Interest in the potential of DNA methylation in peripheral blood as a biomarker of cancer risk is increasing. We aimed to assess whether epigenome-wide DNA methylation measured in peripheral blood samples obtained before onset of the disease is associated with increased risk of breast cancer. We report on three independent prospective nested case-control studies from the European Prospective Investigation into Cancer and Nutrition (EPIC-Italy; n = 162 matched case-control pairs), the Norwegian Women and Cancer study (NOWAC; n = 168 matched pairs), and the Breakthrough Generations Study (BGS; n = 548 matched pairs). We used the Illumina 450k array to measure methylation in the EPIC and NOWAC cohorts. Whole-genome bisulphite sequencing (WGBS) was performed on the BGS cohort using pooled DNA samples, combined to reach 50× coverage across ~16 million CpG sites in the genome including 450k array CpG sites. Mean β values over all probes were calculated as a measurement for epigenome-wide methylation

Agnoli, C

Ashworth, A

Baglietto, L

Chadeau, M

Curry, E

Flanagan, JM

Flower, K

Frasca, G

Garcia-Closas, M

Jones, M

Krogh, V

Lund, E

Masala, G

Mattiello, A

Orr, N

Palli, D

Panico, S

Polidoro, S

Sacerdote, C

Sandanger, T

Severi, G

Swerdlow, A

Tomczyk, K

Tumino, R

van veldhoven, K

vineis, P

Clinical Epigenetics

English

PubMed

Karin van Veldhoven

Silvia Polidoro

Laura Baglietto

Gianluca Severi

Carlotta Sacerdote

Salvatore Panico

Amalia Mattiello

Domenico Palli

Giovanna Masala

Vittorio Krogh

Claudia Agnoli

Rosario Tumino

Graziella Frasca

Kirsty Flower

Ed Curry

Nicholas Orr

Katarzyna Tomczyk

Michael E. Jones

Alan Ashworth

Anthony Swerdlow

Marc Chadeau-Hyam

Eiliv Lund

Montserrat Garcia-Closas

Torkjel M. Sandanger

James M. Flanagan

Paolo Vineis

Crossref

Epigenome-wide association study reveals decreased average methylation levels years before breast cancer diagnosis

Background: Interest in the potential of DNA methylation in peripheral blood as a biomarker of cancer risk is
increasing. We aimed to assess whether epigenome-wide DNA methylation measured in peripheral blood samples
obtained before onset of the disease is associated with increased risk of breast cancer. We report on three independent
prospective nested case-control studies from the European Prospective Investigation into Cancer and Nutrition
(EPIC-Italy; n = 162 matched case-control pairs), the Norwegian Women and Cancer study (NOWAC; n = 168
matched pairs), and the Breakthrough Generations Study (BGS; n = 548 matched pairs). We used the Illumina 450k
array to measure methylation in the EPIC and NOWAC cohorts. Whole-genome bisulphite sequencing (WGBS) was
performed on the BGS cohort using pooled DNA samples, combined to reach 50× coverage across ~16 million CpG
sites in the genome including 450k array CpG sites. Mean β values over all probes were calculated as a measurement
for epigenome-wide methylation.
Results: In EPIC, we found that high epigenome-wide methylation was associated with lower risk of breast cancer
(odds ratio (OR) per 1 SD = 0.61, 95 % confidence interval (CI) 0.47–0.80; −0.2 % average difference in epigenome-wide
methylation for cases and controls). Specifically, this was observed in gene bodies (OR = 0.51, 95 % CI 0.38–0.69) but
not in gene promoters (OR = 0.92, 95 % CI 0.64–1.32). The association was not replicated in NOWAC (OR = 1.03 95 % CI
0.81–1.30). The reasons for heterogeneity across studies are unclear. However, data from the BGS cohort was consistent
with epigenome-wide hypomethylation in breast cancer cases across the overlapping 450k probe sites (difference in
average epigenome-wide methylation in case and control DNA pools = −0.2 %).
Conclusions: We conclude that epigenome-wide hypomethylation of DNA from pre-diagnostic blood samples may
be predictive of breast cancer risk and may thus be useful as a clinical biomarker

van Veldhoven, Karin

Polidoro, Silvia

Baglietto, Laura

Severi, Gianluca

Sacerdote, Carlotta

Panico, Salvatore

Mattiello, Amalia

Palli, Domenico

Masala, Giovanna

Krogh, Vittorio

Agnoli, Claudia

Tumino, Rosario

Frasca, Graziella

Flower, Kirsty

Curry, Ed

Orr, Nicholas

Tomczyk, Katarzyna

Jones, Michael E.

Ashworth, Alan

Swerdlow, Anthony

Chadeau-Hyam, Marc

Lund, Eiliv

Garcia-Closas, Montserrat

Sandanger, Torkjel M

Flanagan, James M.

Vineis, Paolo

NORA - Norwegian Open Research Archives

Interest in the potential of DNA methylation in peripheral blood as a biomarker of cancer risk is increasing. We aimed to assess whether epigenome-wide DNA methylation measured in peripheral blood samples obtained before onset of the disease is associated with increased risk of breast cancer. We report on three independent prospective nested case-control studies from the European Prospective Investigation into Cancer and Nutrition (EPIC-Italy; n = 162 matched case-control pairs), the Norwegian Women and Cancer study (NOWAC; n = 168 matched pairs), and the Breakthrough Generations Study (BGS; n = 548 matched pairs). We used the Illumina 450k array to measure methylation in the EPIC and NOWAC cohorts. Whole-genome bisulphite sequencing (WGBS) was performed on the BGS cohort using pooled DNA samples, combined to reach 50× coverage across ~16 million CpG sites in the genome including 450k array CpG sites. Mean β values over all probes were calculated as a measurement for epigenome-wide methylation

PANICO, SALVATORE

Jones, Michael E

Chadeau Hyam, Marc

Garcia Closas, Montserrat

Flanagan, James M

Archivio della ricerca - Università degli studi di Napoli Federico II

Springer - Publisher Connector

Background. Interest in the potential of DNA methylation in peripheral blood as a biomarker of cancer risk is increasing. We aimed to assess whether epigenome-wide DNA methylation measured in peripheral blood samples obtained before onset of the disease is associated with increased risk of breast cancer.
Methods. We report on three independent prospective nested case-control studies from the European Prospective Investigation into Cancer and Nutrition (EPIC-Italy, n=162 matched case-control pairs); the Norwegian Women and Cancer study (NOWAC, n=168 matched pairs); and the Breakthrough Generations Study (BGS, n=548 matched pairs). We used the Illumina 450k array to measure methylation in the EPIC and NOWAC cohorts. Whole genome bisulphite sequencing (WGBS) was performed on the BGS cohort using pooled DNA samples, combined to reach 50x-coverage across ~16 million CpG sites in the genome including 450k array CpG sites. Mean β values over all probes were calculated as a measurement for epigenome-wide methylation.
Results. In EPIC we found that high epigenome-wide methylation was associated with lower risk of breast cancer (OR per 1SD=0.61, 95%CI 0.47–0.80; -0.2% average difference in epigenome-wide methylation for cases and controls). Specifically, this was observed in gene bodies (OR=0.51, 95%CI 0.38–0.69) but not in gene promoters (OR=0.92, 95%CI 0.64–1.32). The association was not replicated in NOWAC (OR=1.03 95%CI 0.81–1.30). The reasons for heterogeneity across studies are unclear. However, data from the BGS cohort was consistent with epigenome-wide hypomethylation in breast cancer cases across the overlapping 450k probe sites (difference in average epigenome-wide methylation in case and control DNA pools=-0.2%).
Conclusions. We conclude that epigenome-wide hypomethylation of DNA from pre-diagnostic blood samples may be predictive of breast cancer risk and may thus be useful as a clinical biomarker

Spiral - Imperial College Digital Repository

Background: Interest in the potential of DNA methylation in peripheral blood as a biomarker of cancer risk is increasing. We aimed to assess whether epigenome-wide DNA methylation measured in peripheral blood samples obtained before onset of the disease is associated with increased risk of breast cancer. We report on three independent prospective nested case-control studies from the European Prospective Investigation into Cancer and Nutrition (EPIC-Italy; n = 162 matched case-control pairs), the Norwegian Women and Cancer study (NOWAC; n = 168 matched pairs), and the Breakthrough Generations Study (BGS; n = 548 matched pairs). We used the Illumina 450k array to measure methylation in the EPIC and NOWAC cohorts. Whole-genome bisulphite sequencing (WGBS) was performed on the BGS cohort using pooled DNA samples, combined to reach 50× coverage across ~16 million CpG sites in the genome including 450k array CpG sites. Mean β values over all probes were calculated as a measurement for epigenome-wide methylation. Results: In EPIC, we found that high epigenome-wide methylation was associated with lower risk of breast cancer (odds ratio (OR) per 1 SD = 0.61, 95&nbsp;% confidence interval (CI) 0.47–0.80; −0.2&nbsp;% average difference in epigenome-wide methylation for cases and controls). Specifically, this was observed in gene bodies (OR = 0.51, 95&nbsp;% CI 0.38–0.69) but not in gene promoters (OR = 0.92, 95&nbsp;% CI 0.64–1.32). The association was not replicated in NOWAC (OR = 1.03 95&nbsp;% CI 0.81–1.30). The reasons for heterogeneity across studies are unclear. However, data from the BGS cohort was consistent with epigenome-wide hypomethylation in breast cancer cases across the overlapping 450k probe sites (difference in average epigenome-wide methylation in case and control DNA pools = −0.2&nbsp;%). Conclusions: We conclude that epigenome-wide hypomethylation of DNA from pre-diagnostic blood samples may be predictive of breast cancer risk and may thus be useful as a clinical biomarker

BAGLIETTO, LAURA

Sandanger, Torkjel M.

Archivio della Ricerca - Università di Pisa

Background: Interest in the potential of DNA methylation in peripheral blood as a biomarker of cancer risk is
increasing. We aimed to assess whether epigenome-wide DNA methylation measured in peripheral blood samples
obtained before onset of the disease is associated with increased risk of breast cancer. We report on three independent
prospective nested case-control studies from the European Prospective Investigation into Cancer and Nutrition
(EPIC-Italy; n = 162 matched case-control pairs), the Norwegian Women and Cancer study (NOWAC; n = 168
matched pairs), and the Breakthrough Generations Study (BGS; n = 548 matched pairs). We used the Illumina 450k
array to measure methylation in the EPIC and NOWAC cohorts. Whole-genome bisulphite sequencing (WGBS) was
performed on the BGS cohort using pooled DNA samples, combined to reach 50× coverage across ~16 million CpG
sites in the genome including 450k array CpG sites. Mean β values over all probes were calculated as a measurement
for epigenome-wide methylation.
Results: In EPIC, we found that high epigenome-wide methylation was associated with lower risk of breast cancer
(odds ratio (OR) per 1 SD = 0.61, 95 % confidence interval (CI) 0.47–0.80; −0.2 % average difference in epigenome-wide
methylation for cases and controls). Specifically, this was observed in gene bodies (OR = 0.51, 95 % CI 0.38–0.69) but
not in gene promoters (OR = 0.92, 95 % CI 0.64–1.32). The association was not replicated in NOWAC (OR = 1.03 95 % CI
0.81–1.30). The reasons for heterogeneity across studies are unclear. However, data from the BGS cohort was consistent
with epigenome-wide hypomethylation in breast cancer cases across the overlapping 450k probe sites (difference in
average epigenome-wide methylation in case and control DNA pools = −0.2 %).
Conclusions: We conclude that epigenome-wide hypomethylation of DNA from pre-diagnostic blood samples may
be predictive of breast cancer risk and may thus be useful as a clinical biomarker

Munin - Open Research Archive

BACKGROUND: Interest in the potential of DNA methylation in peripheral blood as a biomarker of cancer risk is increasing. We aimed to assess whether epigenome-wide DNA methylation measured in peripheral blood samples obtained before onset of the disease is associated with increased risk of breast cancer. We report on three independent prospective nested case-control studies from the European Prospective Investigation into Cancer and Nutrition (EPIC-Italy; n = 162 matched case-control pairs), the Norwegian Women and Cancer study (NOWAC; n = 168 matched pairs), and the Breakthrough Generations Study (BGS; n = 548 matched pairs). We used the Illumina 450k array to measure methylation in the EPIC and NOWAC cohorts. Whole-genome bisulphite sequencing (WGBS) was performed on the BGS cohort using pooled DNA samples, combined to reach 50× coverage across ~16 million CpG sites in the genome including 450k array CpG sites. Mean β values over all probes were calculated as a measurement for epigenome-wide methylation. RESULTS: In EPIC, we found that high epigenome-wide methylation was associated with lower risk of breast cancer (odds ratio (OR) per 1 SD = 0.61, 95 % confidence interval (CI) 0.47-0.80; -0.2 % average difference in epigenome-wide methylation for cases and controls). Specifically, this was observed in gene bodies (OR = 0.51, 95 % CI 0.38-0.69) but not in gene promoters (OR = 0.92, 95 % CI 0.64-1.32). The association was not replicated in NOWAC (OR = 1.03 95 % CI 0.81-1.30). The reasons for heterogeneity across studies are unclear. However, data from the BGS cohort was consistent with epigenome-wide hypomethylation in breast cancer cases across the overlapping 450k probe sites (difference in average epigenome-wide methylation in case and control DNA pools = -0.2 %). CONCLUSIONS: We conclude that epigenome-wide hypomethylation of DNA from pre-diagnostic blood samples may be predictive of breast cancer risk and may thus be useful as a clinical biomarker

van Veldhoven, K

Jones, ME

Chadeau-Hyam, M

Sandanger, TM

Vineis, P

University of Melbourne Institutional Repository

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Epigenome-wide association study reveals decreased average methylation levels years before breast cancer diagnosis

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