Loss-of-function mutations in ADCY3 cause monogenic severe obesity

被引:0
作者
Sadia Saeed
Amélie Bonnefond
Filippo Tamanini
Muhammad Usman Mirza
Jaida Manzoor
Qasim M. Janjua
Sadia M. Din
Julien Gaitan
Alexandra Milochau
Emmanuelle Durand
Emmanuel Vaillant
Attiya Haseeb
Franck De Graeve
Iandry Rabearivelo
Olivier Sand
Gurvan Queniat
Raphaël Boutry
Dina A. Schott
Hina Ayesha
Muhammad Ali
Waqas I. Khan
Taeed A. Butt
Tuula Rinne
Connie Stumpel
Amar Abderrahmani
Jochen Lang
Muhammad Arslan
Philippe Froguel
机构
[1] University of Lille,Centre National de la Recherche Scientifique (CNRS) UMR 8199, Institut Pasteur de Lille
[2] Imperial College London,Department of Genomics of Common Disease
[3] Katholieke Universiteit Leuven,Department of Pharmaceutical and Pharmacological Sciences, Rega Institute for Medical Research
[4] Children’s Hospital,Department of Pediatric Endocrinology
[5] University of Lahore,Centre for Research in Molecular Medicine
[6] Forman Christian College,Department of Biological Sciences
[7] UMR 5248,CNRS, Laboratory of Membrane Chemistry and Biology (CBMN)
[8] Department of Sciences and Technology,Department of Pediatrics
[9] University of Bordeaux,Department of Pediatrics
[10] Zuyderland Hospital,Department of Pediatrics, Mayo Hospital
[11] Punjab Medical College,Department of Pediatrics
[12] King Edward Medical University,Department of Human Genetics, Donders Institute for Brain, Cognition and Behavior
[13] Children Hospital and Institute of Child Health,Department of Clinical Genetics and GROW–School for Oncology and Developmental Biology
[14] Fatima Memorial Hospital,undefined
[15] Radboud University Medical Center,undefined
[16] Maastricht University Medical Center,undefined
来源
Nature Genetics | 2018年 / 50卷
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摘要
Study of monogenic forms of obesity has demonstrated the pivotal role of the central leptin–melanocortin pathway in controlling energy balance, appetite and body weight1. The majority of loss-of-function mutations (mostly recessive or co-dominant) have been identified in genes that are directly involved in leptin–melanocortin signaling. These genes, however, only explain obesity in <5% of cases, predominantly from outbred populations2. We previously showed that, in a consanguineous population in Pakistan, recessive mutations in known obesity-related genes explain ~30% of cases with severe obesity3–5. These data suggested that new monogenic forms of obesity could also be identified in this population. Here we identify and functionally characterize homozygous mutations in the ADCY3 gene encoding adenylate cyclase 3 in children with severe obesity from consanguineous Pakistani families, as well as compound heterozygous mutations in a severely obese child of European-American descent. These findings highlight ADCY3 as an important mediator of energy homeostasis and an attractive pharmacological target in the treatment of obesity.
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页码:175 / 179
页数:4
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