Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study

Anja Poulsen; Marta Sorokina Alexdóttir; Lene Buhl Riis; Pernille Dige Ovesen; Julie Rasmussen; Mads Damsgaard Wewer; Viviane Lin; Ronja M B Lagström; Marwah Al-Sheikh; Emilie Dahl; Annedorte Ries; Martin Pehrsson; Thomai Tsapanou-Katranara; Peter-Martin Krarup; Ismail Gögenur; Florian Rieder; Johan Burisch; Joachim Høg Mortensen; Jakob Benedict Seidelin

doi:10.1093/ecco-jcc/jjaf085

Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study

Anja Poulsen^*
, Marta Sorokina Alexdóttir
, Lene Buhl Riis
, Pernille Dige Ovesen
, Julie Rasmussen
, Mads Damsgaard Wewer
, Viviane Lin
, Ronja M B Lagström
, Marwah Al-Sheikh
, Emilie Dahl
, Annedorte Ries
, Martin Pehrsson
, Thomai Tsapanou-Katranara
, Peter-Martin Krarup
, Ismail Gögenur
, Florian Rieder
, Johan Burisch
, Joachim Høg Mortensen
, Jakob Benedict Seidelin

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Artikel › Forskning › peer review

Abstract

BACKGROUND AND AIMS: Crohn's disease (CD) is characterized by progressive intestinal transmural damage, including fibrosis and strictures, which impair quality of life and require surgical intervention. No anti-stricture therapies are available, and no accurate biomarkers have been validated allowing prediction of strictures. Collagen fragments synthesis and remodeling show potential as markers of transmural disease activity. This study aimed to evaluate serum collagen markers for their accuracy in differentiating between stenosing and luminal CD and assessing their correlation with histopathology.

METHODS: Sixty-two patients undergoing resection for stricturing CD and 49 with luminal CD were prospectively included. ECM markers were quantified using ELISA, and histological assessments of fibrosis and inflammation were performed on full-thickness tissue samples. Clinical outcomes, biomarkers, and histology were analyzed over a 12-month follow-up.

RESULTS: ECM markers, including PRO-C6, PRO-C3, PRO-C5, C4M, and PRO-C4, distinguished stenosing from luminal CD with and the combination of PRO-C6, PRO-C3, and PRO-C5 achieved the highest discriminative power of (AUC 0.91). Significant changes in levels of the collagen biomarker were observed post-resection. Histological analysis revealed extensive intestinal fibrosis in the submucosa of the stenotic segments, which correlated with PRO-C6 levels. C4M and PRO-C4 positively correlated with neutrophils in lamina propria. CTX-III correlated negatively to the D'Haens score and neutrophils -and mononuclear cells in lamina propria and in epithelium.

CONCLUSION: Collagen markers distinguished stenosing from luminal CD, and they correlated to histological fibrosis and chronic inflammation promising for understanding ECM remodeling. This study highlights the need for extended follow-up to assess long-term stenosis-related outcomes.

Originalsprog	Engelsk
Artikelnummer	jjaf085
Antal sider	18
Tidsskrift	Journal of Crohn's and Colitis
Vol/bind	19
Udgave nummer	6
Tidlig onlinedato	20 maj 2025
DOI	https://doi.org/10.1093/ecco-jcc/jjaf085
Status	Udgivet - 4 jun. 2025

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Overlæge Poul Martin Christiansen og Hustrus Fond
Grosserer L. F. Foghts Fond

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10.1093/ecco-jcc/jjaf085Licens: CC BY

Citationsformater

Poulsen, A., Alexdóttir, M. S., Riis, L. B., Ovesen, P. D., Rasmussen, J., Wewer, M. D., Lin, V., Lagström, R. M. B., Al-Sheikh, M., Dahl, E., Ries, A., Pehrsson, M., Tsapanou-Katranara, T., Krarup, P.-M., Gögenur, I., Rieder, F., Burisch, J., Mortensen, J. H., & Seidelin, J. B. (2025). Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study. Journal of Crohn's and Colitis, 19(6), Artikel jjaf085. https://doi.org/10.1093/ecco-jcc/jjaf085

@article{ec8b9937395b4d929294c05a88e00b56,

title = "Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study",

abstract = "BACKGROUND AND AIMS: Crohn's disease (CD) is characterized by progressive intestinal transmural damage, including fibrosis and strictures, which impair quality of life and require surgical intervention. No anti-stricture therapies are available, and no accurate biomarkers have been validated allowing prediction of strictures. Collagen fragments synthesis and remodeling show potential as markers of transmural disease activity. This study aimed to evaluate serum collagen markers for their accuracy in differentiating between stenosing and luminal CD and assessing their correlation with histopathology.METHODS: Sixty-two patients undergoing resection for stricturing CD and 49 with luminal CD were prospectively included. ECM markers were quantified using ELISA, and histological assessments of fibrosis and inflammation were performed on full-thickness tissue samples. Clinical outcomes, biomarkers, and histology were analyzed over a 12-month follow-up.RESULTS: ECM markers, including PRO-C6, PRO-C3, PRO-C5, C4M, and PRO-C4, distinguished stenosing from luminal CD with and the combination of PRO-C6, PRO-C3, and PRO-C5 achieved the highest discriminative power of (AUC 0.91). Significant changes in levels of the collagen biomarker were observed post-resection. Histological analysis revealed extensive intestinal fibrosis in the submucosa of the stenotic segments, which correlated with PRO-C6 levels. C4M and PRO-C4 positively correlated with neutrophils in lamina propria. CTX-III correlated negatively to the D'Haens score and neutrophils -and mononuclear cells in lamina propria and in epithelium.CONCLUSION: Collagen markers distinguished stenosing from luminal CD, and they correlated to histological fibrosis and chronic inflammation promising for understanding ECM remodeling. This study highlights the need for extended follow-up to assess long-term stenosis-related outcomes.",

keywords = "Extracellular Matrix/metabolism, Diagnosis, Differential, Prospective Studies, Humans, Middle Aged, Intestines/pathology, Male, Fibrosis/blood, Young Adult, Collagen/blood, Crohn Disease/surgery, Biomarkers/blood, Female, Adult, Constriction, Pathologic/blood, Intestinal Obstruction/etiology, Longitudinal Studies, Crohn's disease, Collagen, Biomarkers",

author = "Anja Poulsen and Alexd{\'o}ttir, \{Marta Sorokina\} and Riis, \{Lene Buhl\} and Ovesen, \{Pernille Dige\} and Julie Rasmussen and Wewer, \{Mads Damsgaard\} and Viviane Lin and Lagstr{\"o}m, \{Ronja M B\} and Marwah Al-Sheikh and Emilie Dahl and Annedorte Ries and Martin Pehrsson and Thomai Tsapanou-Katranara and Peter-Martin Krarup and Ismail G{\"o}genur and Florian Rieder and Johan Burisch and Mortensen, \{Joachim H{\o}g\} and Seidelin, \{Jakob Benedict\}",

note = "{\textcopyright} The Author(s) 2025. Published by Oxford University Press on behalf of European Crohn{\textquoteright}s and Colitis Organisation.",

year = "2025",

month = jun,

day = "4",

doi = "10.1093/ecco-jcc/jjaf085",

language = "English",

volume = "19",

journal = "Journal of Crohn's and Colitis",

issn = "1873-9946",

publisher = "Oxford University Press",

number = "6",

}

Poulsen, A, Alexdóttir, MS, Riis, LB, Ovesen, PD, Rasmussen, J, Wewer, MD, Lin, V, Lagström, RMB, Al-Sheikh, M, Dahl, E, Ries, A, Pehrsson, M, Tsapanou-Katranara, T, Krarup, P-M, Gögenur, I, Rieder, F, Burisch, J, Mortensen, JH & Seidelin, JB 2025, 'Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study', Journal of Crohn's and Colitis, bind 19, nr. 6, jjaf085. https://doi.org/10.1093/ecco-jcc/jjaf085

Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study. / Poulsen, Anja; Alexdóttir, Marta Sorokina; Riis, Lene Buhl et al.
I: Journal of Crohn's and Colitis, Bind 19, Nr. 6, jjaf085, 04.06.2025.

Publikation: Bidrag til tidsskrift › Artikel › Forskning › peer review

TY - JOUR

T1 - Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients

T2 - A Pre- and Post-Resection Longitudinal Study

AU - Poulsen, Anja

AU - Alexdóttir, Marta Sorokina

AU - Riis, Lene Buhl

AU - Ovesen, Pernille Dige

AU - Rasmussen, Julie

AU - Wewer, Mads Damsgaard

AU - Lin, Viviane

AU - Lagström, Ronja M B

AU - Al-Sheikh, Marwah

AU - Dahl, Emilie

AU - Ries, Annedorte

AU - Pehrsson, Martin

AU - Tsapanou-Katranara, Thomai

AU - Krarup, Peter-Martin

AU - Gögenur, Ismail

AU - Rieder, Florian

AU - Burisch, Johan

AU - Mortensen, Joachim Høg

AU - Seidelin, Jakob Benedict

N1 - © The Author(s) 2025. Published by Oxford University Press on behalf of European Crohn’s and Colitis Organisation.

PY - 2025/6/4

Y1 - 2025/6/4

N2 - BACKGROUND AND AIMS: Crohn's disease (CD) is characterized by progressive intestinal transmural damage, including fibrosis and strictures, which impair quality of life and require surgical intervention. No anti-stricture therapies are available, and no accurate biomarkers have been validated allowing prediction of strictures. Collagen fragments synthesis and remodeling show potential as markers of transmural disease activity. This study aimed to evaluate serum collagen markers for their accuracy in differentiating between stenosing and luminal CD and assessing their correlation with histopathology.METHODS: Sixty-two patients undergoing resection for stricturing CD and 49 with luminal CD were prospectively included. ECM markers were quantified using ELISA, and histological assessments of fibrosis and inflammation were performed on full-thickness tissue samples. Clinical outcomes, biomarkers, and histology were analyzed over a 12-month follow-up.RESULTS: ECM markers, including PRO-C6, PRO-C3, PRO-C5, C4M, and PRO-C4, distinguished stenosing from luminal CD with and the combination of PRO-C6, PRO-C3, and PRO-C5 achieved the highest discriminative power of (AUC 0.91). Significant changes in levels of the collagen biomarker were observed post-resection. Histological analysis revealed extensive intestinal fibrosis in the submucosa of the stenotic segments, which correlated with PRO-C6 levels. C4M and PRO-C4 positively correlated with neutrophils in lamina propria. CTX-III correlated negatively to the D'Haens score and neutrophils -and mononuclear cells in lamina propria and in epithelium.CONCLUSION: Collagen markers distinguished stenosing from luminal CD, and they correlated to histological fibrosis and chronic inflammation promising for understanding ECM remodeling. This study highlights the need for extended follow-up to assess long-term stenosis-related outcomes.

AB - BACKGROUND AND AIMS: Crohn's disease (CD) is characterized by progressive intestinal transmural damage, including fibrosis and strictures, which impair quality of life and require surgical intervention. No anti-stricture therapies are available, and no accurate biomarkers have been validated allowing prediction of strictures. Collagen fragments synthesis and remodeling show potential as markers of transmural disease activity. This study aimed to evaluate serum collagen markers for their accuracy in differentiating between stenosing and luminal CD and assessing their correlation with histopathology.METHODS: Sixty-two patients undergoing resection for stricturing CD and 49 with luminal CD were prospectively included. ECM markers were quantified using ELISA, and histological assessments of fibrosis and inflammation were performed on full-thickness tissue samples. Clinical outcomes, biomarkers, and histology were analyzed over a 12-month follow-up.RESULTS: ECM markers, including PRO-C6, PRO-C3, PRO-C5, C4M, and PRO-C4, distinguished stenosing from luminal CD with and the combination of PRO-C6, PRO-C3, and PRO-C5 achieved the highest discriminative power of (AUC 0.91). Significant changes in levels of the collagen biomarker were observed post-resection. Histological analysis revealed extensive intestinal fibrosis in the submucosa of the stenotic segments, which correlated with PRO-C6 levels. C4M and PRO-C4 positively correlated with neutrophils in lamina propria. CTX-III correlated negatively to the D'Haens score and neutrophils -and mononuclear cells in lamina propria and in epithelium.CONCLUSION: Collagen markers distinguished stenosing from luminal CD, and they correlated to histological fibrosis and chronic inflammation promising for understanding ECM remodeling. This study highlights the need for extended follow-up to assess long-term stenosis-related outcomes.

KW - Extracellular Matrix/metabolism

KW - Diagnosis, Differential

KW - Prospective Studies

KW - Humans

KW - Middle Aged

KW - Intestines/pathology

KW - Male

KW - Fibrosis/blood

KW - Young Adult

KW - Collagen/blood

KW - Crohn Disease/surgery

KW - Biomarkers/blood

KW - Female

KW - Adult

KW - Constriction, Pathologic/blood

KW - Intestinal Obstruction/etiology

KW - Longitudinal Studies

KW - Crohn's disease

KW - Collagen

KW - Biomarkers

U2 - 10.1093/ecco-jcc/jjaf085

DO - 10.1093/ecco-jcc/jjaf085

M3 - Article

C2 - 40391838

SN - 1873-9946

VL - 19

JO - Journal of Crohn's and Colitis

JF - Journal of Crohn's and Colitis

IS - 6

M1 - jjaf085

ER -

Poulsen A, Alexdóttir MS, Riis LB, Ovesen PD, Rasmussen J, Wewer MD et al. Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study. Journal of Crohn's and Colitis. 2025 jun. 4;19(6):jjaf085. Epub 2025 maj 20. doi: 10.1093/ecco-jcc/jjaf085

Serum biomarkers of collagen remodeling are associated with intestinal fibrosis and differentiate stenotic from luminal Crohn's disease patients: A Pre- and Post-Resection Longitudinal Study

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