Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits

Research output: Contribution to journalJournal articleResearchpeer-review

Standard

Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits. / Dashti, Hassan S; Follis, Jack L; Smith, Caren E; Tanaka, Toshiko; Garaulet, Marta; Gottlieb, Daniel J; Hruby, Adela; Jacques, Paul F; Kiefte-de Jong, Jessica C; Lamon-Fava, Stefania; Scheer, Frank A J L; Bartz, Traci M; Kovanen, Leena; Wojczynski, Mary K; Frazier-Wood, Alexis C; Ahluwalia, Tarun Veer Singh; Perälä, Mia-Maria; Jonsson, Anna; Muka, Taulant; Kalafati, Ioanna P; Mikkilä, Vera; Ordovás, José M; CHARGE Nutrition Study Group.

In: Diabetes Care, Vol. 38, No. 8, 08.2015, p. 1456-66.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Dashti, HS, Follis, JL, Smith, CE, Tanaka, T, Garaulet, M, Gottlieb, DJ, Hruby, A, Jacques, PF, Kiefte-de Jong, JC, Lamon-Fava, S, Scheer, FAJL, Bartz, TM, Kovanen, L, Wojczynski, MK, Frazier-Wood, AC, Ahluwalia, TVS, Perälä, M-M, Jonsson, A, Muka, T, Kalafati, IP, Mikkilä, V, Ordovás, JM & CHARGE Nutrition Study Group 2015, 'Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits', Diabetes Care, vol. 38, no. 8, pp. 1456-66. https://doi.org/10.2337/dc14-2709

APA

Dashti, H. S., Follis, J. L., Smith, C. E., Tanaka, T., Garaulet, M., Gottlieb, D. J., Hruby, A., Jacques, P. F., Kiefte-de Jong, J. C., Lamon-Fava, S., Scheer, F. A. J. L., Bartz, T. M., Kovanen, L., Wojczynski, M. K., Frazier-Wood, A. C., Ahluwalia, T. V. S., Perälä, M-M., Jonsson, A., Muka, T., ... CHARGE Nutrition Study Group (2015). Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits. Diabetes Care, 38(8), 1456-66. https://doi.org/10.2337/dc14-2709

Vancouver

Dashti HS, Follis JL, Smith CE, Tanaka T, Garaulet M, Gottlieb DJ et al. Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits. Diabetes Care. 2015 Aug;38(8):1456-66. https://doi.org/10.2337/dc14-2709

Author

Dashti, Hassan S ; Follis, Jack L ; Smith, Caren E ; Tanaka, Toshiko ; Garaulet, Marta ; Gottlieb, Daniel J ; Hruby, Adela ; Jacques, Paul F ; Kiefte-de Jong, Jessica C ; Lamon-Fava, Stefania ; Scheer, Frank A J L ; Bartz, Traci M ; Kovanen, Leena ; Wojczynski, Mary K ; Frazier-Wood, Alexis C ; Ahluwalia, Tarun Veer Singh ; Perälä, Mia-Maria ; Jonsson, Anna ; Muka, Taulant ; Kalafati, Ioanna P ; Mikkilä, Vera ; Ordovás, José M ; CHARGE Nutrition Study Group. / Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits. In: Diabetes Care. 2015 ; Vol. 38, No. 8. pp. 1456-66.

Bibtex

@article{6b6e435777ad40179395bcc113eea246,
title = "Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits",
abstract = "OBJECTIVE: Common circadian-related gene variants associate with increased risk for metabolic alterations including type 2 diabetes. However, little is known about whether diet and sleep could modify associations between circadian-related variants (CLOCK-rs1801260, CRY2-rs11605924, MTNR1B-rs1387153, MTNR1B-rs10830963, NR1D1-rs2314339) and cardiometabolic traits (fasting glucose [FG], HOMA-insulin resistance, BMI, waist circumference, and HDL-cholesterol) to facilitate personalized recommendations.RESEARCH DESIGN AND METHODS: We conducted inverse-variance weighted, fixed-effect meta-analyses of results of adjusted associations and interactions between dietary intake/sleep duration and selected variants on cardiometabolic traits from 15 cohort studies including up to 28,190 participants of European descent from the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium.RESULTS: We observed significant associations between relative macronutrient intakes and glycemic traits and short sleep duration (<7 h) and higher FG and replicated known MTNR1B associations with glycemic traits. No interactions were evident after accounting for multiple comparisons. However, we observed nominally significant interactions (all P < 0.01) between carbohydrate intake and MTNR1B-rs1387153 for FG with a 0.003 mmol/L higher FG with each additional 1% carbohydrate intake in the presence of the T allele, between sleep duration and CRY2-rs11605924 for HDL-cholesterol with a 0.010 mmol/L higher HDL-cholesterol with each additional hour of sleep in the presence of the A allele, and between long sleep duration (≥9 h) and MTNR1B-rs1387153 for BMI with a 0.60 kg/m(2) higher BMI with long sleep duration in the presence of the T allele relative to normal sleep duration (≥7 to <9 h).CONCLUSIONS: Our results suggest that lower carbohydrate intake and normal sleep duration may ameliorate cardiometabolic abnormalities conferred by common circadian-related genetic variants. Until further mechanistic examination of the nominally significant interactions is conducted, recommendations applicable to the general population regarding diet—specifically higher carbohydrate and lower fat composition—and normal sleep duration should continue to be emphasized among individuals with the investigated circadian-related gene variants.",
author = "Dashti, {Hassan S} and Follis, {Jack L} and Smith, {Caren E} and Toshiko Tanaka and Marta Garaulet and Gottlieb, {Daniel J} and Adela Hruby and Jacques, {Paul F} and {Kiefte-de Jong}, {Jessica C} and Stefania Lamon-Fava and Scheer, {Frank A J L} and Bartz, {Traci M} and Leena Kovanen and Wojczynski, {Mary K} and Frazier-Wood, {Alexis C} and Ahluwalia, {Tarun Veer Singh} and Mia-Maria Per{\"a}l{\"a} and Anna Jonsson and Taulant Muka and Kalafati, {Ioanna P} and Vera Mikkil{\"a} and Ordov{\'a}s, {Jos{\'e} M} and {CHARGE Nutrition Study Group}",
note = "{\textcopyright} 2015 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered.",
year = "2015",
month = aug,
doi = "10.2337/dc14-2709",
language = "English",
volume = "38",
pages = "1456--66",
journal = "Diabetes Care",
issn = "0149-5992",
publisher = "American Diabetes Association",
number = "8",

}

RIS

TY - JOUR

T1 - Gene-Environment Interactions of Circadian-Related Genes for Cardiometabolic Traits

AU - Dashti, Hassan S

AU - Follis, Jack L

AU - Smith, Caren E

AU - Tanaka, Toshiko

AU - Garaulet, Marta

AU - Gottlieb, Daniel J

AU - Hruby, Adela

AU - Jacques, Paul F

AU - Kiefte-de Jong, Jessica C

AU - Lamon-Fava, Stefania

AU - Scheer, Frank A J L

AU - Bartz, Traci M

AU - Kovanen, Leena

AU - Wojczynski, Mary K

AU - Frazier-Wood, Alexis C

AU - Ahluwalia, Tarun Veer Singh

AU - Perälä, Mia-Maria

AU - Jonsson, Anna

AU - Muka, Taulant

AU - Kalafati, Ioanna P

AU - Mikkilä, Vera

AU - Ordovás, José M

AU - CHARGE Nutrition Study Group

N1 - © 2015 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered.

PY - 2015/8

Y1 - 2015/8

N2 - OBJECTIVE: Common circadian-related gene variants associate with increased risk for metabolic alterations including type 2 diabetes. However, little is known about whether diet and sleep could modify associations between circadian-related variants (CLOCK-rs1801260, CRY2-rs11605924, MTNR1B-rs1387153, MTNR1B-rs10830963, NR1D1-rs2314339) and cardiometabolic traits (fasting glucose [FG], HOMA-insulin resistance, BMI, waist circumference, and HDL-cholesterol) to facilitate personalized recommendations.RESEARCH DESIGN AND METHODS: We conducted inverse-variance weighted, fixed-effect meta-analyses of results of adjusted associations and interactions between dietary intake/sleep duration and selected variants on cardiometabolic traits from 15 cohort studies including up to 28,190 participants of European descent from the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium.RESULTS: We observed significant associations between relative macronutrient intakes and glycemic traits and short sleep duration (<7 h) and higher FG and replicated known MTNR1B associations with glycemic traits. No interactions were evident after accounting for multiple comparisons. However, we observed nominally significant interactions (all P < 0.01) between carbohydrate intake and MTNR1B-rs1387153 for FG with a 0.003 mmol/L higher FG with each additional 1% carbohydrate intake in the presence of the T allele, between sleep duration and CRY2-rs11605924 for HDL-cholesterol with a 0.010 mmol/L higher HDL-cholesterol with each additional hour of sleep in the presence of the A allele, and between long sleep duration (≥9 h) and MTNR1B-rs1387153 for BMI with a 0.60 kg/m(2) higher BMI with long sleep duration in the presence of the T allele relative to normal sleep duration (≥7 to <9 h).CONCLUSIONS: Our results suggest that lower carbohydrate intake and normal sleep duration may ameliorate cardiometabolic abnormalities conferred by common circadian-related genetic variants. Until further mechanistic examination of the nominally significant interactions is conducted, recommendations applicable to the general population regarding diet—specifically higher carbohydrate and lower fat composition—and normal sleep duration should continue to be emphasized among individuals with the investigated circadian-related gene variants.

AB - OBJECTIVE: Common circadian-related gene variants associate with increased risk for metabolic alterations including type 2 diabetes. However, little is known about whether diet and sleep could modify associations between circadian-related variants (CLOCK-rs1801260, CRY2-rs11605924, MTNR1B-rs1387153, MTNR1B-rs10830963, NR1D1-rs2314339) and cardiometabolic traits (fasting glucose [FG], HOMA-insulin resistance, BMI, waist circumference, and HDL-cholesterol) to facilitate personalized recommendations.RESEARCH DESIGN AND METHODS: We conducted inverse-variance weighted, fixed-effect meta-analyses of results of adjusted associations and interactions between dietary intake/sleep duration and selected variants on cardiometabolic traits from 15 cohort studies including up to 28,190 participants of European descent from the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium.RESULTS: We observed significant associations between relative macronutrient intakes and glycemic traits and short sleep duration (<7 h) and higher FG and replicated known MTNR1B associations with glycemic traits. No interactions were evident after accounting for multiple comparisons. However, we observed nominally significant interactions (all P < 0.01) between carbohydrate intake and MTNR1B-rs1387153 for FG with a 0.003 mmol/L higher FG with each additional 1% carbohydrate intake in the presence of the T allele, between sleep duration and CRY2-rs11605924 for HDL-cholesterol with a 0.010 mmol/L higher HDL-cholesterol with each additional hour of sleep in the presence of the A allele, and between long sleep duration (≥9 h) and MTNR1B-rs1387153 for BMI with a 0.60 kg/m(2) higher BMI with long sleep duration in the presence of the T allele relative to normal sleep duration (≥7 to <9 h).CONCLUSIONS: Our results suggest that lower carbohydrate intake and normal sleep duration may ameliorate cardiometabolic abnormalities conferred by common circadian-related genetic variants. Until further mechanistic examination of the nominally significant interactions is conducted, recommendations applicable to the general population regarding diet—specifically higher carbohydrate and lower fat composition—and normal sleep duration should continue to be emphasized among individuals with the investigated circadian-related gene variants.

U2 - 10.2337/dc14-2709

DO - 10.2337/dc14-2709

M3 - Journal article

C2 - 26084345

VL - 38

SP - 1456

EP - 1466

JO - Diabetes Care

JF - Diabetes Care

SN - 0149-5992

IS - 8

ER -

ID: 150710336