4.7 Article

Rare Variant Analysis of Obesity-Associated Genes in Young Adults With Severe Obesity From a Consanguineous Population of Pakistan

Journal

DIABETES
Volume 71, Issue 4, Pages 694-705

Publisher

AMER DIABETES ASSOC
DOI: 10.2337/db21-0373

Keywords

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Funding

  1. Medical Research Council (MRC) [MR/S026193/1]
  2. Pakistan Academy of Sciences [MA-03]
  3. French National Research Agency [ANR-10-LABX-46, ANR-10-EQPX-07-01]
  4. European Research Council [ERC GEPIDIAB - 294785, ERC Reg-Seq 7155575]
  5. European Union (FEDER)
  6. Hauts-de-France Regional Council
  7. European Metropolis of Lille (MEL)
  8. National Center for Precision Diabetic Medicine - PreciDIAB - French National Agency for Research [ANR-18-IBHU0001]

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Recent advances in genetic analysis have helped understand the genetic basis of obesity, specifically the disruption of melanocortin signaling by monogenic variants. In this study, rare variants in obesity-causing genes were assessed in young adults with severe obesity from Pakistan. Thirteen subjects were found to carry pathogenic variants in different obesity-related genes, including two homozygous stop-gain mutations in previously unreported genes. Homozygous mutations and copy-loss CNVs in genes previously linked to obesity were also identified. Notably, pathogenic mutations in LEP and LEPR were rarely found in this cohort of young adults, possibly due to differences in morbidity and social disadvantage compared to obese children.
Recent advances in genetic analysis have significantly helped in progressively attenuating the heritability gap of obesity and have brought into focus monogenic variants that disrupt the melanocortin signaling. In a previous study, next-generation sequencing revealed a monogenic etiology in similar to 50% of the children with severe obesity from a consanguineous population in Pakistan. Here we assess rare variants in obesity-causing genes in young adults with severe obesity from the same region. Genomic DNA from 126 randomly selected young adult obese subjects (BMI 37.2 +/- 0.3 kg/m(2); age 18.4 +/- 0.3 years) was screened by conventional or augmented whole-exome analysis for point mutations and copy number variants (CNVs). Leptin, insulin, and cortisol levels were measured by ELISA. We identified 13 subjects carrying 13 different pathogenic or likely pathogenic variants in LEPR, PCSK1, MC4R, NTRK2, POMC, SH2B1, and SIM1. We also identified for the first time in the human, two homozygous stop-gain mutations in ASNSD1 and IFI16 genes. Inactivation of these genes in mouse models has been shown to result in obesity. Additionally, we describe nine homozygous mutations (seven missense, one stop-gain, and one stop-loss) and four copy-loss CNVs in genes or genomic regions previously linked to obesity-associated traits by genome-wide association studies. Unexpectedly, in contrast to obese children, pathogenic mutations in LEP and LEPR were either absent or rare in this cohort of young adults. High morbidity and mortality risks and social disadvantage of children with LEP or LEPR deficiency may in part explain this difference between the two cohorts.

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