Heterozygous Mutations Causing Partial Prohormone Convertase 1 Deficiency Contribute to Human Obesity

Overview

Journal Diabetes

Specialty Endocrinology

Date 2012 Jan 3

PMID 22210313

Citations 49

Authors

John W M Creemers

Helene Choquet

Pieter Stijnen

Vincent Vatin

Marie Pigeyre

Sigri Beckers

Sandra Meulemans

Manuel E Than

Loic Yengo

Maithe Tauber

Beverley Balkau

Paul Elliott

Marjo-Riitta Jarvelin

Wim Van Hul

Luc Van Gaal

Fritz Horber

Francois Pattou

Philippe Froguel

David Meyre

Affiliations

Soon will be listed here.

Abstract

Null mutations in the PCSK1 gene, encoding the proprotein convertase 1/3 (PC1/3), cause recessive monogenic early onset obesity. Frequent coding variants that modestly impair PC1/3 function mildly increase the risk for common obesity. The aim of this study was to determine the contribution of rare functional PCSK1 mutations to obesity. PCSK1 exons were sequenced in 845 nonconsanguineous extremely obese Europeans. Eight novel nonsynonymous PCSK1 mutations were identified, all heterozygous. Seven mutations had a deleterious effect on either the maturation or the enzymatic activity of PC1/3 in cell lines. Of interest, five of these novel mutations, one of the previously described frequent variants (N221D), and the mutation found in an obese mouse model (N222D), affect residues at or near the structural calcium binding site Ca-1. The prevalence of the newly identified mutations was assessed in 6,233 obese and 6,274 lean European adults and children, which showed that carriers of any of these mutations causing partial PCSK1 deficiency had an 8.7-fold higher risk to be obese than wild-type carriers. These results provide the first evidence of an increased risk of obesity in heterozygous carriers of mutations in the PCSK1 gene. Furthermore, mutations causing partial PCSK1 deficiency are present in 0.83% of extreme obesity phenotypes.

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