ESPE2024 Poster Category 2 Fat, Metabolism and Obesity (39 abstracts)
Evaluation of genetic etiology and genotype-phenotype association in endogenous obesity
Esra Koçyiğit , Selen Hürmüzlü Közler , Gözde Gürpınar , Gizem Böke Koçer , Sibel Tuğçe Aygün , Jeremy Jones & Filiz Mine Çizmecioğlu Jones
1University of Kocaeli, Kocaeli, Turkey
Introduction: Many genes have now been identified in which rare, high penetrant variants cause obesity, accounting for ~10% of children with severe obesity.
Aim: To describe clinical characteristics, genetics, and associated comorbidities in pediatirc endogenous obesity due to rare genetic obesity syndromes.
Methods: After excluding patients with obesity due to endocrine disturbances patients with BMI>2.5 SDS, early-onset obesity (<5 years) and/or any of dysmorphic features/behavioral problems/hyperphagia/family history underwent cytogenetic analysis, obesity panel screening, or next-generation WES.
Results: Of the 40 cases, 19 (40%) had a genetic etiology. Eleven (27%) had syndromic obesity; (Prader-Willi syndrome n = 10; Bardet-Biedl syndrome [BBS] n = 1). Fourteen (79%) were male and 17 (89.5%) were prepubertal. The follow-up was 4.1 (0.33-14) years and onset of obesity was 4.9 (1-10) years. Ten (52.6%) had early-onset obesity. Diagnosis age was 7.1 (0.33-14) years. BMI SDS was 2.7 (-3.1 to +7.4) and height SDS was -0.06 (-2.7 to +2.9). Sixteen (84.2%) presented with obesity, two (10.5%) with hypotonia and one (5.3%) with polyuria/polydipsia. The causes of monogenic obesity are shown in Table 1. Nine patients had monogenic obesity (Table 1) with four novel variants (Patients 6, 7, 8 and 9). 6/7 variants of unknown significance (VUS) appear to explain the phenotype, except for Patient 3. Accompanying comorbidities included: hepatosteatosis (n = 4; 21%); dyslipidemia (n = 6; 31.6%); and impaired glucose tolerance (n = 6; 31.6%). Fifteen (78.9%) had mental retardation. Type 2 diabetes developed in one patient with PWS, and in Patient 2 (P2) and P4 (Table 1). P4 had central adrenal insufficiency and central hypothroidism. P9 had polydactyly, retinitis pigmentosa, and grade 1 hydronephrosis.
Discussion: There was a marked male predominance. Four novel variants in obesity-related genes were identified. In patients whose obesity begins >5years, if there are dysmorphic findings and multisystem findings, genetic etiology should be investigated. A genetic diagnosis may be beneficial for the child and their family and suggest patients suitable for a trial of new anti-obesity therapies.
| Patient | Gene | Allele Variant | ACMG Classification | Zygosity |
| 1 | PCSK1 | c.693C>A (p. Tyr231Ter) | Pathogenic | Homozygous |
| 2 | NR0B2 | c.265C>T(p.Gln89Ter) | Pathogenic | Heterozygous |
| 3 | PPP1R3A | c.131 G>A(p.Arg44Gln) | VUS | Heterozygous |
| 4 | MC4R | c.124G>A (p. Glu42Lys) | VUS | Heterozygous |
| 5 | UCP3 | c.211A>C (p. Thr71Pro) | VUS | Heterozygous |
| 6 | LEPR | c.1938 G>T(p.Trp646Cys) c.946C>A(p.Pro316Thr) | VUS | Homozygous Homozygous |
| 7 | SH2B1 | c.558G>T (p.Glu186Asp) | VUS | Homozygous |
| 8 | NTRK2 | c.1156G>A(p.Asp386Asn) | VUS | Heterozygous |
| 9 | BBS7 | c.949C>A (p.Leu317Met) c.342G>T (p.Met114Ile) | VUS | Homozygous Homozygous |
Key Words: Monogenic obesity, syndromic obesity, obesity
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