External validation of serum biomarkers predicting short-term and mid/long-term relapse in patients with Crohn's disease stopping infliximab.
CROHN'S DISEASE
INFLAMMATORY BOWEL DISEASE
INFLIXIMAB
Journal
Gut
ISSN: 1468-3288
Titre abrégé: Gut
Pays: England
ID NLM: 2985108R
Informations de publication
Date de publication:
12 Aug 2024
12 Aug 2024
Historique:
received:
12
04
2024
accepted:
28
07
2024
medline:
13
8
2024
pubmed:
13
8
2024
entrez:
12
8
2024
Statut:
aheadofprint
Résumé
In patients with Crohn's disease (CD) on combination therapy (infliximab and immunosuppressant) and stopping infliximab (cohort from the study of infliximab diSconTinuation in CrOhn's disease patients in stable Remission on combined therapy with Immunosuppressors (STORI)), the risk of short-term (≤6 months) and mid/long-term relapse (>6 months) was associated with distinct blood protein profiles. Our aim was to test the external validity of this finding in the SPARE cohort (A proSpective Randomized Controlled Trial comParing infliximAb-antimetabolites Combination Therapy to Anti-metabolites monotheRapy and Infliximab monothErapy in Crohn's Disease Patients in Sustained Steroid-free Remission on Combination Therapy). In SPARE, patients with CD in sustained steroid-free clinical remission and on combination therapy were randomly allocated to three arms: continuing combination therapy, stopping infliximab or stopping immunosuppressant. In the baseline serum of the STORI and SPARE (arm stopping infliximab) cohorts, we studied 202 immune-related proteins. The proteins associated with time to relapse (univariable Cox model) were compared between STORI and SPARE. The discriminative ability of biomarkers (individually and combined in pairs) was evaluated by the c-statistic (concordance analysis) which was compared with C-reactive protein (CRP), faecal calprotectin and a previously validated model (CEASE). In STORI and SPARE, distinct blood protein profiles were associated with the risk of short-term (eg, high level: CRP, haptoglobin, interleukin-6, C-type lectin domain family 4 member C) and mid/long-term relapse (eg, low level: Fms-related tyrosine kinase 3 ligand, kallistatin, fibroblast growth factor 2). At external validation, the top 10 biomarker pairs showed a higher c-statistic than the CEASE model, CRP and faecal calprotectin in predicting short-term (0.76-0.80 vs 0.74 vs 0.71 vs 0.69, respectively) and mid/long-term relapse (0.66-0.68 vs 0.61 vs 0.52 vs 0.59, respectively). In patients with CD stopping infliximab, we confirm that the risk of short-term and mid/long-term relapse is associated with distinct blood protein profiles showing the potential to guide infliximab withdrawal. NCT00571337 and NCT02177071.
Identifiants
pubmed: 39134391
pii: gutjnl-2024-332648
doi: 10.1136/gutjnl-2024-332648
pii:
doi:
Banques de données
ClinicalTrials.gov
['NCT02177071', 'NCT00571337']
Types de publication
Journal Article
Langues
eng
Sous-ensembles de citation
IM
Investigateurs
Jean-Louis Dupas
(JL)
David Laharie
(D)
Jean-Marie Reimund
(JM)
Yoram Bouhnik
(Y)
Pauline Jouet
(P)
Martine De Vos
(M)
Jacques Belaiche
(J)
Edouard Louis
(E)
Jean-Frédéric Colombel
(JF)
Gwenola Vernier-Massouille
(G)
Stéphane Nancey
(S)
Jean Charles Grimaud
(JC)
Michel Veyrac
(M)
Arnaud Boureille
(A)
Mathurin Flamant
(M)
Raymond Jian
(R)
Philippe Marteau
(P)
Marc Lemann
(M)
Matthieu Allez
(M)
Guillaume Savoye
(G)
Bernard Duclos
(B)
Laurence Picon
(L)
A Andrews
(A)
M Sparrow
(M)
R Leong
(R)
S Connor
(S)
G Radforth-Smith
(G)
P De Cruz
(P)
F Baert
(F)
E Louis
(E)
P Bossuyt
(P)
M Resche-Rignon
(M)
N Ding
(N)
S Almer
(S)
S Ben-Horin
(S)
J F Colombel
(JF)
B Siegmund
(B)
J Preiss
(J)
A Stallmach
(A)
T Liceni
(T)
O Grip
(O)
J Halfvarson
(J)
D Durai
(D)
F Cummings
(F)
C Seilinger
(C)
M Parkes
(M)
J Lindsay
(J)
G Lambrecht
(G)
P Van Hootegem
(P)
J F Rahier
(JF)
M Dewitte
(M)
X Hebuterne
(X)
E Chanteloup
(E)
R Altwegg
(R)
S Nancey
(S)
G Bouguen
(G)
G Pineton de Chambrun
(G)
F Pollenot
(F)
Y Bouhnik
(Y)
L Vuitton
(L)
M Nachury
(M)
D Laharie
(D)
S Nancey
(S)
M Fumery
(M)
G Bouguen
(G)
L Picon
(L)
C Gilletta
(C)
S Viennot
(S)
X Roblin
(X)
J Satsangi
(J)
J Lindsay
(J)
M Parkes
(M)
P Irving
(P)
C Lamb
(C)
D Durai
(D)
R Pollok
(R)
G D'haens
(G)
E Hertervig
(E)
O Grip
(O)
J Halfvarsson
(J)
Informations de copyright
© Author(s) (or their employer(s)) 2024. No commercial re-use. See rights and permissions. Published by BMJ.
Déclaration de conflit d'intérêts
Competing interests: PB has received research grants from AbbVie, Amgen, Celltrion, Mylan, Pfizer and Takeda; lecture fees from AbbVie, Celltrion, Janssen, Lilly and Takeda; and consulting fees from AbbVie, Arena Pharmaceuticals, Bristol Myers Squibb, Celltrion, Dr Falk Pharma, Galapagos, Janssen, Lilly, Pentax, PSI-CRO, Roche, Takeda and Tetrameros. LV has received fees from AbbVie, Amgen, Biogen, Mylan, Takeda, MSD, Janssen, Pfizer, Ferring and Galapagos. SV has received speaker’s fees from AbbVie, Ferring, Janssen and Takeda. J-FC has received grants from AbbVie, Janssen Pharmaceuticals, Prometheus, Takeda and Bristol Myers Squibb; receiving payment for lectures from AbbVie, and Takeda; receiving consulting fees from AbbVie, Amgen, AnaptysBio, Allergan, Arena Pharmaceuticals, Boehringer Ingelheim, Bristol Myers Squibb, Celgene Corporation, Celltrion, Eli Lilly, Ferring Pharmaceuticals, Galmed Research, Glaxo Smith Kline, Genentech (Roche), Janssen Pharmaceuticals, Kaleido Biosciences, Immunic, Invea, Iterative Scopes, Merck, Landos, Microba Life Science, Novartis, Otsuka Pharmaceutical, Pfizer, Protagonist Therapeutics, Prometheus, Sanofi, Seres, Takeda, Teva, TiGenix, Vifor; and hold stock options in Intestinal Biotech Development. EL has received educational and research grants from Janssen, Pfizer, AbbVie and Takeda, Fresenius-Kabi; speaker fees from AbbVie, Dr Falk Pharma, Ferring, Janssen, Pfizer, Celgene, Bristol Myers Squibb (BMS), Galapagos and Takeda; advisory board fees for AbbVie, Celgene, Ferring, Janssen, BMS, Pfizer, Takeda, Gilead-Galapagos, Arena and Elli Lilly; and consultancy fees from AbbVie.