Randomized Controlled Trial

. 2019 Nov 28;9(1):17833.

doi: 10.1038/s41598-019-54436-z.

Pharmacogenetics of amfepramone in healthy Mexican subjects reveals potential markers for tailoring pharmacotherapy of obesity: results of a randomised trial

Magdalena Gómez-Silva^{1

2}, Everardo Piñeyro-Garza³, Rigoberto Vargas-Zapata⁴, María Elena Gamino-Peña⁵, Armando León-García⁶, Mario Bermúdez de León⁷, Adrián Llerena⁸, Rafael B R León-Cachón⁹

Affiliations

¹ Forensic Medicine Service, School of Medicine, Autonomous University of Nuevo Leon, Monterrey, Nuevo Leon, Mexico.
² Analytical Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
³ Clinical Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
⁴ Quality Assurance Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
⁵ Statistical Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
⁶ Pharmaceutical Research S.A, Mexico City, CDMX, Mexico.
⁷ Department of Molecular Biology, Center for Biomedical Research of the Northeast, Mexican Institute of Social Security, Monterrey, Nuevo Leon, Mexico.
⁸ Clinical Research Center of Health Area, Hospital and Medical School of Extremadura University, Badajoz, Spain.
⁹ Center of Molecular Diagnostics and Personalized Medicine, Department of Basic Sciences, Division of Health Sciences, University of Monterrey, San Pedro Garza Garcia, Nuevo Leon, Mexico. rafael.reyesleon@udem.edu.

PMID: 31780765
PMCID: PMC6882847
DOI: 10.1038/s41598-019-54436-z

Randomized Controlled Trial

Pharmacogenetics of amfepramone in healthy Mexican subjects reveals potential markers for tailoring pharmacotherapy of obesity: results of a randomised trial

Magdalena Gómez-Silva et al. Sci Rep. 2019.

. 2019 Nov 28;9(1):17833.

doi: 10.1038/s41598-019-54436-z.

Authors

Affiliations

¹ Forensic Medicine Service, School of Medicine, Autonomous University of Nuevo Leon, Monterrey, Nuevo Leon, Mexico.
² Analytical Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
³ Clinical Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
⁴ Quality Assurance Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
⁵ Statistical Department of the Research Institute for Clinical and Experimental Pharmacology, Ipharma S.A, Monterrey, Nuevo Leon, Mexico.
⁶ Pharmaceutical Research S.A, Mexico City, CDMX, Mexico.
⁷ Department of Molecular Biology, Center for Biomedical Research of the Northeast, Mexican Institute of Social Security, Monterrey, Nuevo Leon, Mexico.
⁸ Clinical Research Center of Health Area, Hospital and Medical School of Extremadura University, Badajoz, Spain.
⁹ Center of Molecular Diagnostics and Personalized Medicine, Department of Basic Sciences, Division of Health Sciences, University of Monterrey, San Pedro Garza Garcia, Nuevo Leon, Mexico. rafael.reyesleon@udem.edu.

PMID: 31780765
PMCID: PMC6882847
DOI: 10.1038/s41598-019-54436-z

Abstract

Amfepramone (AFP) is an appetite-suppressant drug used in the treatment of obesity. Nonetheless, studies on interindividual pharmacokinetic variability and its association with genetic variants are limited. We employed a pharmacokinetic and pharmacogenetic approach to determine possible metabolic phenotypes of AFP and identify genetic markers that could affect the pharmacokinetic variability in a Mexican population. A controlled, randomized, crossover, single-blind, two-treatment, two-period, and two sequence clinical study of AFP (a single 75 mg dose) was conducted in 36 healthy Mexican volunteers who fulfilled the study requirements. Amfepramone plasma levels were measured using high-performance liquid chromatography mass spectrometry. Genotyping was performed using real-time PCR with TaqMan probes. Four AFP metabolizer phenotypes were found in our population: slow, normal, intermediate, and fast. Additionally, two gene polymorphisms, ABCB1-rs1045642 and CYP3A4-rs2242480, had a significant effect on AFP pharmacokinetics (P < 0.05) and were the predictor factors in a log-linear regression model. The ABCB1 and CYP3A4 gene polymorphisms were associated with a fast metabolizer phenotype. These results suggest that metabolism of AFP in the Mexican population is variable. In addition, the genetic variants ABCB1-rs1045642 and CYP3A4-rs2242480 may partially explain the AFP pharmacokinetic variability.

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Conflict of interest statement

The authors declare no competing interests.

Figures

**Figure 1**
Classification of amfepramone (AFP) metabolic phenotypes. (A) Dendrogram generated with Manhattan distance and Ward’s linkage method. (B) Pharmacokinetic profiles of different metabolic phenotypes. Mean peak plasma AFP concentration-time curves after single 75 mg dose of AFP. Data shown are mean ± standard error (SE) concentrations. For both (A,B): slow metabolizers (*red*), intermediate metabolizers (*orange*), normal metabolizers (*green*), and fast metabolizers (*blue*).

See this image and copyright information in PMC

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Pharmacogenetics of amfepramone in healthy Mexican subjects reveals potential markers for tailoring pharmacotherapy of obesity: results of a randomised trial

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Pharmacogenetics of amfepramone in healthy Mexican subjects reveals potential markers for tailoring pharmacotherapy of obesity: results of a randomised trial

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