Open Access Green as soon as Postprint is submitted to ZB.
Meta-analysis of two genome-wide association studies identifies four genetic loci associated with thyroid function.
Hum. Mol. Genet. 21, 3275-3282 (2012)
Thyroid hormones play key roles in cellular growth, development and metabolism. Although there is a strong genetic influence on thyroid hormone levels, the genes involved are widely unknown. The levels of circulating thyroid hormones are tightly regulated by thyrotropin (TSH), which also represents the most important diagnostic marker for thyroid function. Therefore, in order to identify genetic loci associated with TSH levels, we performed a discovery meta-analysis of two genome-wide association studies including two cohorts from Germany, KORA (n 1287) and SHIP (n 2449), resulting in a total sample size of 3736. Four genetic loci at 5q13.3, 1p36, 16q23 and 4q31 were associated with serum TSH levels. The lead single-nucleotide polymorphisms of these four loci were located within PDE8B encoding phosphodiesterase 8B, upstream of CAPZB that encodes the -subunit of the barbed-end F-actin-binding protein, in a former ogene desert' that was recently demonstrated to encode a functional gene (LOC440389) associated with thyroid volume, and upstream of NR3C2 encoding the mineralocorticoid receptor. The latter association for the first time suggests the modulation of thyroid function by mineral corticoids. All four loci were replicated in three additional cohorts: the HUNT study from Norway (n 1487) and the two German studies CARLA (CARLA, n 1357) and SHIP-TREND (n 883). Together, these four quantitative trait loci accounted for approximate to 3.3 of the variance in TSH serum levels. These results contribute to our understanding of genetic factors and physiological mechanisms mediating thyroid function.
Edit extra informations Login
Publication type Article: Journal article
Document type Scientific Article
Keywords SERUM TSH; FEEDBACK-REGULATION; AXIS; THYROTROPIN; VARIANTS; DISEASE; STRESS; EXCESS
ISSN (print) / ISBN 0964-6906
Journal Human Molecular Genetics
Quellenangaben Volume: 21, Issue: 14, Pages: 3275-3282
Publisher Oxford University Press
Reviewing status Peer reviewed