You are here

Article Text

Article menu

Download PDFPDF

Abstracts accepted for Publication
Spondyloarthritis – treatment
AB0704 EFFECTIVENESS AND SAFETY OF INFLIXIMAB AND GOLIMUMAB IN ANKYLOSING SPONDYLITIS PATIENTS FROM A PROSPECTIVE OBSERVATIONAL REGISTRY
Free
  1. Proton Rahman1,
  2. Derek Haaland2,
  3. Dalton Sholter3,
  4. Michael Starr4,
  5. Arthur Karasik5,
  6. Michelle Teo6,
  7. Sanjay Dixit7,
  8. Ariel Masetto8,
  9. Anna Jarosynska9,
  10. Pauline Boulos7,
  11. Maqbool Sheriff10,
  12. Jacqueline Stewart11,
  13. Emmanouil Rampakakis12,
  14. Odalis asin Miilan13,
  15. Allen Lehman13,
  16. Meagan Rachich14,
  17. Francois Nantel13
  1. 1Memorial University of Newfoundland, St. John’s, Canada
  2. 2The Waterside Clinic, Barrie, Canada
  3. 3University of alberta, Edmonton, Canada
  4. 4McGill University Health Centre, Montréal, Canada
  5. 5Ontario Rheumatology association, aurora, Canada
  6. 6Balfour Medical Clinic, Penticton, Canada
  7. 7McMaster University, Hamilton, Canada
  8. 8Université de Sherbrooke, Sherbrooke, Canada
  9. 9Private Clinic, Burlington, Canada
  10. 10Nanaimo Regional General Hospital, Nanaimo, Canada
  11. 11Penticton Regional Hospital, Penticton, Canada
  12. 12JSS Medical Research, Montreal, Canada
  13. 13Janssen inc, Toronto, Canada
  14. 14Janssen inc., Toronto, Canada

Abstract

Background Long-term registries are essential to evaluate new therapies in a patient population that differs from clinical trial and usually varies over time.

Objectives To describe the profile of ankylosing spondylitis (AS) patients treated with infliximab (IFX) or golimumab (GLM) treatment in Canadian routine care along with its long-term effectiveness and safety.

Methods 810 aS patients treated with IFX or GLM were enrolled into the Biologic Treatment Registry across Canada (BioTRAC) registry between 2005-2015 and 2010-2017, respectively. Study visits occurred at baseline and every 6 months thereafter, as needed per routine care. Effectiveness was assessed with changes in aSDAS, BASDAI, BASFI, MDGA, HAQ-DI, PtGA, back pain and acute phase reactants. Safety was evaluated with the incidence of adverse events (AEs) and drug survival rates.

Results Of the 389 IFX- and 421 GLM-treated patients, the proportion of males were 62.7% and 59.1%, the mean age were 45.6 and 45.7 years and the mean disease duration were 8.6 and 6.0 years, respectively. Most patients were bio-naive (>82.7%). Interestingly, we observed a significant decrease in disease duration in the IFX cohort from a median of 8.0 to 3.5 and 1.0 years in 2005-2008, 2009-2012 and 2013-2015, respectively (p<0.001). A reduction in baseline BASFI score (6.3 vs. 5.9 vs 5.1; P=0.011) and in the proportion of patient in aSDAS very high disease activity (48.4%, 43.8%, 30.3%; p=0.004) were also observed. As for the GLM cohort, most disease parameters including median disease duration (1.6 years), mean baseline BASFI (5.3) and the proportion of patients in aSDAS very high disease activity (48%) remained similar from 2010-2017.

Treatment with both IFX and GLM significantly improved all disease parameters over time (P<0.001) from baseline up to 120 and 84 months, respectively, with similar efficacy between agents.

AEs were reported for 67.9% and 70.5% (136 and 131 events/100 PYs) and SAEs for 15.4% and 8.1% (10.5 and 22.7 events/100 PYs) covering 1251.3 and 674.8 years of exposure for IFX- and GLM-treated patients, respectively. The most frequently occurring aEs (>7% of patient in either group) were upper respiratory tract infection, arthralgia and back pain. Two deaths occurred in IFX-treated patients (myocardial infarct, drowning) and two among GLM-treated patients (oropharyngeal cancer; neutropenia, staphylococcal/pseudomonas infections, septic shock).

The proportion of patients who discontinued treatment were 65.8% over a mean 3.2 years of exposure in the IFX cohort and 56.8% over 1.6 years in the GLM cohort.

Conclusion Both IFX and GLM treatment significantly reduced disease activity and improved functionality in a similar fashion and were well tolerated in patients with aS. Differences in baseline characteristics over time demonstrate improvement in early diagnosis of aS and earlier access to biologic therapies.

Disclosure of interests Proton Rahman: None declared, Derek Haaland Grant/research support from: Janssen Sponsored Study, Dalton Sholter Grant/research support from: Janssen Sponsored Study, Michael Starr: None declared, arthur Karasik: None declared, Michelle Teo Grant/research support from: Janssen Sponsored Study, Sanjay Dixit Grant/research support from: Janssen Sponsored Study, Consultant for: Janssen, Speakers bureau: Janssen, ariel Masetto Grant/research support from: amgen, Sanofi, Consultant for: Sanofi, Pfizer, Bristol-Myers Squibb, Novartis, Boehringer ingelheim, Speakers bureau: Novartis, anna Jarosynska Grant/research support from: Janssen Sponsored Study, Pauline Boulos Grant/research support from: Janssen Sponsored Study, Maqbool Sheriff Grant/research support from: Janssen Sponsored Study, Jacqueline Stewart Consultant for: Pfizer, abbvie, amgen, Celgene, Roche, Novartis, Merck, Emmanouil Rampakakis : None declared, Odalis asin MIilan Employee of: Employee of Janssen, allen Lehman Employee of: Employee of Janssen, Meagan Rachich Shareholder of: Janssen, Employee of: Employee of Janssen, Francois Nantel Shareholder of: Janssen, Employee of: Employee of Janssen

https://doi.org/10.1136/annrheumdis-2019-eular.1431

Statistics from Altmetric.com

    Request Permissions

    If you wish to reuse any or all of this article please use the link below which will take you to the Copyright Clearance Center’s RightsLink service. You will be able to get a quick price and instant permission to reuse the content in many different ways.