Next-generation sequencing of the monogenic obesity genes LEP, LEPR, MC4R, PCSK1 and POMC in a Norwegian cohort of patients with morbid obesity and normal weight controls

Gry B N Nordang; Øyvind L Busk; Kristian Tveten; Hans Ivar Hanevik; Anne Kristin M Fell; Jøran Hjelmesæth; Øystein L Holla; Jens K Hertel

doi:10.1016/j.ymgme.2017.03.007

Next-generation sequencing of the monogenic obesity genes LEP, LEPR, MC4R, PCSK1 and POMC in a Norwegian cohort of patients with morbid obesity and normal weight controls

Mol Genet Metab. 2017 May;121(1):51-56. doi: 10.1016/j.ymgme.2017.03.007. Epub 2017 Mar 29.

Authors

Gry B N Nordang¹, Øyvind L Busk², Kristian Tveten², Hans Ivar Hanevik³, Anne Kristin M Fell⁴, Jøran Hjelmesæth⁵, Øystein L Holla², Jens K Hertel⁶

Affiliations

¹ Morbid Obesity Centre, Vestfold Hospital Trust, Tønsberg, Norway; Department of Occupational and Environmental Medicine, Telemark Hospital, Skien, Norway; Section of Medical Genetics, Department of Laboratory Medicine, Telemark Hospital, Skien, Norway. Electronic address: grynor@sthf.no.
² Section of Medical Genetics, Department of Laboratory Medicine, Telemark Hospital, Skien, Norway.
³ Fertilitetsavdelingen Sør, Telemark Hospital, Porsgrunn, Norway.
⁴ Department of Occupational and Environmental Medicine, Telemark Hospital, Skien, Norway.
⁵ Morbid Obesity Centre, Vestfold Hospital Trust, Tønsberg, Norway; Department of Endocrinology, Morbid Obesity and Preventive Medicine, Institute of Clinical Medicine, University of Oslo, Oslo, Norway.
⁶ Morbid Obesity Centre, Vestfold Hospital Trust, Tønsberg, Norway.

PMID: 28377240
DOI: 10.1016/j.ymgme.2017.03.007

Abstract

Background: Rare sequence variants in at least five genes are known to cause monogenic obesity. In this study we aimed to investigate the prevalence of, and characterize, rare coding and splice site variants in LEP, LEPR, MC4R, PCSK1 and POMC in patients with morbid obesity and normal weight controls.

Method: Targeted next-generation sequencing of all exons in LEP, LEPR, MC4R, PCSK1 and POMC was performed in 485 patients with morbid obesity and 327 normal weight population-based controls from Norway.

Results: In total 151 variants were detected. Twenty-eight (18.5%) of these were rare, coding or splice variants and five (3.3%) were novel. All individuals, except one control, were heterozygous for the 28 variants, and the distribution of the rare variants showed a significantly higher carrier frequency among cases than controls (9.9% vs. 4.9%, p=0.011). Four variants in MC4R were classified as pathogenic or likely pathogenic.

Conclusion: Four cases (0.8%) of monogenic obesity were detected, all due to MC4R variants previously linked to monogenic obesity. Significant differences in carrier frequencies among patients with morbid obesity and normal weight controls suggest an association between heterozygous rare coding variants in these five genes and morbid obesity. However, additional studies in larger cohorts and functional testing of the novel variants identified are required to confirm the findings.

Keywords: BMI; Morbid obesity; Mutation; Next-generation sequencing; Rare sequence variant.

MeSH terms

Adolescent
Adult
Age Distribution
Case-Control Studies
Child
Female
Genetic Predisposition to Disease
Genetic Variation*
High-Throughput Nucleotide Sequencing / methods*
Humans
Leptin / genetics
Male
Middle Aged
Mutation Rate
Norway
Obesity, Morbid / genetics*
Pro-Opiomelanocortin / genetics
Proprotein Convertase 1 / genetics
Receptor, Melanocortin, Type 4 / genetics
Receptors, Leptin / genetics
Sequence Analysis, DNA / methods*
Young Adult

Substances

LEPR protein, human
Leptin
MC4R protein, human
Receptor, Melanocortin, Type 4
Receptors, Leptin
Pro-Opiomelanocortin
PCSK1 protein, human
Proprotein Convertase 1