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Serum Oncostatin M in Ulcerative Colitis Patients and Its Relation to Disease Activity
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Ulcerative colitis (UC) is a chronic, relapsing inflammatory bowel disease; non-invasive biomarkers that accurately reflect the endoscopic and histological activity of UC require validation. Therefore, our study focused on exploring the potential of serum oncostatin M (OSM) as a biomarker for evaluating UC severity. A total of UC 89 eligible participants (≥18 years) underwent extensive clinical and paraclinical evaluation. Clinical, endoscopic, and histological activity were assessed using the partial Mayo score (pMS), the Mayo endoscopic score (MES), and the Nancy Histological Index (NHI), respectively. Serum OSM levels were determined by ELISA test and measured in pg/mL; fecal calprotectin (FC) was measured in µ/g. In our study, serum OSM was significantly associated with all four outcome measures: higher OSM levels predicted higher pMS (β = 0.471, p < 0.001, R2 = 0.222), MES (β = 0.422, p < 0.001, R2 = 0.178), NHI (β = 0.422, p < 0.001, R2 = 0.256), and FC (β = 0.431, p < 0.001, R2 = 0.186). Furthermore, ROC curve analyses demonstrated that OSM had excellent diagnostic accuracy for active disease, particularly in relation to histological inflammation (AUC = 0.967). In comparison, FC showed good but slightly lower accuracy (AUC = 0.875). Notably, OSM also outperformed FC in discriminating histological remission. Pairwise ROC curve analyses using DeLong’s test further confirmed the diagnostic accuracy of OSM, FC, and combined biomarker scores (OSM+FC) across clinical, endoscopic, and histological endpoints. The combined score PRE1 (OSM + FC based on NHI) achieved perfect discrimination (AUC = 1.000, p < 0.001). Composite models PRE2 and PRE3 (OSM+FC based on MES and pMS) improved diagnostic accuracy relative to OSM, confirming the value of combining OSM with FC. Although both outperformed OSM (p < 0.05), neither achieved a superior advantage over FC. Serum OSM is strongly associated with histological activity in UC and demonstrates superior performance compared with FC in assessing histological remission.
MDPI AG
Alina-Ecaterina Jucan
Georgiana-Elena Sarbu
Vasile-Claudiu Mihai
Carmen Atodiresei
Simona Juncu
Ioana-Ruxandra Mihai
Mariana Pavel-Tanasa
Daniela Constantinescu
Mihaela Dranga
Otilia Nedelciuc
Diana-Gabriela Iosep
Mihai Danciu
Smaranda Diaconescu
Georgiana-Emmanuela Gîlca-Blanariu
Andrei Mihai Andronic
Elena Toader
Vasile-Liviu Drug
Cristina Cijevschi Prelipcean
Catalina Mihai
Title: Serum Oncostatin M in Ulcerative Colitis Patients and Its Relation to Disease Activity
Description:
Ulcerative colitis (UC) is a chronic, relapsing inflammatory bowel disease; non-invasive biomarkers that accurately reflect the endoscopic and histological activity of UC require validation.
Therefore, our study focused on exploring the potential of serum oncostatin M (OSM) as a biomarker for evaluating UC severity.
A total of UC 89 eligible participants (≥18 years) underwent extensive clinical and paraclinical evaluation.
Clinical, endoscopic, and histological activity were assessed using the partial Mayo score (pMS), the Mayo endoscopic score (MES), and the Nancy Histological Index (NHI), respectively.
Serum OSM levels were determined by ELISA test and measured in pg/mL; fecal calprotectin (FC) was measured in µ/g.
In our study, serum OSM was significantly associated with all four outcome measures: higher OSM levels predicted higher pMS (β = 0.
471, p < 0.
001, R2 = 0.
222), MES (β = 0.
422, p < 0.
001, R2 = 0.
178), NHI (β = 0.
422, p < 0.
001, R2 = 0.
256), and FC (β = 0.
431, p < 0.
001, R2 = 0.
186).
Furthermore, ROC curve analyses demonstrated that OSM had excellent diagnostic accuracy for active disease, particularly in relation to histological inflammation (AUC = 0.
967).
In comparison, FC showed good but slightly lower accuracy (AUC = 0.
875).
Notably, OSM also outperformed FC in discriminating histological remission.
Pairwise ROC curve analyses using DeLong’s test further confirmed the diagnostic accuracy of OSM, FC, and combined biomarker scores (OSM+FC) across clinical, endoscopic, and histological endpoints.
The combined score PRE1 (OSM + FC based on NHI) achieved perfect discrimination (AUC = 1.
000, p < 0.
001).
Composite models PRE2 and PRE3 (OSM+FC based on MES and pMS) improved diagnostic accuracy relative to OSM, confirming the value of combining OSM with FC.
Although both outperformed OSM (p < 0.
05), neither achieved a superior advantage over FC.
Serum OSM is strongly associated with histological activity in UC and demonstrates superior performance compared with FC in assessing histological remission.
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