Uptake of rheumatology biosimilars in the absence of forced switching

Di Giuseppe, Daniela; Frisell, Thomas; Ernestam, Sofia; Forsblad-D’Elia, Helena; Lindqvist, Elisabet; Lindström, Ulf; Sjöwall, Christopher; Askling, Johan

Uptake of rheumatology biosimilars in the absence of forced switching

Mark

Di Giuseppe, Daniela ; Frisell, Thomas ; Ernestam, Sofia ; Forsblad-D’Elia, Helena ; Lindqvist, Elisabet ^LU

; Lindström, Ulf ; Sjöwall, Christopher and Askling, Johan (2018) In Expert Opinion on Biological Therapy 18(5). p.499-504

Abstract: Background: To describe the uptake and system-level effects of the introduction of biosimilars in a setting without forced switching. Research design and methods: We used data from the Swedish Rheumatology Quality register from start of marketing of infliximab (Remsima® and Inflectra®) and etanercept (Benepali®) biosimilars until 31 December 2016. We compared users of each originator-product and its biosimilar(s) by line of treatment: bDMARD-naïve patients, non-medical switchers (vs. matched patients remaining on originator), and patients switching from a previous bDMARD of another type. Results: From the start of marketing 1343 patients started an infliximab biosimilar (22 months) and 2691 started etanercept (9 months). Overall, the... (More); Background: To describe the uptake and system-level effects of the introduction of biosimilars in a setting without forced switching. Research design and methods: We used data from the Swedish Rheumatology Quality register from start of marketing of infliximab (Remsima® and Inflectra®) and etanercept (Benepali®) biosimilars until 31 December 2016. We compared users of each originator-product and its biosimilar(s) by line of treatment: bDMARD-naïve patients, non-medical switchers (vs. matched patients remaining on originator), and patients switching from a previous bDMARD of another type. Results: From the start of marketing 1343 patients started an infliximab biosimilar (22 months) and 2691 started etanercept (9 months). Overall, the introduction of these biosimilars resulted in an increase of the total number of ongoing infliximab and etanercept treatments (originator + biosimilar) . At the end of the study period, biosimilars accounted for 31% of all infliximab treatments and 31% of all etanercept-treated patients. For each line of therapy, we noted only small differences in patient characteristics between those starting the originator product vs. its biosimilar(s). Conclusions: Introduction of biosimilars have effects beyond replacement of the originator product, in terms of an increased rate of bDMARD initiation. Selection to non-medical switching displayed no particular disease- or patient-characteristics.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/56160b18-9f12-4215-9274-0bf00047ee48

author

Di Giuseppe, Daniela ; Frisell, Thomas ; Ernestam, Sofia ; Forsblad-D’Elia, Helena ; Lindqvist, Elisabet ^LU

; Lindström, Ulf ; Sjöwall, Christopher and Askling, Johan

organization

Rheumatology

publishing date

2018-05-04

type

Contribution to journal

publication status

published

subject

Rheumatology and Autoimmunity

keywords

in

Expert Opinion on Biological Therapy

volume

18

issue

5

pages

499 - 504

publisher

Ashley Publications

external identifiers

pmid:29633865
scopus:85045151363

ISSN

1471-2598

DOI

10.1080/14712598.2018.1458089

language

English

LU publication?

yes

id

56160b18-9f12-4215-9274-0bf00047ee48

date added to LUP

2018-04-17 14:47:51

date last changed

2024-04-15 06:39:17

@article{56160b18-9f12-4215-9274-0bf00047ee48,
  abstract     = {{<p>Background: To describe the uptake and system-level effects of the introduction of biosimilars in a setting without forced switching. Research design and methods: We used data from the Swedish Rheumatology Quality register from start of marketing of infliximab (Remsima® and Inflectra®) and etanercept (Benepali®) biosimilars until 31 December 2016. We compared users of each originator-product and its biosimilar(s) by line of treatment: bDMARD-naïve patients, non-medical switchers (vs. matched patients remaining on originator), and patients switching from a previous bDMARD of another type. Results: From the start of marketing 1343 patients started an infliximab biosimilar (22 months) and 2691 started etanercept (9 months). Overall, the introduction of these biosimilars resulted in an increase of the total number of ongoing infliximab and etanercept treatments (originator + biosimilar) . At the end of the study period, biosimilars accounted for 31% of all infliximab treatments and 31% of all etanercept-treated patients. For each line of therapy, we noted only small differences in patient characteristics between those starting the originator product vs. its biosimilar(s). Conclusions: Introduction of biosimilars have effects beyond replacement of the originator product, in terms of an increased rate of bDMARD initiation. Selection to non-medical switching displayed no particular disease- or patient-characteristics.</p>}},
  author       = {{Di Giuseppe, Daniela and Frisell, Thomas and Ernestam, Sofia and Forsblad-D’Elia, Helena and Lindqvist, Elisabet and Lindström, Ulf and Sjöwall, Christopher and Askling, Johan}},
  issn         = {{1471-2598}},
  keywords     = {{bDMARD; biosimilar; rheumatology; uptake}},
  language     = {{eng}},
  month        = {{05}},
  number       = {{5}},
  pages        = {{499--504}},
  publisher    = {{Ashley Publications}},
  series       = {{Expert Opinion on Biological Therapy}},
  title        = {{Uptake of rheumatology biosimilars in the absence of forced switching}},
  url          = {{http://dx.doi.org/10.1080/14712598.2018.1458089}},
  doi          = {{10.1080/14712598.2018.1458089}},
  volume       = {{18}},
  year         = {{2018}},
}

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Uptake of rheumatology biosimilars in the absence of forced switching