DISCONTINUATION RATES FOLLOWING A SWITCH FROM A REFERENCE TO A BIOSIMILAR BIOLOGIC IN PATIENTS WITH INFLAMMATORY BOWEL DISEASE: A SYSTEMATIC REVIEW AND META-ANALYSIS

QUEIROZ, Natália Sousa Freitas; SAAD-HOSSNE, Rogerio; FRÓES, Renata de Sá Brito; PENNA, Francisco Guilherme Cancela e; GABRIEL, Stefania Burjack; MARTINS, Adalberta Lima; TEIXEIRA, Fabio Vieira

doi:10.1590/S0004-2803.202000000-45

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ORIGINAL ARTICLE • Arq. Gastroenterol. 57 (03) • Jul-Sep 2020 • https://doi.org/10.1590/S0004-2803.202000000-45 copy

DISCONTINUATION RATES FOLLOWING A SWITCH FROM A REFERENCE TO A BIOSIMILAR BIOLOGIC IN PATIENTS WITH INFLAMMATORY BOWEL DISEASE: A SYSTEMATIC REVIEW AND META-ANALYSIS

Taxas de descontinuação do tratamento após a troca de um biológico originador por um biossimilar em pacientes com doenças inflamatórias intestinais: revisão sistemática e metanálise

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

BACKGROUND:

Biologics have revolutionized the treatment of inflammatory bowel disease (IBD). However, these drugs had a significant influence on treatment-related costs, which resulted in the development of biosimilars.

OBJECTIVE:

This systematic review and meta-analysis aimed to evaluate the drug discontinuation rate in the IBD population who switched from originator to biosimilars in real-world switching studies and address potential nocebo effects as reasons for drug discontinuation.

METHODS:

Medline (via PubMed), EMBASE, Cochrane Library, and abstract databases of selected congresses were screened for reports of monoclonal antibody (mAb) switching with a minimum post-switch follow-up of >6 months or three infusions. All available information on discontinuation rates was assessed.

RESULTS:

A total of 30 observational studies were included, involving 3,594 patients with IBD. Twenty-six studies reported a switch from infliximab to CT-P13, two studies involved a switch to SB2, and switching information was not available in two studies. The discontinuation rates were 8%, 14%, and 21% at 6, 12, and 24 months, respectively. The main reasons for drug discontinuation and their respective risks were: disease worsening (2%), remission (4%), loss of adherence (4%), adverse events (5%), and loss of response (7%). The quality of the evidence ranged from low to very low depending on the outcome analyzed. Subjective symptoms leading to drug discontinuation were infrequently reported, and the nocebo effect was clearly assessed in just one of the included papers.

CONCLUSION:

Discontinuation rates following a switch to a biosimilar in patients with IBD increase over time. However, it was not possible to confirm the nocebo effect as a reason for discontinuation. Therefore, long-term studies evaluating the use of biosimilars to monitor adverse events and potential nocebo effects in post-marketing surveillance are still needed.

HEADINGS:
Inflammatory bowel diseases, drug therapy; Biological products; Therapeutic equivalency; Biosimilar pharmaceuticals; Review

Study	Population	Intervention	Follow-up	Study period
MEDLINE
Kim NH 2019	IBD (n: 368) (227 CD, 141 UC)	Switched infliximab to CT-P13 (n: 101)	12 months	No information
Chaparro M 2019	IBD (142 CD, 57 UC)	Switched infliximab to CT-P13 (n: 199)	18 months	45 months
Armuzzi A 2019	IBD (n: 810) (452 CD, 358 UC)	Switched infliximab to CT-P13 (n: 155)	392.8±232 days	17±13 infusions
Smits LJT 2019	IBD (n: 83) (57 CD, 24 UC, 2 IBD-U)	Switched infliximab to CT-P13 (n: 83)	12 and 24 months	24 months
Guerra Veloz MF 2018	IBD (n: 98) (67 CD, 31 UC)	Switched infliximab to CT-P13 (n: 98)	12 months	60 months
Bergqvist V 2018	IBD (n: 313) (195 CD, 118 UC)	Switched infliximab to CT-P13 (n: 313)	12 months	53 months
Guerra Veloz MF 2018	IBD (n: 167) (116 CD, 51 UC)	Switched infliximab to CT-P13 (n: 167)	12 months	No information
Høivik ML 2018	IBD (n: 143) (99 CD, 44 UC)	Switched infliximab to CT-P13 (n: 143)	18 months	81 months
Ratnakumaran R 2018	IBD (n: 191) (173 CD, 14 UC, 4 IBD-U)	Switched infliximab to CT-P13 (n: 191)	12 months	55 months
Boone NW 2018	IBD (n: 101) (73 CD, 28 UC)	Switched infliximab to CT-P13 (n: 101)	9 months	42 months
Avouac J 2018	IBD (n: 64) (41 CD, 23 UC)	Switched Infliximab to CT-P13 (n: 64)	9 months	47 months
Schmitz EMH 2018	IBD (n: 133) (88 CD, 45 UC)	Switched infliximab to CT-P13 (n: 133)	12 months	52 months
Smits LJT 2017	IBD (n: 83) (57 CD, 24 UC, 2 IBD-U)	Switched infliximab to CT-P13 (n: 83)	12 months	25 months
Argüelles-Arias F 2017	IBD (n: 98) (67 CD, 31 UC)	Switched infliximab to CT-P13 (n: 98)	12 months	60 months
Guerrero Puente L 2017	IBD (n: 36) (23 CD, 13 UC)	Switched infliximab to CT-P13 (n: 36)	9 months	33 months
Razanskaite V 2017	IBD (n: 143) (118 CD, 14 UC, 4 IBD-U)	Switched infliximab to CT-P13 (n: 143)	12 months	10 infusions
Fiorino G 2017	IBD (n: 547) (313 CD, 234 UC)	Switched infliximab to CT-P13 (n: 97)	6 months	18±14 infusions
Jahnsen J 2017	IBD (n: 56) (37 CD, 19 UC)	Switched infliximab to CT-P13 (n: 56)	6 months	44 months
Kolar M 2017	IBD (n: 74) (56 CD, 18 UC)	Switched infliximab toCT-P13 (n: 74)	14 months	36 months
Smits LJ 2016	IBD (n: 83) (57 CD, 24 UC, 2 IBD-U)	Switched infliximab toCT-P13 (n: 83)	6 months	24 months
Jung YS 2015	IBD (n: 36) (27 CD, 9 UC)	Switched infliximab or adalimumab to CT-P13 (n: 36)	8±3 infusions	No information
EMBASE
Fischer S 2018 (a)	IBD (n: 114) (72 CD, 42 UC)	Switched infliximab to sb2 (n: 114)	6 months	33 months
Bronswijk M 2018	IBD (n: 401) (285 CD, 116 UC)	Switched infliximab to ct-p13 (n: 361)	6 months	72 months
Fischer S 2018 (b)	IBD (n: 119) (76 CD, 43 UC)	Switched infliximab to sb2 (n: 119)	6 months	33 months
Plevris N 2018	CD (n: 110)	Switched infliximab to ct-p13 (n: 110)	12 months	48 months
Soret PA 2017	IBD (n: 64) (42 CD, 21 UC)	Switched infliximab to ct-p13 (n: 64)	9 months	35 months
Rodríguez Glez GE 2017	IBD (n: 72) (62 CD, 10 UC)	Switched infliximab to bs (n: 72)	12 months	51 months
Bennett KJ 2016	IBD (n: 104) (73 CD, 22 UC, 2 IBD-U)	Switched infliximab to bs (n: 104)	6 months	37 months
ECCO 2019
Guerra Veloz M 2019	IBD (n: 100) (64 CD, 36 UC)	Switched infliximab to CT-P13 (n: 100)	24 months	58 months
Bhandare AP 2019	IBD (n: 96) (52 CD, 44 UC)	Switched infliximab to CT-P13 (n: 96)	13 months	49 months

Certainty assessment							Results summary
N. participants (studies)	Risk of	Inconsistency	Indirect	Inaccuracy	Publishing Bias	Overall certainty	Study event rates (%)		Relative effect (95% CI)	Potential absolute effects
Follow-up	bias		Evidence			of evidence	BEFORE SWITCH	AFTER SWITCH		Risk BEFORE SWITCH	Risk difference AFTER SWITCH
Discontinuation 6m
2762 (10 observational studies)	not serious	very serious ^a	not serious	not serious	none	□〇〇〇 VERY LOW	0/1381 (0.0%)	111/1381 (8.0%)	RR 18.30 (7.40 to 45.28)	0 out of 100	8 more per 100 (from 5 more to 11 more) ^b
Discontinuation 9m
530 (4 observational studies)	not serious	not serious	not serious	not serious	none	□□〇〇 LOW	0/265 (0.0%)	38/265 (14.3%)	RR 20.00 (4.88 to 81.98)	0 out of 100	14 more per 100 (from 10 more to 19 more) ^b
Discontinuation 12m
3298 (12 observational studies)	not serious	very serious ^a	not serious	not serious	none	□〇〇〇 VERY LOW	0/1649 (0.0%)	250/1649 (15.2%)	RR 34.56 (15.36 to 77.77)	0 out of 100	14 more per 100 (from 10 more to 18 more) ^b
Discontinuation 18m
684 (2 observational studies)	not serious	very serious^a	not serious	serious^c	highly suspicious publication bias^d	□〇〇〇 VERY LOW	0/342 (0.0%)	96/342 (28.1%)	RR 65.95 (8.76 to 496.66)	0 out of 1.000	25 more per 1.000 (from 13 more to 63 more) ^b
Discontinuation 24m
383 (2 observational studies)	not serious	very serious^a	not serious	serious^c	none	□〇〇〇 VERY LOW	0/200 (0.0%)	40/183 (21.9%)	RR 41.53 (5.75 to 300.14)	0 out of 1.000	21 more per 1.000 (from 7 more to 35 more) ^b
Remission reason
1832 (7 observational studies)	not serious	not serious	not serious	not serious	none	□□〇〇 LOW	0/916 (0.0%)	35/916 (3.8%)	RR 11.0 (3.7 to 32.7)	0 out of 100	4 more per 100 (from 2 more to 5 more) ^b
Reason increased loss of response (disease worsening)
1024 (3 observational studies)	not serious	not serious	not serious	not serious	none	□□〇〇 LOW	0/512 (0.0%)	11/512 (2.1%)	RR 8.33 (1.54 to 45.12)	0 out of 100	2 more per 100 (from 1 more to 4 more) ^b
Reason loss of response
3076 (13 observational studies)	not serious	serious ^e	not serious	not serious	none	□〇〇〇 LOW	0/1538 (0.0%)	125/1538 (8.1%)	RR 15.39 (6.93 to 34.19)	0 out of 100	7 more per 100 (from 5 more to 10 more) ^b
Reason loss of adherence
1542 (8 observational studies)	not serious	not serious	not serious	not serious	none	□□〇〇 LOW	0/771 (0.0%)	31/771 (4.0%)	RR 8.75 (3.12 to 24.51)	0 out of 100	4 more per 100 (from 2 more to 6 more) ^b
Reason adverse events
4042 (17 observational studies)	not serious	not serious	not serious	not serious	none	□□〇〇 LOW	0/2021 (0.0%)	108/2021 (5.3%)	RR 13.71 (6.85 to 27.43)	0 out of 100	5 more per 100 (from 4 more to 6 more) ^b

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[1] Corresponding author: Natália Sousa Freitas Queiroz. E-mail: natalia.freitas@hc.fm.usp.br