A Descriptive Analysis of Real-World Treatment Patterns in a Turkish Rheumatology Population That Continued Innovator Infliximab (Remicade) Therapy or Switched to Biosimilar Infliximab

Yusuf Yazici¹, Lin Xie², Adesuwa Ogbomo³, Dennis Parenti⁴, Kavitha Goyal⁴, Amanda Teeple⁴, Lorie A. Ellis⁵ and Ismail Simsek⁶, ¹New York University, Hospital of Joint Diseases, New York, NY, ²Director, Health Economics & Outcomes Research, STATinMED Research, Ann Arbor, MI, ³STATinMED Research Inc., Ann Arbor, MI, ⁴Janssen Scientific Affairs, LLC, Horsham, PA, ⁵Health Economics & Outcomes Research, Janssen Scientific Affairs, LLC, Horsham, PA, ⁶Guven Hospital, Ankara, Turkey

Meeting: 2016 ACR/ARHP Annual Meeting

Date of first publication: September 28, 2016

Keywords: rheumatoid arthritis (RA) and treatment

Session Information

Date: Tuesday, November 15, 2016

Title: Health Services Research - Poster III

Session Type: ACR Poster Session C

Session Time: 9:00AM-11:00AM

Background/Purpose: This study examined treatment patterns in a rheumatology patient (pt) population initially prescribed innovator infliximab (IFX) that either switched to biosimilar infliximab (CT-P13) or continued on IFX following availability of CT-P13 in the Turkish healthcare system.

Methods: Adult pts with ≥1 diagnosis code (ICD-10-CM M05.X; M06.X) for rheumatoid arthritis (RA) and a prescription for IFX were identified in a national Turkish health care database during the study period (01DEC2010-01DEC2015). Eligible pts were those who continued on IFX (Continuers cohort; CC) or switched from IFX to CT-P13 (Switchers cohort; SC) during the identification period; had continuous medical/pharmacy benefit enrollment ≥12 months before and ≥6 months after the index date (date of switch for SC and a random IFX prescription date for CC); had a prescription claim for IFX within 16 weeks of the index date during the baseline period. Demographics, concomitant disease, medications, and treatment patterns (dose, refill interval, discontinuation, and switch) were summarized. A confirmed discontinuation was defined as a switch to another biologic medication or the absence of an index biologic claim for ≥120 days without censoring. Patient weight was unavailable in the dataset.

Results: Key results are shown in the Table and Figure. A total of 3018 pts met study criteria. The majority (95%; n=2870; CC) continued on IFX and had a mean age of 44 years; 46% were female and mean follow up of 12 months. A total of 148 pts (5%) switched to CT-P13 ( SC) and had mean age of 44 years; 51% female and mean follow up of 9 months. Approximately 40% of pts in each cohort had a concomitant diagnosis for ankylosing spondylitis (AS; Table). Other concomitant diseases and medications appeared balanced between cohorts. In the CC, pts had an average of 4.7 infusions at a mean dose of 4.4 vials approximately every 10 weeks. In the SC, pts had an average of 2.6 infusions at a mean dose of 3.6 vials approximately every 10 weeks. Therapy discontinuation occurred in 38% in the CC; average time to any discontinuation or censoring of IFX was 256 days (Table). In the SC, CT-P13 discontinuation was observed in 82%; average time to any discontinuation or censoring of CT-P13 was 124 days; 74% of SC switched to another biologic with 94% of these returning to IFX.

Conclusion: This study shows switching from IFX to CT-P13 was infrequent. However, in those switching to CT-P13, a high percentage (82%) of CT-P13 discontinuation was observed and the majority returned to IFX. Further studies are needed to understand the reasons for these observations.

	Switchers Cohort		Continuers Cohort
	(N=148)		(N=2870)
	N/Mean	%/SD	N/Mean	%/SD
Age (Mean) (years)	44	13	44	12
Gender
Female	75	51%	1,332	46 %
Average Length of Follow up Period ( in Months)	9	2	12	3
Concomitant Disease During Baseline Period
Ankylosing Spondylitis	73	49%	1,214	42%
Psoriatic Arthritis or Psoriasis	19	13%	582	20%
Crohn’s Disease	6	4%	191	7%
Ulcerative Colitis	8	5%	157	5%
Concomitant RA-Medications During Follow-Up Period
Methotrexate	31	21%	652	23%
Sulfasalazine	21	14%	340	12%
Dosing Characteristics
Average # of doses within follow up period	2.6	1.6	4.7	2.4
Mean # of weeks between doses	10.1	5.1	9.9	3.8
Mean # of days between 1st and 2^nd dose	75	48	70	34
Mean # of days between 2nd and 3rd dose	72	38	70	29
Mean # of days between 3rd and 4th dose	65	31	67	26
Mean # of vials per Infusion	3.6	1.6	4.4	1.9
Switching
# and % of patients with ≥1 switch	110	74%	471	16%
% of Primary Switches from CT-P13 to IFX	103	94%	NA	NA
Discontinuation
# of Patients Confirmed to Have Discontinued	121	82%	1,089	38%
Time to confirmed discontinuation (days)	94	58	126	91
Time to any discontinuation or censoring (days):	124	87	256	138

Disclosure: Y. Yazici, Janssen Scientific Affairs, LLC, 2; L. Xie, Janssen Scientific Affairs, LLC, 5; A. Ogbomo, Janssen Scientific Affairs, LLC, 5; D. Parenti, Janssen Scientific Affairs, LLC, 3; K. Goyal, Janssen Scientific Affairs, LLC, 3; A. Teeple, Janssen Scientific Affairs, LLC, 3; L. A. Ellis, Janssen Scientific Affairs, LLC, 3; I. Simsek, Janssen Scientific Affairs, LLC, 2.

To cite this abstract in AMA style:

Yazici Y, Xie L, Ogbomo A, Parenti D, Goyal K, Teeple A, Ellis LA, Simsek I. A Descriptive Analysis of Real-World Treatment Patterns in a Turkish Rheumatology Population That Continued Innovator Infliximab (Remicade) Therapy or Switched to Biosimilar Infliximab [abstract]. Arthritis Rheumatol. 2016; 68 (suppl 10). https://acrabstracts.org/abstract/a-descriptive-analysis-of-real-world-treatment-patterns-in-a-turkish-rheumatology-population-that-continued-innovator-infliximab-remicade-therapy-or-switched-to-biosimilar-infliximab/. Accessed .

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