Please use this identifier to cite or link to this item: http://hdl.handle.net/1942/47628
Title: IBD-linked Genetic Variance in Intestinal Transplantation A Multicenter Cohort Analysis
Authors: Dubois, Antoine
Jans, Deborah S.
Canovai, Emilio
Gentilini, Maria V.
Butler, Andrew J.
Amin, Irum
Sharkey, Lisa
Lacaille, Florence
Chardot, Christophe
Talayero, Paloma
Lasa-Lazaro, Maria
Calvo-Pulido, Jorge
Wauters, Lucas
Vanuytsel, Tim
Gondolesi, Gabriel E.
Pirenne, Jacques
Hannes, Laurens
FIEUWS, Steffen 
Cleynen, Isabelle
Verstockt, Sare
Ceulemans, Laurens J.
Issue Date: 2025
Publisher: LIPPINCOTT WILLIAMS & WILKINS
Source: Annals of surgery, 282 (5) , p. 827 -836
Abstract: Background: In solid organ transplantation, the intestine remains the most challenging. Previous studies have linked NOD2 genetic variation to intestinal transplantation (ITx) outcomes. Since then, a larger set of inflammatory bowel disease-associated genetic variants (IBDGVs) has been identified. This study aims to explore the prevalence and association of these IBDGVs with ITx outcomes. Method: Clinical data and DNA from 150 donor/recipient pairs were collected from 5 ITx centers (Leuven, Cambridge, Paris, Madrid, Buenos Aires). Genotyping-by-sequencing of 540 IBDGVs was performed, and genetic European individuals (53 donors, 101 recipients, EUR cohort) were selected. Associations between ITx outcomes [patient/graft survival and acute/chronic rejection (AR/CR)] and IBDGVs were separately analyzed if carried by the donors, the recipients, and the donor-AND-recipient using Cox regression, followed by pathway analysis (P<0.05). Results: Across all analyses (EUR cohort), multiple associations (P<0.05) were identified between IBDGVs and ITx outcomes, including 79 with AR, 34 with CR, 113 with patient survival, and 102 with graft survival. Donor/recipient IBDGVs had mixed protective (HR<1) and detrimental influences (HR>1) on outcomes, while donor-AND-recipient IBDGVs were predominantly harmful. Pathway analysis of donor-AND-recipient IBDGV-related genes showed enrichment in innate/adaptive immunity and epithelial barrier function, particularly in IL-12 and S100 family signaling, phagosome formation, and microbial pattern recognition. Upstream regulatory analysis confirmed the link to microbial sensing (31% of the genes) and antibody-mediated immune responses (20%). Conclusion: Several IBDGVs associated with ITx outcomes were identified in a multicenter genetic European cohort. These findings highlight potential markers for improving donor selection and post-transplant management.
Notes: Ceulemans, LJ (corresponding author), Univ Hosp Leuven, Leuven Intestinal Failure & Transplantat LIFT, Leuven, Belgium.; Ceulemans, LJ (corresponding author), Univ Hosp Leuven, Dept Thorac Surg, Leuven, Belgium.; Ceulemans, LJ (corresponding author), Katholieke Univ Leuven, Dept Chron Dis & Metab, Lab Resp Dis & Thorac Surg BREATHE, Leuven, Belgium.
antoine.dubois@kuleuven.be; deborah.jans@kuleuven.be;
emilio.canovai@ouh.nhs.uk; mgentilini@ffavaloro.org;
andrew.butler13@nhs.net; irum.amin@nhs.net; lisasharkey@icloud.com;
florence.lacaille@aphp.fr; christophe.chardot@aphp.fr;
paloma.talayero@salud.madrid.org; marialasalazaro@gmail.com;
jcalvopulido@outlook.es; lucas.wauters@uzleuven.be;
tim.vanuytsel@uzleuven.be; gegondolesi@me.com;
jacques.pirenne@uzleuven.be; laurens.hannes@kuleuven.be;
steffen.fieuws@kuleuven.be; isabelle.cleynen@kuleuven.be;
sare.verstockt@kuleuven.be; laurens.ceulemans@uzleuven.be
Keywords: genetic association study;inflammatory bowel disease;intestinal transplantation
Document URI: http://hdl.handle.net/1942/47628
ISSN: 0003-4932
e-ISSN: 1528-1140
DOI: 10.1097/SLA.0000000000006896
ISI #: 001591650000013
Category: A1
Type: Journal Contribution
Appears in Collections:Research publications

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