DNA methylation signature in blood mirrors successful weight-loss during lifestyle interventions: the CENTRAL trial

Maria Keller; Anat Yaskolka Meir; Stephan H. Bernhart; Yftach Gepner; Ilan Shelef; Dan Schwarzfuchs; Gal Tsaban; Hila Zelicha; Lydia Hopp; Luise Müller; Kerstin Rohde; Yvonne Böttcher; Peter F. Stadler; Michael Stumvoll; Matthias Blüher; Peter Kovacs; Iris Shai

doi:10.1186/s13073-020-00794-7

DNA methylation signature in blood mirrors successful weight-loss during lifestyle interventions: the CENTRAL trial

Maria Keller, Anat Yaskolka Meir, Stephan H. Bernhart, Yftach Gepner, Ilan Shelef, Dan Schwarzfuchs, Gal Tsaban, Hila Zelicha, Lydia Hopp, Luise Müller, Kerstin Rohde, Yvonne Böttcher, Peter F. Stadler, Michael Stumvoll, Matthias Blüher, Peter Kovacs^*, Iris Shai^*

^*Corresponding author for this work

School of Public Health

Research output: Contribution to journal › Article › peer-review

37 Scopus citations

Abstract

Background: One of the major challenges in obesity treatment is to explain the high variability in the individual’s response to specific dietary and physical activity interventions. With this study, we tested the hypothesis that specific DNA methylation changes reflect individual responsiveness to lifestyle intervention and may serve as epigenetic predictors for a successful weight-loss. Methods: We conducted an explorative genome-wide DNA methylation analysis in blood samples from 120 subjects (90% men, mean ± SD age = 49 ± 9 years, body mass-index (BMI) = 30.2 ± 3.3 kg/m²) from the 18-month CENTRAL randomized controlled trial who underwent either Mediterranean/low-carbohydrate or low-fat diet with or without physical activity. Results: Analyses comparing male subjects with the most prominent body weight-loss (responders, mean weight change − 16%) vs. non-responders (+ 2.4%) (N = 10 each) revealed significant variation in DNA methylation of several genes including LRRC27, CRISP2, and SLFN12 (all adj. P < 1 × 10⁻⁵). Gene ontology analysis indicated that biological processes such as cell adhesion and molecular functions such as calcium ion binding could have an important role in determining the success of interventional therapies in obesity. Epigenome-wide association for relative weight-loss (%) identified 15 CpGs being negatively correlated with weight change after intervention (all combined P < 1 × 10^{− 4}) including new and also known obesity candidates such as NUDT3 and NCOR2. A baseline DNA methylation score better predicted successful weight-loss [area under the curve (AUC) receiver operating characteristic (ROC) = 0.95–1.0] than predictors such as age and BMI (AUC ROC = 0.56). Conclusions: Body weight-loss following 18-month lifestyle intervention is associated with specific methylation signatures. Moreover, methylation differences in the identified genes could serve as prognostic biomarkers to predict a successful weight-loss therapy and thus contribute to advances in patient-tailored obesity treatment.

Original language	English
Article number	97
Journal	Genome Medicine
Volume	12
Issue number	1
DOIs	https://doi.org/10.1186/s13073-020-00794-7
State	Published - Dec 2020

Funding

Funders	Funder number
Deutsches Zentrum für Diabetesforschung
Diabetes Hilfs- und Forschungsfonds Deutschland
Floor Pepers
German Diabetes Association
Hadassah Hebrew University Medical Center
ServiceXS
Veronica Atkins Research Foundation
California Walnut Commission
Deutsche Forschungsgemeinschaft	B11, SPP 1629 TO 718/2- 1, 209933838 – SFB 1052, KE 2182/1-1
Bundesministerium für Bildung und Forschung	K7-117, AD2-06E95, AD2-7123, AD2-7118, ADI-K50D, 01EO1501, ADI-K7-39, AD2-060E
Israel Science Foundation
Ministry of Science and Technology, Israel	3-13604
Freistaat Sachsen

Keywords

DNA methylation
Epigenetics
Gene
Lifestyle intervention
Weight-loss

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1186/s13073-020-00794-7

Cite this

Keller, M., Yaskolka Meir, A., Bernhart, S. H., Gepner, Y., Shelef, I., Schwarzfuchs, D., Tsaban, G., Zelicha, H., Hopp, L., Müller, L., Rohde, K., Böttcher, Y., Stadler, P. F., Stumvoll, M., Blüher, M., Kovacs, P., & Shai, I. (2020). DNA methylation signature in blood mirrors successful weight-loss during lifestyle interventions: the CENTRAL trial. Genome Medicine, 12(1), Article 97. https://doi.org/10.1186/s13073-020-00794-7

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abstract = "Background: One of the major challenges in obesity treatment is to explain the high variability in the individual{\textquoteright}s response to specific dietary and physical activity interventions. With this study, we tested the hypothesis that specific DNA methylation changes reflect individual responsiveness to lifestyle intervention and may serve as epigenetic predictors for a successful weight-loss. Methods: We conducted an explorative genome-wide DNA methylation analysis in blood samples from 120 subjects (90% men, mean ± SD age = 49 ± 9 years, body mass-index (BMI) = 30.2 ± 3.3 kg/m2) from the 18-month CENTRAL randomized controlled trial who underwent either Mediterranean/low-carbohydrate or low-fat diet with or without physical activity. Results: Analyses comparing male subjects with the most prominent body weight-loss (responders, mean weight change − 16%) vs. non-responders (+ 2.4%) (N = 10 each) revealed significant variation in DNA methylation of several genes including LRRC27, CRISP2, and SLFN12 (all adj. P < 1 × 10−5). Gene ontology analysis indicated that biological processes such as cell adhesion and molecular functions such as calcium ion binding could have an important role in determining the success of interventional therapies in obesity. Epigenome-wide association for relative weight-loss (%) identified 15 CpGs being negatively correlated with weight change after intervention (all combined P < 1 × 10− 4) including new and also known obesity candidates such as NUDT3 and NCOR2. A baseline DNA methylation score better predicted successful weight-loss [area under the curve (AUC) receiver operating characteristic (ROC) = 0.95–1.0] than predictors such as age and BMI (AUC ROC = 0.56). Conclusions: Body weight-loss following 18-month lifestyle intervention is associated with specific methylation signatures. Moreover, methylation differences in the identified genes could serve as prognostic biomarkers to predict a successful weight-loss therapy and thus contribute to advances in patient-tailored obesity treatment.",

keywords = "DNA methylation, Epigenetics, Gene, Lifestyle intervention, Weight-loss",

author = "Maria Keller and {Yaskolka Meir}, Anat and Bernhart, {Stephan H.} and Yftach Gepner and Ilan Shelef and Dan Schwarzfuchs and Gal Tsaban and Hila Zelicha and Lydia Hopp and Luise M{\"u}ller and Kerstin Rohde and Yvonne B{\"o}ttcher and Stadler, {Peter F.} and Michael Stumvoll and Matthias Bl{\"u}her and Peter Kovacs and Iris Shai",

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Keller, M, Yaskolka Meir, A, Bernhart, SH, Gepner, Y, Shelef, I, Schwarzfuchs, D, Tsaban, G, Zelicha, H, Hopp, L, Müller, L, Rohde, K, Böttcher, Y, Stadler, PF, Stumvoll, M, Blüher, M, Kovacs, P & Shai, I 2020, 'DNA methylation signature in blood mirrors successful weight-loss during lifestyle interventions: the CENTRAL trial', Genome Medicine, vol. 12, no. 1, 97. https://doi.org/10.1186/s13073-020-00794-7

TY - JOUR

T1 - DNA methylation signature in blood mirrors successful weight-loss during lifestyle interventions

T2 - the CENTRAL trial

AU - Keller, Maria

AU - Yaskolka Meir, Anat

AU - Bernhart, Stephan H.

AU - Gepner, Yftach

AU - Shelef, Ilan

AU - Schwarzfuchs, Dan

AU - Tsaban, Gal

AU - Zelicha, Hila

AU - Hopp, Lydia

AU - Müller, Luise

AU - Rohde, Kerstin

AU - Böttcher, Yvonne

AU - Stadler, Peter F.

AU - Stumvoll, Michael

AU - Blüher, Matthias

AU - Kovacs, Peter

AU - Shai, Iris

PY - 2020/12

Y1 - 2020/12

N2 - Background: One of the major challenges in obesity treatment is to explain the high variability in the individual’s response to specific dietary and physical activity interventions. With this study, we tested the hypothesis that specific DNA methylation changes reflect individual responsiveness to lifestyle intervention and may serve as epigenetic predictors for a successful weight-loss. Methods: We conducted an explorative genome-wide DNA methylation analysis in blood samples from 120 subjects (90% men, mean ± SD age = 49 ± 9 years, body mass-index (BMI) = 30.2 ± 3.3 kg/m2) from the 18-month CENTRAL randomized controlled trial who underwent either Mediterranean/low-carbohydrate or low-fat diet with or without physical activity. Results: Analyses comparing male subjects with the most prominent body weight-loss (responders, mean weight change − 16%) vs. non-responders (+ 2.4%) (N = 10 each) revealed significant variation in DNA methylation of several genes including LRRC27, CRISP2, and SLFN12 (all adj. P < 1 × 10−5). Gene ontology analysis indicated that biological processes such as cell adhesion and molecular functions such as calcium ion binding could have an important role in determining the success of interventional therapies in obesity. Epigenome-wide association for relative weight-loss (%) identified 15 CpGs being negatively correlated with weight change after intervention (all combined P < 1 × 10− 4) including new and also known obesity candidates such as NUDT3 and NCOR2. A baseline DNA methylation score better predicted successful weight-loss [area under the curve (AUC) receiver operating characteristic (ROC) = 0.95–1.0] than predictors such as age and BMI (AUC ROC = 0.56). Conclusions: Body weight-loss following 18-month lifestyle intervention is associated with specific methylation signatures. Moreover, methylation differences in the identified genes could serve as prognostic biomarkers to predict a successful weight-loss therapy and thus contribute to advances in patient-tailored obesity treatment.

AB - Background: One of the major challenges in obesity treatment is to explain the high variability in the individual’s response to specific dietary and physical activity interventions. With this study, we tested the hypothesis that specific DNA methylation changes reflect individual responsiveness to lifestyle intervention and may serve as epigenetic predictors for a successful weight-loss. Methods: We conducted an explorative genome-wide DNA methylation analysis in blood samples from 120 subjects (90% men, mean ± SD age = 49 ± 9 years, body mass-index (BMI) = 30.2 ± 3.3 kg/m2) from the 18-month CENTRAL randomized controlled trial who underwent either Mediterranean/low-carbohydrate or low-fat diet with or without physical activity. Results: Analyses comparing male subjects with the most prominent body weight-loss (responders, mean weight change − 16%) vs. non-responders (+ 2.4%) (N = 10 each) revealed significant variation in DNA methylation of several genes including LRRC27, CRISP2, and SLFN12 (all adj. P < 1 × 10−5). Gene ontology analysis indicated that biological processes such as cell adhesion and molecular functions such as calcium ion binding could have an important role in determining the success of interventional therapies in obesity. Epigenome-wide association for relative weight-loss (%) identified 15 CpGs being negatively correlated with weight change after intervention (all combined P < 1 × 10− 4) including new and also known obesity candidates such as NUDT3 and NCOR2. A baseline DNA methylation score better predicted successful weight-loss [area under the curve (AUC) receiver operating characteristic (ROC) = 0.95–1.0] than predictors such as age and BMI (AUC ROC = 0.56). Conclusions: Body weight-loss following 18-month lifestyle intervention is associated with specific methylation signatures. Moreover, methylation differences in the identified genes could serve as prognostic biomarkers to predict a successful weight-loss therapy and thus contribute to advances in patient-tailored obesity treatment.

KW - DNA methylation

KW - Epigenetics

KW - Gene

KW - Lifestyle intervention

KW - Weight-loss

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DNA methylation signature in blood mirrors successful weight-loss during lifestyle interventions: the CENTRAL trial

Abstract

Funding

Keywords

UN SDGs

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