Effect of the Melanocortin 4-Receptor Ile269Asn Mutation on Weight Loss Response to Dietary, Phentermine and Bariatric Surgery Interventions

Author:

Salazar-Valencia Itzel G.,Villamil-Ramírez Hugo,Barajas-Olmos FranciscoORCID,Guevara-Cruz MarthaORCID,Macias-Kauffer Luis R.ORCID,García-Ortiz HumbertoORCID,Hernández-Vergara Omar,Díaz de Sandy-Galán David Alberto,León-Mimila Paola,Centeno-Cruz FedericoORCID,González-Salazar Luis E.ORCID,Guizar-Heredia Rocío,Pichardo-Ontiveros Edgar,Jacobo-Albavera LeonorORCID,Posadas-Sánchez RosalindaORCID,Vargas-Alarcón GilbertoORCID,Velazquez-Cruz RafaelORCID,Gutiérrez-Aguilar RuthORCID,Zerrweck Carlos,Rocha-González Héctor IsaacORCID,Reyes-García Juan GerardoORCID,Carrasco-Portugal Miriam del C.,Flores-Murrieta Francisco Javier,Tovar Armando R.,Orozco Lorena,Villarreal-Molina TeresaORCID,Canizales-Quinteros SamuelORCID

Abstract

The loss of function melanocortin 4-receptor (MC4R) Ile269Asn mutation has been proposed as one of the most important genetic contributors to obesity in the Mexican population. However, whether patients bearing this mutation respond differently to weight loss treatments is unknown. We tested the association of this mutation with obesity in 1683 Mexican adults, and compared the response of mutation carriers and non-carriers to three different weight loss interventions: dietary restriction intervention, phentermine 30 mg/day treatment, and Roux-en-Y gastric bypass (RYGB) surgery. The Ile269Asn mutation was associated with obesity [OR = 3.8, 95% CI (1.5–9.7), p = 0.005]. Regarding interventions, in the dietary restriction group only two patients were MC4R Ile269Asn mutation carriers. After 1 month of treatment, both mutation carriers lost weight: −4.0 kg (−2.9%) in patient 1, and −1.8 kg (−1.5%) in patient 2; similar to the mean weight loss observed in six non-carrier subjects (−2.9 kg; −2.8%). Phentermine treatment produced similar weight loss in six carriers (−12.7 kg; 15.5%) and 18 non-carriers (−11.3 kg; 13.6%) after 6 months of pharmacological treatment. RYGB also caused similar weight loss in seven carriers (29.9%) and 24 non-carriers (27.8%), 6 months after surgery. Our findings suggest that while the presence of a single MC4R loss of function Ile269Asn allele significantly increases obesity risk, the presence of at least one functional MC4R allele seems sufficient to allow short-term weight loss in response to dietary restriction, phentermine and RYGB. Thus, these three different interventions may be useful for the short-term treatment of obesity in MC4R Ile269Asn mutation carriers.

Funder

CONACyT-PEI

CONACyT-FOSISS

CONACyT scholarship

Publisher

MDPI AG

Subject

Genetics (clinical),Genetics

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