GAD2 on Chromosome 10p12 Is a Candidate Gene for Human Obesity | Zendy

Philippe Boutin | Zendy; Christian Dina | Zendy; Francis Vasseur | Zendy; Séverine Dubois | Zendy; Laetitia Corset | Zendy; Karin Séron | Zendy; Lynn M. Bekris | Zendy; Janice Cabellon | Zendy; Bernadette Neve | Zendy; Valérie Vasseur-Delannoy | Zendy; Mohamed Chikri | Zendy; MarieAline Charles | Zendy; Karine Clément | Zendy; Åke Lernmark | Zendy; Philippe Froguel | Zendy

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GAD2 on Chromosome 10p12 Is a Candidate Gene for Human Obesity

Author(s) -

Philippe Boutin,

Christian Dina,

Francis Vasseur,

Séverine Dubois,

Laetitia Corset,

Karin Séron,

Lynn M. Bekris,

Janice Cabellon,

Bernadette Neve,

Valérie Vasseur-Delannoy,

Mohamed Chikri,

MarieAline Charles,

Karine Clément,

Åke Lernmark,

Philippe Froguel

Publication year - 2003

Publication title -

plos biology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 4.127

H-Index - 271

eISSN - 1545-7885

pISSN - 1544-9173

DOI - 10.1371/journal.pbio.0000068

Subject(s) - biology , single nucleotide polymorphism , haplotype , genetics , snp , candidate gene , allele , glutamate decarboxylase , endocrinology , medicine , gene , genotype , enzyme , biochemistry

The gene GAD2 encoding the glutamic acid decarboxylase enzyme (GAD65) is a positional candidate gene for obesity on Chromosome 10p11-12, a susceptibility locus for morbid obesity in four independent ethnic populations. GAD65 catalyzes the formation of gamma-aminobutyric acid (GABA), which interacts with neuropeptide Y in the paraventricular nucleus to contribute to stimulate food intake. A case-control study (575 morbidly obese and 646 control subjects) analyzing GAD2 variants identified both a protective haplotype, including the most frequent alleles of single nucleotide polymorphisms (SNPs) +61450 C>A and +83897 T>A (OR = 0.81, 95% CI [0.681-0.972], p = 0.0049) and an at-risk SNP (-243 A>G) for morbid obesity (OR = 1.3, 95% CI [1.053-1.585], p = 0.014). Furthermore, familial-based analyses confirmed the association with the obesity of SNP +61450 C>A and +83897 T>A haplotype (chi(2) = 7.637, p = 0.02). In the murine insulinoma cell line betaTC3, the G at-risk allele of SNP -243 A>G increased six times GAD2 promoter activity (p < 0.0001) and induced a 6-fold higher affinity for nuclear extracts. The -243 A>G SNP was associated with higher hunger scores (p = 0.007) and disinhibition scores (p = 0.028), as assessed by the Stunkard Three-Factor Eating Questionnaire. As GAD2 is highly expressed in pancreatic beta cells, we analyzed GAD65 antibody level as a marker of beta-cell activity and of insulin secretion. In the control group, -243 A>G, +61450 C>A, and +83897 T>A SNPs were associated with lower GAD65 autoantibody levels (p values of 0.003, 0.047, and 0.006, respectively). SNP +83897 T>A was associated with lower fasting insulin and insulin secretion, as assessed by the HOMA-B% homeostasis model of beta-cell function (p = 0.009 and 0.01, respectively). These data support the hypothesis of the orexigenic effect of GABA in humans and of a contribution of genes involved in GABA metabolism in the modulation of food intake and in the development of morbid obesity

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