The body mass index increases the genetic risk scores' ability to predict risk of hepatic damage in European adolescents: The HELENA study

Author:

Seral‐Cortes Miguel12ORCID,Sabroso‐Lasa Sergio3ORCID,Gonzalez‐Gross Marcela245ORCID,Quesada‐Gonzalez Carlos46ORCID,Stehle Peter5ORCID,Gottrand Frederic7ORCID,Marcos Ascension28,Esperanza‐Diaz Ligia8ORCID,Manios Yannis910ORCID,Androutsos Odysseas11ORCID,Widhalm Kurt1213ORCID,Molnar Denes14ORCID,Huybrechts Inge1516ORCID,Muntaner Manon17,Meirhaeghe Aline17ORCID,Salazar‐Tortosa Diego18ORCID,Ruiz Jonatan R.21920ORCID,Esteban Luis Mariano21,Labayen Idoia222ORCID,Moreno Luis A.12ORCID,

Affiliation:

1. Growth, Exercise, Nutrition and Development (GENUD) Research Group, Faculty of Health Sciences Instituto Agroalimentario de Aragón (IA2), Instituto de Investigación Sanitaria Aragón (IIS Aragón), Universidad de Zaragoza Zaragoza Spain

2. CIBER Fisiopatología de la Obesidad y Nutrición (CIBERobn) Instituto de Salud Carlos III Madrid Spain

3. Genetic and Molecular Epidemiology Group (GMEG), Spanish National Cancer Research Centre (CNIO) Madrid Spain

4. ImFine Research Group, Department of Health and Human Performance, Facultad de Ciencias de la Actividad Física y del Deporte‐INEF Universidad Politécnica de Madrid Madrid Spain

5. Institute of Nutritional and Food Sciences, Nutritional Physiology University of Bonn Bonn Germany

6. Department of Applied Mathematics to Information and Communication Technologies Universidad Politécnica de Madrid Madrid Spain

7. CHU Lille, Inserm U1286 INFINITE University of Lille Lille France

8. Immunonutrition Group, Department of Metabolism and Nutrition Institute of Food Science, Technology and Nutrition (ICTAN), Spanish National Research Council (CSIC) Madrid Spain

9. Department of Nutrition and Dietetics, School of Health Science & Education Harokopio University Athens Greece

10. Institute of Agri‐food and Life Sciences Hellenic Mediterranean University Research Centre Heraklion Greece

11. Lab of Clinical Nutrition and Dietetics, Department of Nutrition and Dietetics, School of Physical Education, Sport Science and Dietetics University of Thessaly Trikala Greece

12. Division of Clinical Nutrition and Prevention, Department of Paediatrics Medical University of Vienna Vienna Austria

13. Austrian Academic Institute for Clinical Nutrition Vienna Austria

14. Department of Pediatrics, Medical School University of Pécs Pécs Hungary

15. International Agency for Research on Cancer, World Health Organization Lyon France

16. French Network for Nutrition and Cancer Research (NACRe network) Jouy‐en‐Josas France

17. UMR1167, RID‐AGE, Risk Factors and Molecular Determinants of Aging‐Related Diseases, Centre Hosp, Institut Pasteur de Lille Université de Lille Lille France

18. Department of Ecology and Evolutionary Biology University of Arizona Tucson Arizona USA

19. Department of Physical Education and Sports, Faculty of Sports Science Sport and Health University Research Institute (iMUDS) Granada Spain

20. Instituto de Investigación Biosanitaria, ibs.Granada Granada Spain

21. Escuela Politécnica de La Almunia Universidad de Zaragoza Zaragoza Spain

22. Department of Health Sciences Public University of Navarra Pamplona Spain

Abstract

AbstractBackgroundHepatic disorders are often complex and multifactorial, modulated by genetic and environmental determinants. During the last years, the hepatic disease has been progressively established from early stages in life. The use of genetic risk scores (GRS) to predict the genetic susceptibility to a particular phenotype among youth has gained interest in recent years. Moreover, the alanine aminotransferase (ALT) blood biomarker is often considered as hepatic screening tool, in combination with imaging techniques. The aim of the present study was to develop an ALT‐specific GRS to help in the evaluation of hepatic damage risk in European adolescents.MethodsA total of 972 adolescents (51.3% females), aged 12.5–17.5 years, from the Healthy Lifestyle in Europe by Nutrition in Adolescence study were included in the analyses. The sample incorporated adolescents in all body mass index (BMI) categories and was divided considering healthy/unhealthy ALT levels, using sex‐specific cut‐off points. From 1212 a priori ALT‐related single nucleotide polymorphisms (SNPs) extracted from candidate gene selection, a first screening of 234 SNPs univariately associated was established, selecting seven significant SNPs (p < .05) in the multivariate model. An unweighted GRS (uGRS) was developed by summing the number of reference alleles, and a weighted GRS (wGRS), by multiplying each allele to its estimated coefficient.ResultsThe uGRS and wGRS were significantly associated with ALT (p < .001). The area under curve was obtained integrating BMI as clinical factor, improving the predictive ability for uGRS (.7039) and wGRS (.7035), using 10‐fold internal cross‐validation.ConclusionsConsidering BMI status, both GRSs could contribute as complementary tools to help in the early diagnosis of hepatic damage risk in European adolescents.

Publisher

Wiley

Subject

Clinical Biochemistry,Biochemistry,General Medicine

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