Integration of methylation quantitative trait loci (mQTL) on dietary intake on DNA methylation levels: an example of n-3 PUFA and ABCA1 gene

Ryosuke Fujii; Yoshitaka Ando; Hiroya Yamada; Yoshiki Tsuboi; Eiji Munetsuna; Mirai Yamazaki; Genki Mizuno; Keisuke Maeda; Koji Ohashi; Hiroaki Ishikawa; Mami Watanabe; Nahomi Imaeda; Chiho Goto; Kenji Wakai; Shuji Hashimoto; Koji Suzuki

doi:10.1038/s41430-023-01315-6

Integration of methylation quantitative trait loci (mQTL) on dietary intake on DNA methylation levels: an example of n-3 PUFA and ABCA1 gene

Ryosuke Fujii, Yoshitaka Ando, Hiroya Yamada, Yoshiki Tsuboi, Eiji Munetsuna, Mirai Yamazaki, Genki Mizuno, Keisuke Maeda, Koji Ohashi, Hiroaki Ishikawa, Mami Watanabe, Nahomi Imaeda, Chiho Goto, Kenji Wakai, Shuji Hashimoto, Koji Suzuki

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

抄録

Background: Epigenetic studies have reported relationships between dietary nutrient intake and methylation levels. However, genetic variants that may affect DNA methylation (DNAm) pattern, called methylation quantitative loci (mQTL), are usually overlooked in these analyses. We investigated whether mQTL change the relationship between dietary nutrient intake and leukocyte DNAm levels with an example of estimated fatty acid intake and ATP-binding cassette transporter A1 (ABCA1). Methods: A cross-sectional study on 231 participants (108 men, mean age: 62.7 y) without clinical history of cancer and no prescriptions for dyslipidemia. We measured leukocyte DNAm levels of 8 CpG sites within ABCA1 gene by pyrosequencing method and used mean methylation levels for statistical analysis. TaqMan assay was used for genotyping a genetic variant of ABCA1 (rs1800976). Dietary fatty acid intake was estimated with a validated food frequency questionnaire and adjusted for total energy intake by using residual methods. Results: Mean ABCA1 DNAm levels were 5% lower with the number of minor alleles in rs1800976 (CC, 40.6%; CG, 35.9%; GG, 30.6%). Higher dietary n-3 PUFA intake was associated with lower ABCA1 DNAm levels (1st (ref) vs. 4th, β [95% CI]: –2.52 [–4.77, –0.28]). After controlling for rs180076, the association between dietary n-3 PUFA intake and ABCA1 DNAm levels was attenuated, but still showed an independent association (1st (ref) vs. 4th, β [95% CI]: –2.00 [–3.84, –0.18]). The interaction of mQTL and dietary n-3 PUFA intake on DNAm levels was not significant. Conclusions: This result suggested that dietary n-3 PUFA intake would be an independent predictor of DNAm levels in ABCA1 gene after adjusting for individual genetic background. Considering mQTL need to broaden into other genes and nutrients for deeper understanding of DNA methylation, which can contribute to personalized nutritional intervention.

本文言語	英語
ページ（範囲）	881-887
ページ数	7
ジャーナル	European Journal of Clinical Nutrition
巻	77
号	9
DOI	https://doi.org/10.1038/s41430-023-01315-6
出版ステータス	出版済み - 09-2023

All Science Journal Classification (ASJC) codes

医学（その他）
栄養および糖尿病

UN SDG

この成果は、次の持続可能な開発目標に貢献しています

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10.1038/s41430-023-01315-6

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引用スタイル

Fujii, R., Ando, Y., Yamada, H., Tsuboi, Y., Munetsuna, E., Yamazaki, M., Mizuno, G., Maeda, K., Ohashi, K., Ishikawa, H., Watanabe, M., Imaeda, N., Goto, C., Wakai, K., Hashimoto, S., & Suzuki, K. (2023). Integration of methylation quantitative trait loci (mQTL) on dietary intake on DNA methylation levels: an example of n-3 PUFA and ABCA1 gene. European Journal of Clinical Nutrition, 77(9), 881-887. https://doi.org/10.1038/s41430-023-01315-6

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title = "Integration of methylation quantitative trait loci (mQTL) on dietary intake on DNA methylation levels: an example of n-3 PUFA and ABCA1 gene",

abstract = "Background: Epigenetic studies have reported relationships between dietary nutrient intake and methylation levels. However, genetic variants that may affect DNA methylation (DNAm) pattern, called methylation quantitative loci (mQTL), are usually overlooked in these analyses. We investigated whether mQTL change the relationship between dietary nutrient intake and leukocyte DNAm levels with an example of estimated fatty acid intake and ATP-binding cassette transporter A1 (ABCA1). Methods: A cross-sectional study on 231 participants (108 men, mean age: 62.7 y) without clinical history of cancer and no prescriptions for dyslipidemia. We measured leukocyte DNAm levels of 8 CpG sites within ABCA1 gene by pyrosequencing method and used mean methylation levels for statistical analysis. TaqMan assay was used for genotyping a genetic variant of ABCA1 (rs1800976). Dietary fatty acid intake was estimated with a validated food frequency questionnaire and adjusted for total energy intake by using residual methods. Results: Mean ABCA1 DNAm levels were 5% lower with the number of minor alleles in rs1800976 (CC, 40.6%; CG, 35.9%; GG, 30.6%). Higher dietary n-3 PUFA intake was associated with lower ABCA1 DNAm levels (1st (ref) vs. 4th, β [95% CI]: –2.52 [–4.77, –0.28]). After controlling for rs180076, the association between dietary n-3 PUFA intake and ABCA1 DNAm levels was attenuated, but still showed an independent association (1st (ref) vs. 4th, β [95% CI]: –2.00 [–3.84, –0.18]). The interaction of mQTL and dietary n-3 PUFA intake on DNAm levels was not significant. Conclusions: This result suggested that dietary n-3 PUFA intake would be an independent predictor of DNAm levels in ABCA1 gene after adjusting for individual genetic background. Considering mQTL need to broaden into other genes and nutrients for deeper understanding of DNA methylation, which can contribute to personalized nutritional intervention.",

author = "Ryosuke Fujii and Yoshitaka Ando and Hiroya Yamada and Yoshiki Tsuboi and Eiji Munetsuna and Mirai Yamazaki and Genki Mizuno and Keisuke Maeda and Koji Ohashi and Hiroaki Ishikawa and Mami Watanabe and Nahomi Imaeda and Chiho Goto and Kenji Wakai and Shuji Hashimoto and Koji Suzuki",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2023",

month = sep,

doi = "10.1038/s41430-023-01315-6",

language = "English",

volume = "77",

pages = "881--887",

journal = "European Journal of Clinical Nutrition",

issn = "0954-3007",

publisher = "Springer Nature",

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Fujii, R , Ando, Y , Yamada, H , Tsuboi, Y, Munetsuna, E, Yamazaki, M, Mizuno, G, Maeda, K , Ohashi, K , Ishikawa, H, Watanabe, M, Imaeda, N, Goto, C, Wakai, K, Hashimoto, S & Suzuki, K 2023, 'Integration of methylation quantitative trait loci (mQTL) on dietary intake on DNA methylation levels: an example of n-3 PUFA and ABCA1 gene', European Journal of Clinical Nutrition, vol. 77, no. 9, pp. 881-887. https://doi.org/10.1038/s41430-023-01315-6

TY - JOUR

T1 - Integration of methylation quantitative trait loci (mQTL) on dietary intake on DNA methylation levels

T2 - an example of n-3 PUFA and ABCA1 gene

AU - Fujii, Ryosuke

AU - Ando, Yoshitaka

AU - Yamada, Hiroya

AU - Tsuboi, Yoshiki

AU - Munetsuna, Eiji

AU - Yamazaki, Mirai

AU - Mizuno, Genki

AU - Maeda, Keisuke

AU - Ohashi, Koji

AU - Ishikawa, Hiroaki

AU - Watanabe, Mami

AU - Imaeda, Nahomi

AU - Goto, Chiho

AU - Wakai, Kenji

AU - Hashimoto, Shuji

AU - Suzuki, Koji

PY - 2023/9

Y1 - 2023/9

N2 - Background: Epigenetic studies have reported relationships between dietary nutrient intake and methylation levels. However, genetic variants that may affect DNA methylation (DNAm) pattern, called methylation quantitative loci (mQTL), are usually overlooked in these analyses. We investigated whether mQTL change the relationship between dietary nutrient intake and leukocyte DNAm levels with an example of estimated fatty acid intake and ATP-binding cassette transporter A1 (ABCA1). Methods: A cross-sectional study on 231 participants (108 men, mean age: 62.7 y) without clinical history of cancer and no prescriptions for dyslipidemia. We measured leukocyte DNAm levels of 8 CpG sites within ABCA1 gene by pyrosequencing method and used mean methylation levels for statistical analysis. TaqMan assay was used for genotyping a genetic variant of ABCA1 (rs1800976). Dietary fatty acid intake was estimated with a validated food frequency questionnaire and adjusted for total energy intake by using residual methods. Results: Mean ABCA1 DNAm levels were 5% lower with the number of minor alleles in rs1800976 (CC, 40.6%; CG, 35.9%; GG, 30.6%). Higher dietary n-3 PUFA intake was associated with lower ABCA1 DNAm levels (1st (ref) vs. 4th, β [95% CI]: –2.52 [–4.77, –0.28]). After controlling for rs180076, the association between dietary n-3 PUFA intake and ABCA1 DNAm levels was attenuated, but still showed an independent association (1st (ref) vs. 4th, β [95% CI]: –2.00 [–3.84, –0.18]). The interaction of mQTL and dietary n-3 PUFA intake on DNAm levels was not significant. Conclusions: This result suggested that dietary n-3 PUFA intake would be an independent predictor of DNAm levels in ABCA1 gene after adjusting for individual genetic background. Considering mQTL need to broaden into other genes and nutrients for deeper understanding of DNA methylation, which can contribute to personalized nutritional intervention.

AB - Background: Epigenetic studies have reported relationships between dietary nutrient intake and methylation levels. However, genetic variants that may affect DNA methylation (DNAm) pattern, called methylation quantitative loci (mQTL), are usually overlooked in these analyses. We investigated whether mQTL change the relationship between dietary nutrient intake and leukocyte DNAm levels with an example of estimated fatty acid intake and ATP-binding cassette transporter A1 (ABCA1). Methods: A cross-sectional study on 231 participants (108 men, mean age: 62.7 y) without clinical history of cancer and no prescriptions for dyslipidemia. We measured leukocyte DNAm levels of 8 CpG sites within ABCA1 gene by pyrosequencing method and used mean methylation levels for statistical analysis. TaqMan assay was used for genotyping a genetic variant of ABCA1 (rs1800976). Dietary fatty acid intake was estimated with a validated food frequency questionnaire and adjusted for total energy intake by using residual methods. Results: Mean ABCA1 DNAm levels were 5% lower with the number of minor alleles in rs1800976 (CC, 40.6%; CG, 35.9%; GG, 30.6%). Higher dietary n-3 PUFA intake was associated with lower ABCA1 DNAm levels (1st (ref) vs. 4th, β [95% CI]: –2.52 [–4.77, –0.28]). After controlling for rs180076, the association between dietary n-3 PUFA intake and ABCA1 DNAm levels was attenuated, but still showed an independent association (1st (ref) vs. 4th, β [95% CI]: –2.00 [–3.84, –0.18]). The interaction of mQTL and dietary n-3 PUFA intake on DNAm levels was not significant. Conclusions: This result suggested that dietary n-3 PUFA intake would be an independent predictor of DNAm levels in ABCA1 gene after adjusting for individual genetic background. Considering mQTL need to broaden into other genes and nutrients for deeper understanding of DNA methylation, which can contribute to personalized nutritional intervention.

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