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Identification of a Rare and Potential Pathogenic MC4R Variant in a Brazilian Patient With Adulthood-Onset Severe Obesity

Kaio Cezar Rodrigues Salum, Guilherme Orofino de Souza, Gabriella de Medeiros Abreu, Mário Campos, Fabiana B. Kohlrausch, João Régis Ivar Carneiro, José Firmino Nogueira Neto, Fernanda Cristina Carvalho Mattos Magno, Eliane Lopes Rosado, Lohanna Palhinha, Clarissa M. Maya‐Monteiro, Giselda Maria Kalil de Cabello, Pedro Hernán Cabello, Patrı́cia T. Bozza, Verônica Marques Zembrzuski, Ana Carolina Proença da Fonseca

2020Frontiers in Genetics10 citationsDOIOpen Access PDF

Abstract

Background The melanocortinergic pathway orchestrates the energy homeostasis and impairments in this system often lead to an increase in body weight. Rare variants in the melanocortin 4 receptor ( MC4R ) gene resulting in partial or complete loss of function have been described with autosomal co-dominant inheritance. These mutations are the most common cause of non-syndromic monogenic obesity. In this context, this study aimed to sequence the MC4R gene in a Brazilian cohort of adults with severe obesity. Methods This study included 163 unrelated probands with Body Mass Index (BMI) ≥ 35 kg/m 2 , stratified into three groups, according to the period of obesity onset. From the total sample, 25 patients were enrolled in the childhood-onset group (0–11 years), 19 patients in the adolescence/youth-onset group (12–21 years), and 119 patients in the adult-onset group (>21 years). Blood pressure, anthropometric and biochemical characteristics were obtained, and the MC4R coding region of each subject’s DNA was assessed using automated Sanger sequencing. Results Significant anthropometric differences between the groups were observed. Higher body weight and BMI medians were found in patients with childhood-onset or adolescence/youth-onset when compared to the adulthood-onset obesity group. A total of five mutations were identified, including four missense variants: p.Ser36Thr, p.Val103Ile, p.Ala175Thr, and p.Ile251Leu. Additionally, we observed one synonymous variant (p.Ile198=). The p.Ala175Thr variant was identified in a female case with severe obesity and adulthood-onset. This variant was previously described as a partial loss-of-function mutation, in which the minor allele poses dominant-negative effect, probably resulting in reduced cAMP activity. Conclusion This study showed a prevalence of common and rare variants in a cohort of Brazilian adults with severe obesity and candidates to bariatric surgery. We have identified a rare potentially pathogenic MC4R variant in a Brazilian patient with severe and adulthood-onset obesity.

Topics & Concepts

ObesityMissense mutationBody mass indexSanger sequencingMelanocortin 4 receptorMedicineContext (archaeology)CohortChildhood obesityInternal medicineProbandAge of onsetPediatricsEndocrinologyBiologyGeneticsMutationOverweightGeneDiseaseMelanocortinReceptorPaleontologyPancreatic function and diabetesGenomics and Rare DiseasesAdipose Tissue and Metabolism
Identification of a Rare and Potential Pathogenic MC4R Variant in a Brazilian Patient With Adulthood-Onset Severe Obesity | Litcius