Association between leptin receptor (LEPR) and brain-derived neurotrophic factor (BDNF) gene variants and obesity: a case-control study

Marti, A.; Santos, J. L.; Gratacos, M.; Moreno Aliaga, M. J.; Maiz, A.; Martinez, J. A.; Estivill, X.

artículo

Fecha

2009

Registro en:

10.1179/147683009X423355

1476-8305

1028-415X

MEDLINE:19622243

https://doi.org/10.1179/147683009X423355

https://repositorio.uc.cl/handle/11534/75775

WOS:000267975700007

Autor

Marti, A.

Santos, J. L.

Gratacos, M.

Moreno Aliaga, M. J.

Maiz, A.

Martinez, J. A.

Estivill, X.

Institución

Pontificia Universidad Católica de Chile

Resumen

Introduction: Human and animal studies provide evidence for a relevant role of the leptin receptor (LEPR) and the brain-derived neurotrophic factor (BDNF) genes in energy homeostasis.

Aim: To assess the association between human LEPR and BDNF genetic variants with adult obesity. Design and methods: Case-control study in Pamplona (Navarra, Spain) with adult obese subjects (n = 159) and normal weight controls (n = 154) Four common polymorphisms of the LEPR gene (Lys109Arg, Gln223Arg, Ser34Ser, Lys656Asn) and 17 variants of the BDNF gene, including the Val66Met variant, were genotyped.

Results: No significant case-control differences were found in allele/genotype frequencies after adjusting for relevant co-variates. Haplotype analysis did not detect any significant association between LEPR or BDNF variants and obesity. No associations were found between LEPR variants and serum leptin levels.

Conclusions: Our results do not support a major role of LEPR or BDNF common polymorphisms in multifactorial adult obesity.

Materias

obesity

leptin receptor

brain-derived neurotrophic factor

case-control study

BODY-MASS INDEX

ANOREXIA-NERVOSA

WEIGHT

RISK

SPECTRUM

EXTREME

LINKAGE

GAIN

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