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Tofacitinib shows no evidence of an increased risk for malignancies compared with TNF inhibitors when used to treat rheumatoid arthritis, according to data published in Arthritis &Rheumatology.
“We were interested in generating real-world evidence on the safety of tofacitinib compared with TNF inhibitors in patients with RA while waiting for the final data release from the ORAL Surveillance trial,” Seoyoung C. Kim, MD, ScD, associate professor of medicine at Brigham and Women’s Hospital and Harvard Medical School, told Healio.
To examine the risk for increased malignancy associated with tofacitinib (Xeljanz, Pfizer), Kim and colleagues conducted an active-comparator, new-user cohort study. The study used claims data sourced from Optum Clinformatics, IBM Marketscan and fee-for-service Medicare. Collection spanned November 2012 through June 2020.
The researchers identified patients in each data source who were receiving tofacitinib or a TNF inhibitor, with the entry date defined as first record of medication dispensation for TNF inhibitors or tofacitinib. Patients were also required to have a minimum of 365 days of continuous health care enrollment before and during the study period. Patients with RA were included if they had at least two visits between 7 and 365 days apart for the disease.
The researchers created two separate cohorts — a real-world evidence group and a group designed to assess comparability of the current study with the ORAL surveillance trial. The real-world evidence cohort included all patients with RA aged 18 years or older, while the comparator cohort required patients to be aged 50 years or older. Patients were followed from the date of treatment initiation with either drug until treatment discontinuation of 60 days or switch, insurance disenrollment, death or the end of the study period.
The primary outcome was a composite endpoint of any new malignancies, excluding non-melanoma skin cancer, defined as two inpatient or outpatient ICD-9 or ICD-10 diagnosis codes of the same type of malignancy occurring within 60 days. Individual types of malignancy, including lung, breast and colorectal cancers, were secondary outcomes.
In all, the real-world cohort included 83,295 patients. Of that group, 10,504 initiated tofacitinib. According to the researchers, the weighted HRs for any malignancy associated with tofacitinib compared with TNF inhibitors were 1.01 (95% CI, 0.83-1.22) in the real-world group and 1.17 (95% CI, 0.85-1.62) in the comparator cohort.
“Our study did not find evidence for an increased risk for malignancy with tofacitinib vs. TNF inhibitors in adult patients with RA treated in the real-world setting,” Kim said. “However, as our study has a relatively short follow-up time, with a mean follow-up of less than 1 year, and we cannot rule out a possibility of an increase in risk that may accrue with a longer treatment duration. Furthermore, tofacitinib was associated with a numerically increased risk of malignancies in our RCT-duplicate population, which consisted of patients 50 years of age and older and with at least one cardiovascular risk factor.
“While our study includes a large cohort of almost 84,000 RA patients using real-world data, we had limited statistical power to run some of the subgroup/cancer-type specific analyses,” she added. “This highlights the need for continuous monitoring of the safety of tofacitinib not only in the United States but also in other countries.”