation signatures. Here, we applied a novel set of analytic approaches to assess the association between cancer case-status and DNA methylation adjusted for leukocyte variation using blood specimens from three case-control cancer studies (bladder: 223 cases, 205 controls; head and neck: 92 cases, 92 controls; and ovarian: 131 cases, 274 controls). Using previously published data on leukocyte-specific CpG loci and a recently described approach to deconvolute subject-specific blood composition, we performed an epigenome-wide analysis to examine the association between blood-based DNA methylation patterns and each of the three aforementioned solid tumor types adjusted for cellular heterogeneity in blood. After adjusting for leukocyte profile in our epigenome-wide analysis, the omnibus association between case-status and methylation was significant for all three studies (bladder cancer: P = 0.047; HNSCC: P = 0.013; ovarian cancer: P = 0.0002). Subsequent analyses revealed that CpG sites associated with cancer were enriched for transcription factor binding motifs involved with cancer-associated pathways. These results support the existence of cancer-associated DNA methylation profiles in the blood of solid tumor patients that are independent of alterations in normal leukocyte distributions. Adoption of the methods developed here will make it feasible to rigorously assess the influence of variability of normal leukocyte profiles when investigating cancer related changes in blood-based epigenome-wide association studies.

Original languageEnglish (US)
Pages (from-to)884-895
Number of pages12
JournalEpigenetics
Volume9
Issue number6
DOIs
StatePublished - Mar 26 2014

Bibliographical note

Funding Information:
This work was supported by the National Cancer Institute (R01CA121147, R01CA100679, and R01CA078609 to K.T.K., R01CA057494 to M.R.K., R01CA082354 to H.H.N., R01 CA126831 J.K.W., and K22CA172358 to S.M.L.); and National Institute of Environmental Health Sciences (P42ES007373 to M.R.K. and T32ES07272 to S.M.L.).

Keywords

  • Bladder cancer
  • EWAS
  • Epigenomics
  • HNSCC
  • Ovarian cancer

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