Pharmacogenetic aspects of methotrexate in a cohort of Colombian patients with rheumatoid arthritis

John Londono; Eugenia-Lucia Saldarriaga; Juan C Rueda; Rodrigo Giraldo-Bustos; Jose-Ignacio Angarita; Luisa Restrepo; Jesus Ballesteros-Muñoz; Camilo González; Maria J Ospina; Sofia Arias-Correal; Viviana Reyes-Martinez; Santiago Bernalmacias; Catalina Villota-Eraso; Pedro Santos-Moreno; Nancy Martinez-Rodriguez; Ana M Santos

doi:10.3892/br.2020.1341

Pharmacogenetic aspects of methotrexate in a cohort of Colombian patients with rheumatoid arthritis

John Londono, Eugenia-Lucia Saldarriaga, Juan C Rueda, Rodrigo Giraldo-Bustos, Jose-Ignacio Angarita, Luisa Restrepo, Jesus Ballesteros-Muñoz, Camilo González, Maria J Ospina, Sofia Arias-Correal, Viviana Reyes-Martinez, Santiago Bernalmacias, Catalina Villota-Eraso, Pedro Santos-Moreno, Nancy Martinez-Rodriguez, Ana M Santos

Producción: Contribución a una revista › Artículo › revisión exhaustiva

4 Citas (Scopus)

Resumen

Methotrexate (MTX) is the most commonly used disease-modifying antirheumatic drug for the treatment of rheumatoid arthritis (RA). However, over time, ~40% of patients may experience therapeutic failure or drug toxicity. The genetic variability of the enzymes involved in the MTX metabolic pathway seem to serve an important role in the eventual therapeutic failure or drug toxicity. Depending on the enzymes affected, the toxicity or the therapeutic response may change. The present study reports some of the polymorphisms identified in enzymes in the MTX metabolic pathway that are present in a group of Colombian patients with RA, and assesses the associations of these polymorphisms with toxicity or therapeutic response to the medication. A total of 400 patients with RA were evaluated, of which 76% were women. the average age was 60.7±13.9 years and the duration of the disease was 13.2±10.9 years. The disease activity scoring method, DAS28-CRP, was used to evaluate the therapeutic response. Toxicity was determined based on reports of adverse events during the evaluation of the patients. The single nucleotide polymorphisms (SNPs) assessed using reverse transcription-PCR in the present study were MTHFR C677T, A1298C, ATIC C347G, RFC-1-G80A, FPGS-AG and DHFR-CT. The SNPs of MTHFR C677T (P=0.05) and A1298C (P=0.048) were significantly associated with the efficacy of MTX, and DHFR-CT (P=0.01) and ATIC C347 (P=0.005) were significantly associated with documented toxicity. Haematological, hepatic or renal toxicity was not associated with any of the SNPs. The results obtained in Colombian patients with RA receiving MTX are similar to those reported in other populations; however, the SNPs associated with a lack of response previously reported in the literature were not observed in our data. The SNPs identified in the present study may be used as biomarkers to predict response to MTX in terms of efficacy and toxicity in Colombian patients with RA.

Idioma original	Inglés
Páginas (desde-hasta)	34-39
Número de páginas	6
Publicación	Biomedical Reports
Volumen	13
N.º	4
DOI	https://doi.org/10.3892/br.2020.1341
Estado	Publicada - ago. 2020
Publicado de forma externa	Sí

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Londono, J., Saldarriaga, E.-L., Rueda, J. C., Giraldo-Bustos, R., Angarita, J.-I., Restrepo, L., Ballesteros-Muñoz, J., González, C., Ospina, M. J., Arias-Correal, S., Reyes-Martinez, V., Bernalmacias, S., Villota-Eraso, C., Santos-Moreno, P., Martinez-Rodriguez, N., & Santos, A. M. (2020). Pharmacogenetic aspects of methotrexate in a cohort of Colombian patients with rheumatoid arthritis. Biomedical Reports, 13(4), 34-39. https://doi.org/10.3892/br.2020.1341

@article{f04e18209f454a8084b06b9b30108c80,

title = "Pharmacogenetic aspects of methotrexate in a cohort of Colombian patients with rheumatoid arthritis",

abstract = "Methotrexate (MTX) is the most commonly used disease-modifying antirheumatic drug for the treatment of rheumatoid arthritis (RA). However, over time, \textasciitilde{}40\% of patients may experience therapeutic failure or drug toxicity. The genetic variability of the enzymes involved in the MTX metabolic pathway seem to serve an important role in the eventual therapeutic failure or drug toxicity. Depending on the enzymes affected, the toxicity or the therapeutic response may change. The present study reports some of the polymorphisms identified in enzymes in the MTX metabolic pathway that are present in a group of Colombian patients with RA, and assesses the associations of these polymorphisms with toxicity or therapeutic response to the medication. A total of 400 patients with RA were evaluated, of which 76\% were women. the average age was 60.7±13.9 years and the duration of the disease was 13.2±10.9 years. The disease activity scoring method, DAS28-CRP, was used to evaluate the therapeutic response. Toxicity was determined based on reports of adverse events during the evaluation of the patients. The single nucleotide polymorphisms (SNPs) assessed using reverse transcription-PCR in the present study were MTHFR C677T, A1298C, ATIC C347G, RFC-1-G80A, FPGS-AG and DHFR-CT. The SNPs of MTHFR C677T (P=0.05) and A1298C (P=0.048) were significantly associated with the efficacy of MTX, and DHFR-CT (P=0.01) and ATIC C347 (P=0.005) were significantly associated with documented toxicity. Haematological, hepatic or renal toxicity was not associated with any of the SNPs. The results obtained in Colombian patients with RA receiving MTX are similar to those reported in other populations; however, the SNPs associated with a lack of response previously reported in the literature were not observed in our data. The SNPs identified in the present study may be used as biomarkers to predict response to MTX in terms of efficacy and toxicity in Colombian patients with RA.",

keywords = "methotrexate, rheumatoid arthritis, single nucleotide polymorphism, toxicity, efficacy",

author = "John Londono and Eugenia-Lucia Saldarriaga and Rueda, \{Juan C\} and Rodrigo Giraldo-Bustos and Jose-Ignacio Angarita and Luisa Restrepo and Jesus Ballesteros-Mu{\~n}oz and Camilo Gonz{\'a}lez and Ospina, \{Maria J\} and Sofia Arias-Correal and Viviana Reyes-Martinez and Santiago Bernalmacias and Catalina Villota-Eraso and Pedro Santos-Moreno and Nancy Martinez-Rodriguez and Santos, \{Ana M\}",

note = "Copyright {\textcopyright} 2020, Spandidos Publications.",

year = "2020",

month = aug,

doi = "10.3892/br.2020.1341",

language = "English",

volume = "13",

pages = "34--39",

journal = "Biomedical Reports",

issn = "2049-9434",

publisher = "Spandidos Publications",

number = "4",

}

Londono, J, Saldarriaga, E-L, Rueda, JC, Giraldo-Bustos, R, Angarita, J-I, Restrepo, L, Ballesteros-Muñoz, J, González, C, Ospina, MJ, Arias-Correal, S, Reyes-Martinez, V, Bernalmacias, S, Villota-Eraso, C, Santos-Moreno, P, Martinez-Rodriguez, N & Santos, AM 2020, 'Pharmacogenetic aspects of methotrexate in a cohort of Colombian patients with rheumatoid arthritis', Biomedical Reports, vol. 13, n.º 4, pp. 34-39. https://doi.org/10.3892/br.2020.1341

TY - JOUR

T1 - Pharmacogenetic aspects of methotrexate in a cohort of Colombian patients with rheumatoid arthritis

AU - Londono, John

AU - Saldarriaga, Eugenia-Lucia

AU - Rueda, Juan C

AU - Giraldo-Bustos, Rodrigo

AU - Angarita, Jose-Ignacio

AU - Restrepo, Luisa

AU - Ballesteros-Muñoz, Jesus

AU - González, Camilo

AU - Ospina, Maria J

AU - Arias-Correal, Sofia

AU - Reyes-Martinez, Viviana

AU - Bernalmacias, Santiago

AU - Villota-Eraso, Catalina

AU - Santos-Moreno, Pedro

AU - Martinez-Rodriguez, Nancy

AU - Santos, Ana M

PY - 2020/8

Y1 - 2020/8

N2 - Methotrexate (MTX) is the most commonly used disease-modifying antirheumatic drug for the treatment of rheumatoid arthritis (RA). However, over time, ~40% of patients may experience therapeutic failure or drug toxicity. The genetic variability of the enzymes involved in the MTX metabolic pathway seem to serve an important role in the eventual therapeutic failure or drug toxicity. Depending on the enzymes affected, the toxicity or the therapeutic response may change. The present study reports some of the polymorphisms identified in enzymes in the MTX metabolic pathway that are present in a group of Colombian patients with RA, and assesses the associations of these polymorphisms with toxicity or therapeutic response to the medication. A total of 400 patients with RA were evaluated, of which 76% were women. the average age was 60.7±13.9 years and the duration of the disease was 13.2±10.9 years. The disease activity scoring method, DAS28-CRP, was used to evaluate the therapeutic response. Toxicity was determined based on reports of adverse events during the evaluation of the patients. The single nucleotide polymorphisms (SNPs) assessed using reverse transcription-PCR in the present study were MTHFR C677T, A1298C, ATIC C347G, RFC-1-G80A, FPGS-AG and DHFR-CT. The SNPs of MTHFR C677T (P=0.05) and A1298C (P=0.048) were significantly associated with the efficacy of MTX, and DHFR-CT (P=0.01) and ATIC C347 (P=0.005) were significantly associated with documented toxicity. Haematological, hepatic or renal toxicity was not associated with any of the SNPs. The results obtained in Colombian patients with RA receiving MTX are similar to those reported in other populations; however, the SNPs associated with a lack of response previously reported in the literature were not observed in our data. The SNPs identified in the present study may be used as biomarkers to predict response to MTX in terms of efficacy and toxicity in Colombian patients with RA.

AB - Methotrexate (MTX) is the most commonly used disease-modifying antirheumatic drug for the treatment of rheumatoid arthritis (RA). However, over time, ~40% of patients may experience therapeutic failure or drug toxicity. The genetic variability of the enzymes involved in the MTX metabolic pathway seem to serve an important role in the eventual therapeutic failure or drug toxicity. Depending on the enzymes affected, the toxicity or the therapeutic response may change. The present study reports some of the polymorphisms identified in enzymes in the MTX metabolic pathway that are present in a group of Colombian patients with RA, and assesses the associations of these polymorphisms with toxicity or therapeutic response to the medication. A total of 400 patients with RA were evaluated, of which 76% were women. the average age was 60.7±13.9 years and the duration of the disease was 13.2±10.9 years. The disease activity scoring method, DAS28-CRP, was used to evaluate the therapeutic response. Toxicity was determined based on reports of adverse events during the evaluation of the patients. The single nucleotide polymorphisms (SNPs) assessed using reverse transcription-PCR in the present study were MTHFR C677T, A1298C, ATIC C347G, RFC-1-G80A, FPGS-AG and DHFR-CT. The SNPs of MTHFR C677T (P=0.05) and A1298C (P=0.048) were significantly associated with the efficacy of MTX, and DHFR-CT (P=0.01) and ATIC C347 (P=0.005) were significantly associated with documented toxicity. Haematological, hepatic or renal toxicity was not associated with any of the SNPs. The results obtained in Colombian patients with RA receiving MTX are similar to those reported in other populations; however, the SNPs associated with a lack of response previously reported in the literature were not observed in our data. The SNPs identified in the present study may be used as biomarkers to predict response to MTX in terms of efficacy and toxicity in Colombian patients with RA.

KW - methotrexate

KW - rheumatoid arthritis

KW - single nucleotide polymorphism

KW - toxicity

KW - efficacy

U2 - 10.3892/br.2020.1341

DO - 10.3892/br.2020.1341

M3 - Article

C2 - 32793348

SN - 2049-9434

VL - 13

SP - 34

EP - 39

JO - Biomedical Reports

JF - Biomedical Reports

IS - 4

ER -

Pharmacogenetic aspects of methotrexate in a cohort of Colombian patients with rheumatoid arthritis

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