The Influence of Subclinical Active Inflammation on IFX Pharmacokinetic Modeling and Disease Progression Assessment: Findings from a Prospective Real-World Study in Inflammatory Bowel Disease Patients-Reference-Cited by-同舟云学术

The Influence of Subclinical Active Inflammation on IFX Pharmacokinetic Modeling and Disease Progression Assessment: Findings from a Prospective Real-World Study in Inflammatory Bowel Disease Patients

Published:2024-01-19 Issue:7 Volume:18 Page:1102-1112
ISSN:1873-9946
Container-title:Journal of Crohn's and Colitis
language:en
Short-container-title:

Author:

Magro Fernando¹²³⁴⁵^ORCID,Fernandes Samuel⁶⁷,Patita Marta⁸,Arroja Bruno⁹,Lago Paula⁵¹⁰,Rosa Isadora¹¹,Tavares de Sousa Helena¹²¹³,Ministro Paula⁵¹⁴,Mocanu Irina⁸,Vieira Ana⁸,Castela Joana¹¹,Moleiro Joana¹¹,Roseira Joana¹²¹³^ORCID,Cancela Eugénia¹⁴,Sousa Paula¹⁴^ORCID,Portela Francisco⁵¹⁵,Correia Luís⁵⁶,Moreira Paula⁴,Dias Sandra⁵,Afonso Joana⁵,Danese Silvio¹⁶¹⁷^ORCID,Peyrin-Biroulet Laurent¹⁸,Vucicevic Katarina M¹⁹,Santiago Mafalda⁵

Affiliation:

1. Department of Biomedicine, Unit of Pharmacology and Therapeutics, Faculty of Medicine, University of Porto , Porto , Portugal

2. Department of Gastroenterology, São João Hospital University Centre , Porto , Portugal

3. Centre for Health Technology and Services Research, Health Research Network (CINTESIS@RISE), Faculty of Medicine of the University of Porto , Portugal

4. Clinical Pharmacology Unit, São João Hospital University Centre , Porto , Portugal

5. Portuguese Group of Studies in Inflammatory Bowel Disease (Grupo de Estudos da Doença Inflamatória Intestinal - GEDII) , Porto , Portugal

6. Department of Gastroenterology, Northern Lisbon University Hospital Centre , Lisbon , Portugal

7. Clinica Universitária de Gastrenterologia da Universidade de Medicina de Lisboa , Lisbon , Portugal

8. Department of Gastroenterology, Garcia da Orta Hospital , Almada , Portugal

9. Department of Gastroenterology, Braga Hospital , Braga , Portugal

10. Department of Gastroenterology, Porto Hospital University Centre , Porto , Portugal

11. Department of Gastroenterology, IPOLFG, EPE , Lisbon , Portugal

12. Department of Gastroenterology, Algarve Hospital University Centre - Portimão Unit , Portimão , Portugal

13. ABC – Algarve Biomedical Center, University of Algarve , Faro , Portugal

14. Department of Gastroenterology, Viseu-Tondela Hospital Centre , Viseu , Portugal

15. Department of Gastroenterology, Coimbra Hospital University Centre , Coimbra , Portugal

16. Department of Biomedical Sciences, Humanitas University , Milan , Italy

17. IBD Center, Humanitas Research Hospital, IRCCS , Milan , Italy

18. Department of Gastroenterology and Inserm NGERE U1256, University Hospital of Nancy, University of Lorraine , Nancy , France

19. Department of Pharmacokinetics and Clinical Pharmacy, University of Belgrade , Serbia

Abstract

Abstract Background and aims Effective management of inflammatory bowel disease (IBD) relies on a comprehensive understanding of infliximab (IFX) pharmacokinetics (PK). This study’s primary goal was to develop a robust PK model, identifying key covariates influencing IFX clearance (CL), while concurrently evaluating the risk of disease progression during the maintenance phase of IBD treatment. Methods The multicenter, prospective, real-world DIRECT study was conducted in several care centers, which included 369 IBD patients in the maintenance phase of IFX therapy. A two-compartment population PK model was used to determine IFX CL and covariates. Logistic and Cox regressions were applied to elucidate the associations between disease progression and covariates embedded in the PK model. Results The PK model included the contributions of weight, albumin, antidrug antibody (ADA), and fecal calprotectin (FC). On average, higher ADA, FC concentration and weight, and lower albumin concentration resulted in higher IFX CL. In the multivariate regression analyses, FC levels influenced the odds of disease progression in the majority of its definitions, when adjusted for several confounding factors. Additionally, alongside FC, both IFX and CL demonstrated a significant impact on the temporal aspect of disease progression. Conclusion In this 2-year real-world study, readily available clinical covariates, notably FC, significantly impacted IFX availability in IBD patients. We demonstrated that subclinical active inflammation, as mirrored by FC or CRP, substantially influenced IFX clearance. Importantly, FC emerged as a pivotal determinant, not only of IFX pharmacokinetics but also of disease progression. These findings underscore the need to integrate FC into forthcoming IFX pharmacokinetic models, amplifying its clinical significance.

Funder

Portuguese Study Group in Inflammatory Bowel Disease

Publisher

Oxford University Press (OUP)

Link

https://academic.oup.com/ecco-jcc/advance-article-pdf/doi/10.1093/ecco-jcc/jjae014/56658479/jjae014.pdf

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