Predictors of anti-TNF treatment failure in anti-TNF-naive patients with active luminal Crohn's disease: a prospective, multicentre, cohort study.

Adalimumab / immunology Adult Age Factors Antibodies / immunology Azathioprine / therapeutic use Cohort Studies Crohn Disease / drug therapy Drug Therapy, Combination Female Humans Immunosuppressive Agents / therapeutic use Infliximab / immunology Leukocyte Count Male Mercaptopurine / therapeutic use Methotrexate / therapeutic use Middle Aged Proportional Hazards Models Prospective Studies Risk Factors Serum Albumin / metabolism Smoking / epidemiology Treatment Failure Treatment Outcome Tumor Necrosis Factor Inhibitors / immunology Young Adult

Journal

The lancet. Gastroenterology & hepatology

ISSN: 2468-1253

Titre abrégé: Lancet Gastroenterol Hepatol

Pays: Netherlands

ID NLM: 101690683

Informations de publication

Date de publication:
05 2019

Historique:

received: 21 10 2018

revised: 13 12 2018

accepted: 18 12 2018

pubmed: 3 3 2019

medline: 3 6 2020

entrez: 3 3 2019

Statut: ppublish

Résumé

Anti-TNF drugs are effective treatments for the management of Crohn's disease but treatment failure is common. We aimed to identify clinical and pharmacokinetic factors that predict primary non-response at week 14 after starting treatment, non-remission at week 54, and adverse events leading to drug withdrawal. The personalised anti-TNF therapy in Crohn's disease study (PANTS) is a prospective observational UK-wide study. We enrolled anti-TNF-naive patients (aged ≥6 years) with active luminal Crohn's disease at the time of first exposure to infliximab or adalimumab between March 7, 2013, and July 15, 2016. Patients were evaluated for 12 months or until drug withdrawal. Demographic data, smoking status, age at diagnosis, disease duration, location, and behaviour, previous medical and drug history, and previous Crohn's disease-related surgeries were recorded at baseline. At every visit, disease activity score, weight, therapy, and adverse events were recorded; drug and total anti-drug antibody concentrations were also measured. Treatment failure endpoints were primary non-response at week 14, non-remission at week 54, and adverse events leading to drug withdrawal. We used regression analyses to identify which factors were associated with treatment failure. We enrolled 955 patients treated with infliximab (753 with originator; 202 with biosimilar) and 655 treated with adalimumab. Primary non-response occurred in 295 (23·8%, 95% CI 21·4-26·2) of 1241 patients who were assessable at week 14. Non-remission at week 54 occurred in 764 (63·1%, 60·3-65·8) of 1211 patients who were assessable, and adverse events curtailed treatment in 126 (7·8%, 6·6-9·2) of 1610 patients. In multivariable analysis, the only factor independently associated with primary non-response was low drug concentration at week 14 (infliximab: odds ratio 0·35 [95% CI 0·20-0·62], p=0·00038; adalimumab: 0·13 [0·06-0·28], p<0·0001); the optimal week 14 drug concentrations associated with remission at both week 14 and week 54 were 7 mg/L for infliximab and 12 mg/L for adalimumab. Continuing standard dosing regimens after primary non-response was rarely helpful; only 14 (12·4% [95% CI 6·9-19·9]) of 113 patients entered remission by week 54. Similarly, week 14 drug concentration was also independently associated with non-remission at week 54 (0·29 [0·16-0·52] for infliximab; 0·03 [0·01-0·12] for adalimumab; p<0·0001 for both). The proportion of patients who developed anti-drug antibodies (immunogenicity) was 62·8% (95% CI 59·0-66·3) for infliximab and 28·5% (24·0-32·7) for adalimumab. For both drugs, suboptimal week 14 drug concentrations predicted immunogenicity, and the development of anti-drug antibodies predicted subsequent low drug concentrations. Combination immunomodulator (thiopurine or methotrexate) therapy mitigated the risk of developing anti-drug antibodies (hazard ratio 0·39 [95% CI 0·32-0·46] for infliximab; 0·44 [0·31-0·64] for adalimumab; p<0·0001 for both). For infliximab, multivariable analysis of immunododulator use, and week 14 drug and anti-drug antibody concentrations showed an independent effect of immunomodulator use on week 54 non-remission (odds ratio 0·56 [95% CI 0·38-0·83], p=0·004). Anti-TNF treatment failure is common and is predicted by low drug concentrations, mediated in part by immunogenicity. Clinical trials are required to investigate whether personalised induction regimens and treatment-to-target dose intensification improve outcomes. Guts UK, Crohn's and Colitis UK, Cure Crohn's Colitis, AbbVie, Merck Sharp and Dohme, Napp Pharmaceuticals, Pfizer, and Celltrion.

Sections du résumé

BACKGROUND

METHODS

The personalised anti-TNF therapy in Crohn's disease study (PANTS) is a prospective observational UK-wide study. We enrolled anti-TNF-naive patients (aged ≥6 years) with active luminal Crohn's disease at the time of first exposure to infliximab or adalimumab between March 7, 2013, and July 15, 2016. Patients were evaluated for 12 months or until drug withdrawal. Demographic data, smoking status, age at diagnosis, disease duration, location, and behaviour, previous medical and drug history, and previous Crohn's disease-related surgeries were recorded at baseline. At every visit, disease activity score, weight, therapy, and adverse events were recorded; drug and total anti-drug antibody concentrations were also measured. Treatment failure endpoints were primary non-response at week 14, non-remission at week 54, and adverse events leading to drug withdrawal. We used regression analyses to identify which factors were associated with treatment failure.

FINDINGS

We enrolled 955 patients treated with infliximab (753 with originator; 202 with biosimilar) and 655 treated with adalimumab. Primary non-response occurred in 295 (23·8%, 95% CI 21·4-26·2) of 1241 patients who were assessable at week 14. Non-remission at week 54 occurred in 764 (63·1%, 60·3-65·8) of 1211 patients who were assessable, and adverse events curtailed treatment in 126 (7·8%, 6·6-9·2) of 1610 patients. In multivariable analysis, the only factor independently associated with primary non-response was low drug concentration at week 14 (infliximab: odds ratio 0·35 [95% CI 0·20-0·62], p=0·00038; adalimumab: 0·13 [0·06-0·28], p<0·0001); the optimal week 14 drug concentrations associated with remission at both week 14 and week 54 were 7 mg/L for infliximab and 12 mg/L for adalimumab. Continuing standard dosing regimens after primary non-response was rarely helpful; only 14 (12·4% [95% CI 6·9-19·9]) of 113 patients entered remission by week 54. Similarly, week 14 drug concentration was also independently associated with non-remission at week 54 (0·29 [0·16-0·52] for infliximab; 0·03 [0·01-0·12] for adalimumab; p<0·0001 for both). The proportion of patients who developed anti-drug antibodies (immunogenicity) was 62·8% (95% CI 59·0-66·3) for infliximab and 28·5% (24·0-32·7) for adalimumab. For both drugs, suboptimal week 14 drug concentrations predicted immunogenicity, and the development of anti-drug antibodies predicted subsequent low drug concentrations. Combination immunomodulator (thiopurine or methotrexate) therapy mitigated the risk of developing anti-drug antibodies (hazard ratio 0·39 [95% CI 0·32-0·46] for infliximab; 0·44 [0·31-0·64] for adalimumab; p<0·0001 for both). For infliximab, multivariable analysis of immunododulator use, and week 14 drug and anti-drug antibody concentrations showed an independent effect of immunomodulator use on week 54 non-remission (odds ratio 0·56 [95% CI 0·38-0·83], p=0·004).

INTERPRETATION

Anti-TNF treatment failure is common and is predicted by low drug concentrations, mediated in part by immunogenicity. Clinical trials are required to investigate whether personalised induction regimens and treatment-to-target dose intensification improve outcomes.

FUNDING

Guts UK, Crohn's and Colitis UK, Cure Crohn's Colitis, AbbVie, Merck Sharp and Dohme, Napp Pharmaceuticals, Pfizer, and Celltrion.

Identifiants

DOI: 10.1016/S2468-1253(19)30012-3 PMID: 30824404

pubmed: 30824404

pii: S2468-1253(19)30012-3

doi: 10.1016/S2468-1253(19)30012-3

pii:

doi:

Substances chimiques

Antibodies 0

Immunosuppressive Agents 0

Serum Albumin 0

Tumor Necrosis Factor Inhibitors 0

Infliximab B72HH48FLU

Mercaptopurine E7WED276I5

Adalimumab FYS6T7F842

Azathioprine MRK240IY2L

Methotrexate YL5FZ2Y5U1

Types de publication

Journal Article Multicenter Study Observational Study Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

Pagination

341-353

Subventions

Organisme : Medical Research Council

ID : MC_PC_14127

Pays : United Kingdom

Organisme : Medical Research Council

ID : MR/M00533X/1

Pays : United Kingdom

Organisme : Medical Research Council

ID : MR/S034919/1

Pays : United Kingdom

Investigateurs

Vinod Patel (V)

Zia Mazhar (Z)

Rebecca Saich (R)

Ben Colleypriest (B)

Tony C Tham (TC)

Tariq H Iqbal (TH)

Vishal Kaushik (V)

Senthil Murugesan (S)

Salil Singh (S)

Sean Weaver (S)

Cathryn Preston (C)

Assad Butt (A)

Melissa Smith (M)

Dharamveer Basude (D)

Amanda Beale (A)

Sarah Langlands (S)

Natalie Direkze (N)

Miles Parkes (M)

Franco Torrente (F)

Juan De La Revella Negro (J)

Chris Ewen MacDonald (CE)

Stephen M Evans (SM)

Anton V J Gunasekera (AVJ)

Alka Thakur (A)

David Elphick (D)

Achuth Shenoy (A)

Chuka U Nwokolo (CU)

Anjan Dhar (A)

Andrew T Cole (AT)

Anurag Agrawal (A)

Stephen Bridger (S)

Julie Doherty (J)

Sheldon C Cooper (SC)

Shanika de Silva (S)

Craig Mowat (C)

Phillip Mayhead (P)

Charlie Lees (C)

Gareth Jones (G)

Tariq Ahmad (T)

James W Hart (JW)

Daniel R Gaya (DR)

Richard K Russell (RK)

Lisa Gervais (L)

Paul Dunckley (P)

Tariq Mahmood (T)

Paul J R Banim (PJR)

Sunil Sonwalkar (S)

Deb Ghosh (D)

Rosemary H Phillips (RH)

Amer Azaz (A)

Shaji Sebastian (S)

Richard Shenderey (R)

Lawrence Armstrong (L)

Claire Bell (C)

Radhakrishnan Hariraj (R)

Helen Matthews (H)

Hasnain Jafferbhoy (H)

Christian P Selinger (CP)

Veena Zamvar (V)

John S De Caestecker (JS)

Anne Willmott (A)

Richard Miller (R)

Palani Sathish Babu (PS)

Christos Tzivinikos (C)

Stuart L Bloom (SL)

Guy Chung-Faye (G)

Nicholas M Croft (NM)

John Me Fell (JM)

Marcus Harbord (M)

Ailsa Hart (A)

Ben Hope (B)

Peter M Irving (PM)

James O Lindsay (JO)

Joel E Mawdsley (JE)

Alistair McNair (A)

Kevin J Monahan (KJ)

Charles D Murray (CD)

Timothy Orchard (T)

Thankam Paul (T)

Richard Pollok (R)

Neil Shah (N)

Sonia Bouri (S)

Matt W Johnson (MW)

Anita Modi (A)

Kasamu Dawa Kabiru (KD)

B K Baburajan (BK)

Bim Bhaduri (B)

Andrew Adebayo Fagbemi (AA)

Scott Levison (S)

Jimmy K Limdi (JK)

Gill Watts (G)

Stephen Foley (S)

Arvind Ramadas (A)

George MacFaul (G)

John Mansfield (J)

Leonie Grellier (L)

Mary-Anne Morris (MA)

Mark Tremelling (M)

Chris Hawkey (C)

Sian Kirkham (S)

Charles Pj Charlton (CP)

Astor Rodrigues (A)

Alison Simmons (A)

Stephen J Lewis (SJ)

Jonathon Snook (J)

Mark Tighe (M)

Patrick M Goggin (PM)

Aminda N De Silva (AN)

Simon Lal (S)

Mark S Smith (MS)

Simon Panter (S)

J R Fraser Cummings (JRF)

Suranga Dharmisari (S)

Martyn Carter (M)

David Watts (D)

Zahid Mahmood (Z)

Bruce McLain (B)

Sandip Sen (S)

Anna J Pigott (AJ)

David Hobday (D)

Emma Wesley (E)

Richard Johnston (R)

Cathryn Edwards (C)

John Beckly (J)

Deven Vani (D)

Subramaniam Ramakrishnan (S)

Rakesh Chaudhary (R)

Nigel J Trudgill (NJ)

Rachel Cooney (R)

Andy Bell (A)

Neeraj Prasad (N)

John N Gordon (JN)

Matthew J Brookes (MJ)

Andy Li (A)

Stephen Gore (S)

Commentaires et corrections

Type : CommentIn

Predictors of anti-TNF treatment failure in anti-TNF-naive patients with active luminal Crohn's disease: a prospective, multicentre, cohort study.

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