Real-world safety data of first-line drugs for rheumatoid arthritis: insights from the Portuguese Reuma.pt database

Joana Ramos Rodrigues; L. Pires; L. Inês; M. Morgado; M. Pontes Ferreira; A. Cunha; S. Almeida; M. Santos; A. C. Moniz; D. Melim; M. Bernardes; C. Marques Gomes; M. Diz Lopes; D. Carvalho; J. Polido Pereira; J. Aguiar; I. Sopa; C. Duarte; F. Canhão; S. Palos; C. Miguel; A. Vieira; L. Reynolds; M. Oliveira; F. Pinheiro; C. Abreu; S. Matias; A. C. Duarte; A. Chícharo; V. Teixeira; P. M. Teixeira; A. R. Fonseca; M. H. Lourenço; C. Rua; C. Silva; M. Oliveira; A. Águeda; M. Rodrigues; H. Assunção; P. Nero; M. Couto; H. Santos Carneiro; D. Augusto; M. F. Magalhães; J. Dias; T. Melo; C. Campinho; P. Pereira; A. Raposo; J. Lagoas Gomes; J. Valido; F. Farinha; J. A. Pereira da Silva; A. Vilar; J. A. Costa; M. Cruz; J. Garcia; F. Araújo; G. Sequeira; A. C. Cordeiro; A. F. Mourão

doi:10.63032/XQFS6110

Real-world safety data of first-line drugs for rheumatoid arthritis: insights from the Portuguese Reuma.pt database

Joana Ramos Rodrigues
, L. Pires
, L. Inês
, M. Morgado
, M. Pontes Ferreira
, A. Cunha
, S. Almeida
, M. Santos
, A. C. Moniz
, D. Melim
, M. Bernardes
, C. Marques Gomes
, M. Diz Lopes
, D. Carvalho
, J. Polido Pereira
, J. Aguiar
, I. Sopa
, C. Duarte
, F. Canhão
, S. Palos

C. Miguel, A. Vieira, L. Reynolds, M. Oliveira, F. Pinheiro, C. Abreu, S. Matias, A. C. Duarte, A. Chícharo, V. Teixeira, P. M. Teixeira, A. R. Fonseca, M. H. Lourenço, C. Rua, C. Silva, M. Oliveira, A. Águeda, M. Rodrigues, H. Assunção, P. Nero, M. Couto, H. Santos Carneiro, D. Augusto, M. F. Magalhães, J. Dias, T. Melo, C. Campinho, P. Pereira, A. Raposo, J. Lagoas Gomes, J. Valido, F. Farinha, J. A. Pereira da Silva, A. Vilar, J. A. Costa, M. Cruz, J. Garcia, F. Araújo, G. Sequeira, A. C. Cordeiro, A. F. Mourão

Resultado de pesquisa: ???type-name??? › ???researchoutput.researchoutputtypes.contributiontojournal.article??? › revisão de pares

Resumo

Objectives: To assess adverse events (AE) associated with first-line therapies for rheumatoid arthritis (RA) in a real-world setting. Material and Methods: Retrospective multicenter cohort study of patients fulfilling classification criteria for RA and followed up in 66 rheumatology centers from the Rheumatic Diseases Portuguese Registry (Reuma.pt). All AE reports associated with first-line disease-modifying antirheumatic drugs (DMARDs) up to November 2024 were included. Demographic and clinical data were analyzed, and AE characteristics were investigated. Categorical and continuous variables were compared using chi-square tests and Mann–Whitney U tests, respectively. Statistical significance was defined as p < 0.05. Results: Among 1 880 AE entries, 377 (20.1%) were attributed to first-line DMARDs, most commonly methotrexate (62.9%) although no information on drug dosage was available. The median age at AE occurrence was 58.6 years (IQR: 19.32), and 82% were female. A causality assessment was available in 317 reports, with 40.3% deemed “probable,” 28.1% “possible,” and 10.6% “definitive.” Severe AE were reported in 13.2% of cases, with pulmonary involvement being the most common (20.8%). Overall, 46.7% of patients discontinued treatment for any reason. Male sex was significantly associated with severe AE (OR = 2.31; 95% CI: 1.17–4.55; p = .014), and older patients were more likely to experience severe AE (median age 65.7 vs. 57.9 years; p < .001). The most affected body organ systems were gastrointestinal (9.3%), skin (8.2%), and hematological (8.2%). The median time to AE onset from treatment initiation was 1.27 years (IQR: 2.63), and from disease onset was 8.56 years (IQR: 11.76). Conclusions: AE related to first-line RA therapies can lead to significant clinical consequences, including treatment discontinuation. Male sex and advanced age were associated with increased AE severity. The most affected systems appear consistent with known drug safety profiles, particularly that of methotrexate; however, the absence of information regarding drug dosage precludes more detailed conclusions. These findings emphasize the need for individualized monitoring strategies and improved pharmacovigilance to optimize long-term treatment safety and adherence in RA management.

Idioma original	???core.languages.en_GB???
Páginas (de-até)	267-275
Número de páginas	9
Revista	ARP Rheumatology
Volume	4
Número de emissão	4
DOIs	https://doi.org/10.63032/XQFS6110
Estado da publicação	???researchoutput.status.published??? - 1 out. 2025
Publicado externamente	Sim

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Ramos Rodrigues, J., Pires, L., Inês, L., Morgado, M., Pontes Ferreira, M., Cunha, A., Almeida, S., Santos, M., Moniz, A. C., Melim, D., Bernardes, M., Marques Gomes, C., Diz Lopes, M., Carvalho, D., Polido Pereira, J., Aguiar, J., Sopa, I., Duarte, C., Canhão, F., ... Mourão, A. F. (2025). Real-world safety data of first-line drugs for rheumatoid arthritis: insights from the Portuguese Reuma.pt database. ARP Rheumatology, 4(4), 267-275. https://doi.org/10.63032/XQFS6110

@article{d293ebc69c3944058111fa06383b3b98,

title = "Real-world safety data of first-line drugs for rheumatoid arthritis: insights from the Portuguese Reuma.pt database",

abstract = "Objectives: To assess adverse events (AE) associated with first-line therapies for rheumatoid arthritis (RA) in a real-world setting. Material and Methods: Retrospective multicenter cohort study of patients fulfilling classification criteria for RA and followed up in 66 rheumatology centers from the Rheumatic Diseases Portuguese Registry (Reuma.pt). All AE reports associated with first-line disease-modifying antirheumatic drugs (DMARDs) up to November 2024 were included. Demographic and clinical data were analyzed, and AE characteristics were investigated. Categorical and continuous variables were compared using chi-square tests and Mann–Whitney U tests, respectively. Statistical significance was defined as p < 0.05. Results: Among 1 880 AE entries, 377 (20.1\%) were attributed to first-line DMARDs, most commonly methotrexate (62.9\%) although no information on drug dosage was available. The median age at AE occurrence was 58.6 years (IQR: 19.32), and 82\% were female. A causality assessment was available in 317 reports, with 40.3\% deemed “probable,” 28.1\% “possible,” and 10.6\% “definitive.” Severe AE were reported in 13.2\% of cases, with pulmonary involvement being the most common (20.8\%). Overall, 46.7\% of patients discontinued treatment for any reason. Male sex was significantly associated with severe AE (OR = 2.31; 95\% CI: 1.17–4.55; p = .014), and older patients were more likely to experience severe AE (median age 65.7 vs. 57.9 years; p < .001). The most affected body organ systems were gastrointestinal (9.3\%), skin (8.2\%), and hematological (8.2\%). The median time to AE onset from treatment initiation was 1.27 years (IQR: 2.63), and from disease onset was 8.56 years (IQR: 11.76). Conclusions: AE related to first-line RA therapies can lead to significant clinical consequences, including treatment discontinuation. Male sex and advanced age were associated with increased AE severity. The most affected systems appear consistent with known drug safety profiles, particularly that of methotrexate; however, the absence of information regarding drug dosage precludes more detailed conclusions. These findings emphasize the need for individualized monitoring strategies and improved pharmacovigilance to optimize long-term treatment safety and adherence in RA management.",

keywords = "Adverse Drug Reaction Reporting Systems, Antirheumatic Agents, Methotrexate, Rheumatoid Arthritis, Treatment Outcome",

author = "\{Ramos Rodrigues\}, Joana and L. Pires and L. In{\^e}s and M. Morgado and \{Pontes Ferreira\}, M. and A. Cunha and S. Almeida and M. Santos and Moniz, \{A. C.\} and D. Melim and M. Bernardes and \{Marques Gomes\}, C. and \{Diz Lopes\}, M. and D. Carvalho and \{Polido Pereira\}, J. and J. Aguiar and I. Sopa and C. Duarte and F. Canh{\~a}o and S. Palos and C. Miguel and A. Vieira and L. Reynolds and M. Oliveira and F. Pinheiro and C. Abreu and S. Matias and Duarte, \{A. C.\} and A. Ch{\'i}charo and V. Teixeira and Teixeira, \{P. M.\} and Fonseca, \{A. R.\} and Louren{\c c}o, \{M. H.\} and C. Rua and C. Silva and M. Oliveira and A. {\'A}gueda and M. Rodrigues and H. Assun{\c c}{\~a}o and P. Nero and M. Couto and \{Santos Carneiro\}, H. and D. Augusto and Magalh{\~a}es, \{M. F.\} and J. Dias and T. Melo and C. Campinho and P. Pereira and A. Raposo and \{Lagoas Gomes\}, J. and J. Valido and F. Farinha and \{Pereira da Silva\}, \{J. A.\} and A. Vilar and Costa, \{J. A.\} and M. Cruz and J. Garcia and F. Ara{\'u}jo and G. Sequeira and Cordeiro, \{A. C.\} and Mour{\~a}o, \{A. F.\}",

year = "2025",

month = oct,

day = "1",

doi = "10.63032/XQFS6110",

language = "English",

volume = "4",

pages = "267--275",

journal = "ARP Rheumatology",

issn = "0303-464X",

publisher = "Sociedade Portuguesa de Reumatologia",

number = "4",

}

Ramos Rodrigues, J, Pires, L, Inês, L, Morgado, M, Pontes Ferreira, M, Cunha, A, Almeida, S, Santos, M, Moniz, AC, Melim, D, Bernardes, M, Marques Gomes, C, Diz Lopes, M, Carvalho, D, Polido Pereira, J, Aguiar, J, Sopa, I, Duarte, C, Canhão, F, Palos, S, Miguel, C, Vieira, A, Reynolds, L, Oliveira, M, Pinheiro, F, Abreu, C, Matias, S, Duarte, AC, Chícharo, A, Teixeira, V, Teixeira, PM, Fonseca, AR, Lourenço, MH, Rua, C, Silva, C, Oliveira, M, Águeda, A, Rodrigues, M, Assunção, H, Nero, P, Couto, M, Santos Carneiro, H, Augusto, D, Magalhães, MF, Dias, J, Melo, T, Campinho, C, Pereira, P, Raposo, A, Lagoas Gomes, J, Valido, J, Farinha, F, Pereira da Silva, JA, Vilar, A, Costa, JA, Cruz, M, Garcia, J, Araújo, F, Sequeira, G, Cordeiro, AC & Mourão, AF 2025, 'Real-world safety data of first-line drugs for rheumatoid arthritis: insights from the Portuguese Reuma.pt database', ARP Rheumatology, vol. 4, n.º 4, pp. 267-275. https://doi.org/10.63032/XQFS6110

TY - JOUR

T1 - Real-world safety data of first-line drugs for rheumatoid arthritis

T2 - insights from the Portuguese Reuma.pt database

AU - Ramos Rodrigues, Joana

AU - Pires, L.

AU - Inês, L.

AU - Morgado, M.

AU - Pontes Ferreira, M.

AU - Cunha, A.

AU - Almeida, S.

AU - Santos, M.

AU - Moniz, A. C.

AU - Melim, D.

AU - Bernardes, M.

AU - Marques Gomes, C.

AU - Diz Lopes, M.

AU - Carvalho, D.

AU - Polido Pereira, J.

AU - Aguiar, J.

AU - Sopa, I.

AU - Duarte, C.

AU - Canhão, F.

AU - Palos, S.

AU - Miguel, C.

AU - Vieira, A.

AU - Reynolds, L.

AU - Oliveira, M.

AU - Pinheiro, F.

AU - Abreu, C.

AU - Matias, S.

AU - Duarte, A. C.

AU - Chícharo, A.

AU - Teixeira, V.

AU - Teixeira, P. M.

AU - Fonseca, A. R.

AU - Lourenço, M. H.

AU - Rua, C.

AU - Silva, C.

AU - Oliveira, M.

AU - Águeda, A.

AU - Rodrigues, M.

AU - Assunção, H.

AU - Nero, P.

AU - Couto, M.

AU - Santos Carneiro, H.

AU - Augusto, D.

AU - Magalhães, M. F.

AU - Dias, J.

AU - Melo, T.

AU - Campinho, C.

AU - Pereira, P.

AU - Raposo, A.

AU - Lagoas Gomes, J.

AU - Valido, J.

AU - Farinha, F.

AU - Pereira da Silva, J. A.

AU - Vilar, A.

AU - Costa, J. A.

AU - Cruz, M.

AU - Garcia, J.

AU - Araújo, F.

AU - Sequeira, G.

AU - Cordeiro, A. C.

AU - Mourão, A. F.

PY - 2025/10/1

Y1 - 2025/10/1

N2 - Objectives: To assess adverse events (AE) associated with first-line therapies for rheumatoid arthritis (RA) in a real-world setting. Material and Methods: Retrospective multicenter cohort study of patients fulfilling classification criteria for RA and followed up in 66 rheumatology centers from the Rheumatic Diseases Portuguese Registry (Reuma.pt). All AE reports associated with first-line disease-modifying antirheumatic drugs (DMARDs) up to November 2024 were included. Demographic and clinical data were analyzed, and AE characteristics were investigated. Categorical and continuous variables were compared using chi-square tests and Mann–Whitney U tests, respectively. Statistical significance was defined as p < 0.05. Results: Among 1 880 AE entries, 377 (20.1%) were attributed to first-line DMARDs, most commonly methotrexate (62.9%) although no information on drug dosage was available. The median age at AE occurrence was 58.6 years (IQR: 19.32), and 82% were female. A causality assessment was available in 317 reports, with 40.3% deemed “probable,” 28.1% “possible,” and 10.6% “definitive.” Severe AE were reported in 13.2% of cases, with pulmonary involvement being the most common (20.8%). Overall, 46.7% of patients discontinued treatment for any reason. Male sex was significantly associated with severe AE (OR = 2.31; 95% CI: 1.17–4.55; p = .014), and older patients were more likely to experience severe AE (median age 65.7 vs. 57.9 years; p < .001). The most affected body organ systems were gastrointestinal (9.3%), skin (8.2%), and hematological (8.2%). The median time to AE onset from treatment initiation was 1.27 years (IQR: 2.63), and from disease onset was 8.56 years (IQR: 11.76). Conclusions: AE related to first-line RA therapies can lead to significant clinical consequences, including treatment discontinuation. Male sex and advanced age were associated with increased AE severity. The most affected systems appear consistent with known drug safety profiles, particularly that of methotrexate; however, the absence of information regarding drug dosage precludes more detailed conclusions. These findings emphasize the need for individualized monitoring strategies and improved pharmacovigilance to optimize long-term treatment safety and adherence in RA management.

AB - Objectives: To assess adverse events (AE) associated with first-line therapies for rheumatoid arthritis (RA) in a real-world setting. Material and Methods: Retrospective multicenter cohort study of patients fulfilling classification criteria for RA and followed up in 66 rheumatology centers from the Rheumatic Diseases Portuguese Registry (Reuma.pt). All AE reports associated with first-line disease-modifying antirheumatic drugs (DMARDs) up to November 2024 were included. Demographic and clinical data were analyzed, and AE characteristics were investigated. Categorical and continuous variables were compared using chi-square tests and Mann–Whitney U tests, respectively. Statistical significance was defined as p < 0.05. Results: Among 1 880 AE entries, 377 (20.1%) were attributed to first-line DMARDs, most commonly methotrexate (62.9%) although no information on drug dosage was available. The median age at AE occurrence was 58.6 years (IQR: 19.32), and 82% were female. A causality assessment was available in 317 reports, with 40.3% deemed “probable,” 28.1% “possible,” and 10.6% “definitive.” Severe AE were reported in 13.2% of cases, with pulmonary involvement being the most common (20.8%). Overall, 46.7% of patients discontinued treatment for any reason. Male sex was significantly associated with severe AE (OR = 2.31; 95% CI: 1.17–4.55; p = .014), and older patients were more likely to experience severe AE (median age 65.7 vs. 57.9 years; p < .001). The most affected body organ systems were gastrointestinal (9.3%), skin (8.2%), and hematological (8.2%). The median time to AE onset from treatment initiation was 1.27 years (IQR: 2.63), and from disease onset was 8.56 years (IQR: 11.76). Conclusions: AE related to first-line RA therapies can lead to significant clinical consequences, including treatment discontinuation. Male sex and advanced age were associated with increased AE severity. The most affected systems appear consistent with known drug safety profiles, particularly that of methotrexate; however, the absence of information regarding drug dosage precludes more detailed conclusions. These findings emphasize the need for individualized monitoring strategies and improved pharmacovigilance to optimize long-term treatment safety and adherence in RA management.

KW - Adverse Drug Reaction Reporting Systems

KW - Antirheumatic Agents

KW - Methotrexate

KW - Rheumatoid Arthritis

KW - Treatment Outcome

UR - https://www.scopus.com/pages/publications/105028737832

U2 - 10.63032/XQFS6110

DO - 10.63032/XQFS6110

M3 - Article

AN - SCOPUS:105028737832

SN - 0303-464X

VL - 4

SP - 267

EP - 275

JO - ARP Rheumatology

JF - ARP Rheumatology

IS - 4

ER -

Real-world safety data of first-line drugs for rheumatoid arthritis: insights from the Portuguese Reuma.pt database

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