TY - JOUR
T1 - Safety outcomes in patients with rheumatoid arthritis treated with abatacept
T2 - results from a multinational surveillance study across seven European registries
AU - Dominique, Alyssa
AU - Hetland, Merete Lund
AU - Finckh, Axel
AU - Gottenberg, Jacques Eric
AU - Iannone, Florenzo
AU - Caporali, Roberto
AU - Kou, Tzuyung Douglas
AU - Nordstrom, Dan
AU - Hernandez, Maria Victoria
AU - Sánchez-Piedra, Carlos
AU - Sánchez-Alonso, Fernando
AU - Pavelka, Karel
AU - Bond, T. Christopher
AU - Simon, Teresa A.
N1 - Funding Information:
The authors are grateful to all investigators who contributed to the registries. DANBIO: Mette Nørgaard, MD, PhD (consultant); Nickolaj Risbo Kristensen, MSc; Frank Mehnert, MSc; Professor Henrik Toft Sørensen, MD, PhD, DMSc; Bente Glintborg, MD, PhD (consultant); and Kathrine Lederballe Grøn, MD. Myriam Riek (SCQM Foundation, Zürich, Switzerland) performed the statistical analysis of the SCQM data. ROB-FIN: Nina Trokovic, PhD (data manager), and Arja Kaarto (study nurse). ORA: Xavier Mariette, MD, PhD (co-coordinated the study). Professional medical writing and editorial assistance was provided by Catriona McKay, PhD, and Candice Dcosta, MSc, at Caudex and was funded by Bristol Myers Squibb.
Funding Information:
The authors are grateful to all investigators who contributed to the registries. DANBIO: Mette Nørgaard, MD, PhD (consultant); Nickolaj Risbo Kristensen, MSc; Frank Mehnert, MSc; Professor Henrik Toft Sørensen, MD, PhD, DMSc; Bente Glintborg, MD, PhD (consultant); and Kathrine Lederballe Grøn, MD. Myriam Riek (SCQM Foundation, Zürich, Switzerland) performed the statistical analysis of the SCQM data. ROB-FIN: Nina Trokovic, PhD (data manager), and Arja Kaarto (study nurse). ORA: Xavier Mariette, MD, PhD (co-coordinated the study). Professional medical writing and editorial assistance was provided by Catriona McKay, PhD, and Candice Dcosta, MSc, at Caudex and was funded by Bristol Myers Squibb.
Publisher Copyright:
© 2023, The Author(s).
PY - 2023/12
Y1 - 2023/12
N2 - Background: Patients with rheumatoid arthritis (RA) have an increased risk of infection and malignancy compared with the general population. Infection risk is increased further with the use of disease-modifying antirheumatic drugs (DMARDs), whereas evidence on whether the use of biologic DMARDs increases cancer risk remains equivocal. This single-arm, post-marketing study estimated the incidence of prespecified infection and malignancy outcomes in patients with RA treated with intravenous or subcutaneous abatacept. Methods: Data were included from seven European RA quality registries: ATTRA (Anti-TNF Therapy in Rheumatoid Arthritis [Czech Republic]), DANBIO (Danish Rheumatologic Database), ROB-FIN (National Registry of Antirheumatic and Biological Treatment in Finland), ORA (Orencia and Rheumatoid Arthritis [France]), GISEA (Italian Group for the Study of Early Arthritis), BIOBADASER (Spanish Register of Adverse Events of Biological Therapies in Rheumatic Diseases), and the SCQM (Swiss Clinical Quality Management) system. Each registry is unique with respect to design, data collection, definition of the study cohort, reporting, and validation of outcomes. In general, registries defined the index date as the first day of abatacept treatment and reported data for infections requiring hospitalization and overall malignancies; data for other infection and malignancy outcomes were not available for every cohort. Abatacept exposure was measured in patient-years (p-y). Incidence rates (IRs) were calculated as the number of events per 1000 p-y of follow-up with 95% confidence intervals. Results: Over 5000 patients with RA treated with abatacept were included. Most patients (78–85%) were female, and the mean age range was 52–58 years. Baseline characteristics were largely consistent across registries. Among patients treated with abatacept, IRs for infections requiring hospitalization across the registries ranged from 4 to 100 events per 1000 p-y, while IRs for overall malignancy ranged from 3 to 19 per 1000 p-y. Conclusions: Despite heterogeneity between registries in terms of design, data collection, and ascertainment of safety outcomes, as well as the possibility of under-reporting of adverse events in observational studies, the safety profile of abatacept reported here was largely consistent with previous findings in patients with RA treated with abatacept, with no new or increased risks of infection or malignancy.
AB - Background: Patients with rheumatoid arthritis (RA) have an increased risk of infection and malignancy compared with the general population. Infection risk is increased further with the use of disease-modifying antirheumatic drugs (DMARDs), whereas evidence on whether the use of biologic DMARDs increases cancer risk remains equivocal. This single-arm, post-marketing study estimated the incidence of prespecified infection and malignancy outcomes in patients with RA treated with intravenous or subcutaneous abatacept. Methods: Data were included from seven European RA quality registries: ATTRA (Anti-TNF Therapy in Rheumatoid Arthritis [Czech Republic]), DANBIO (Danish Rheumatologic Database), ROB-FIN (National Registry of Antirheumatic and Biological Treatment in Finland), ORA (Orencia and Rheumatoid Arthritis [France]), GISEA (Italian Group for the Study of Early Arthritis), BIOBADASER (Spanish Register of Adverse Events of Biological Therapies in Rheumatic Diseases), and the SCQM (Swiss Clinical Quality Management) system. Each registry is unique with respect to design, data collection, definition of the study cohort, reporting, and validation of outcomes. In general, registries defined the index date as the first day of abatacept treatment and reported data for infections requiring hospitalization and overall malignancies; data for other infection and malignancy outcomes were not available for every cohort. Abatacept exposure was measured in patient-years (p-y). Incidence rates (IRs) were calculated as the number of events per 1000 p-y of follow-up with 95% confidence intervals. Results: Over 5000 patients with RA treated with abatacept were included. Most patients (78–85%) were female, and the mean age range was 52–58 years. Baseline characteristics were largely consistent across registries. Among patients treated with abatacept, IRs for infections requiring hospitalization across the registries ranged from 4 to 100 events per 1000 p-y, while IRs for overall malignancy ranged from 3 to 19 per 1000 p-y. Conclusions: Despite heterogeneity between registries in terms of design, data collection, and ascertainment of safety outcomes, as well as the possibility of under-reporting of adverse events in observational studies, the safety profile of abatacept reported here was largely consistent with previous findings in patients with RA treated with abatacept, with no new or increased risks of infection or malignancy.
KW - Abatacept
KW - Biologic DMARD
KW - Infections
KW - Malignancy
KW - Rheumatoid arthritis
KW - Safety
U2 - 10.1186/s13075-023-03067-x
DO - 10.1186/s13075-023-03067-x
M3 - Journal article
C2 - 37308978
AN - SCOPUS:85161900168
SN - 1478-6354
VL - 25
JO - Arthritis Research and Therapy
JF - Arthritis Research and Therapy
IS - 1
M1 - 101
ER -