Clinical and Demographic Profile of Patients Receiving Fingolimod in Clinical Practice in Germany and the Benefit–Risk Profile of Fingolimod After 1 Year of Treatment: Initial Results From the Observational, Noninterventional Study PANGAEA

Research output: Contribution to journalResearch articleContributedpeer-review

Contributors

  • PANGAEA Study Group - (Author)
  • Department of Neurology
  • NeuroPoint Patient Academy and Neurological Practice
  • University of Marburg
  • Bonn Neurological Practice Schmidt, Viebahn, Kronenberger, Schuller
  • Neurological Practice
  • University of Münster
  • Jüdisches Krankenhaus Berlin
  • Kassel and Vellmar Neurological Practice
  • Novartis AG
  • Novartis Pharma AG

Abstract

The population with multiple sclerosis receiving treatment in clinical practice differs from that in randomized controlled trials (RCTs). An assessment of the real-world benefit–risk profile of therapies is needed. This analysis used data from the large, noninterventional, observational German study Post-Authorization Non-interventional German sAfety study of GilEnyA (PANGAEA) to assess prospectively baseline characteristics and outcomes after 12 months (± 90 days) of fingolimod treatment. Patients were divided into 2 cohorts: fingolimod starter [first received fingolimod in PANGAEA (n = 3315)] and previous study [received fingolimod before enrollment in PANGAEA in RCTs (n = 875), some of whom also had baseline data at entry into RCTs (n = 505)]. At PANGAEA baseline, patients in the fingolimod starter versus the previous study cohort had a higher annualized relapse rate [ARR (95% confidence interval): 1.79 (1.75–1.83) vs 1.32 (1.25–1.40)] and Expanded Disability Status Scale score [3.11 (3.04–3.17) vs 2.55 (2.44–2.66)]. A greater proportion in the fingolimod starter versus previous study cohort had diabetes (2.0% vs 0.7%). After 12 months of fingolimod, ARRs were lower than in the 12 months before PANGAEA enrollment in the fingolimod starter [0.386 (0.360–0.414)] and previous study [0.276 (0.238–0.320)] cohorts. Expanded Disability Status Scale scores were stable versus baseline. Adverse events were experienced by similar proportions in both cohorts during fingolimod treatment. Relevant differences exist in disease activity and comorbidities between patients receiving fingolimod in clinical practice versus RCTs. Irrespective of baseline differences indicating a higher proportion at an advanced stage of multiple sclerosis in the real world versus RCTs, fingolimod remains effective, with a manageable safety profile.

Details

Original languageEnglish
Pages (from-to)190-199
Number of pages10
JournalNeurotherapeutics
Volume15
Issue number1
Publication statusPublished - 1 Jan 2018
Peer-reviewedYes

External IDs

PubMed 29274026
ORCID /0000-0001-8799-8202/work/171553629

Keywords

Sustainable Development Goals

Keywords

  • Benefit–risk profile, Fingolimod, Multiple sclerosis, Observational study, Real-world evidence

Library keywords