Determination of NAT2 Genotypes in a Cohort of Patients with Suspected TB in the State of Rio de Janeiro

Author:

Dutra Cecília Alvim12,Teixeira Raquel Lima de Figueiredo2,Lopes Márcia Quinhones Pires2,Silva Victória de Moraes2,Suffys Philip Noel2,Carvalho Ricardo de Souza3,Moreira Adriana Rezende1ORCID,Santos Adalberto Rezende2ORCID,Kritski Afrânio Lineu1ORCID

Affiliation:

1. Academic Tuberculosis Program, Faculty of Medicine, HUCFF-IDT Hospital Complex, Federal University of Rio de Janeiro, Rio de Janeiro 21941-913, Brazil

2. Laboratory of Molecular Biology Applied to Mycobacteria, Oswaldo Cruz Institute, IOC/Fiocruz, Avenida Brasil, 4365, Rio de Janeiro 21040-360, Brazil

3. Department of General Medicine, University of Rio de Janeiro (UniRio), Rio de Janeiro 20270-330, Brazil

Abstract

The human N-acetyltransferase 2 enzyme, encoded by the NAT2 gene, plays an important role in the metabolism of isoniazid, the main drug used to treat tuberculosis. The interindividual variation in the response of patients to drug treatment for tuberculosis may be responsible for the occurrence of unfavorable outcomes. The presence of polymorphisms in genes associated with the metabolism and transport of drugs, receptors, and therapeutic targets has been identified as a major determinant of this variability. The objective of this study was to identify the genetic profile of NAT2 in the study population. Using the obtained genomic DNA followed by PCR amplification and sequencing, the frequency of nine SNPs as well as alleles associated with slow (47.9%), intermediate (38.7%), and fast acetylation phenotypes (11.3%), in addition to those whose phenotype has not yet been characterized (2.1%), was estimated. The NAT2*5B allele was identified more frequently (31.3%). The description of SNPs in pharmacogenes and the establishment of their relationship with the pharmacokinetics of an individual offer an individualized approach that allows us to reduce the unfavorable outcomes of a therapy, ensure better adherence to treatment, prevent the emergence of MDR strains, reduce the cost of treatment, and improve the quality of patients’ lives.

Funder

Budget and Target Program of the Oswaldo Cruz Institute, Oswaldo Cruz Foundation

Publisher

MDPI AG

Reference24 articles.

1. WHO (2022). Global Tuberculosis Report 2022, World Health Organization.

2. (2022). Epidemiological Tuberculosis Bulletin.

3. WHO (2021). Global Tuberculosis Report 2021, World Health Organization.

4. (2023, May 14). Information System for Notifiable Diseases Tuberculosis, Available online: http://sistemas.saude.rj.gov.br/tabnetbd/webtabx.exe?sinan/tf_tuberculose.def/.

5. Serum drug concentrations of INH and RMP predict 2-month sputum culture results in tuberculosis patients;Mah;Int. J. Tuberc. Lung Dis.,2015

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