Frontier
Copyright ©The Author(s) 2021.
World J Gastroenterol. Nov 21, 2021; 27(43): 7402-7422
Published online Nov 21, 2021. doi: 10.3748/wjg.v27.i43.7402
Table 3 Biomarker applications of antimicrobial peptides in patients with inflammatory bowel disease
Ref.
Antimicrobial peptides
Type of IBD
Biomarker application
Key findings
Holgersen et al[110]Alpha defensins 5 and 6 (DEFA5/DEFA6)UCIBD diagnosis Marked upregulation of DEFA5 and DEFA6 in terminal ileal biopsies of inflamed ulcerative colitis relative to normal controls
Wehkamp et al[111]Alpha defensin (HD -5/6)UC/CDIBD diagnosis HD-5/6 both decreased in ileal Crohn's, and this correlated with a decrease in transcription factor Tcf-4, a known regulator of Paneth cell differentiation. Normal levels were observed in UC and colonic Crohn's
Yamaguchi et al[112]Alpha defensin (HNP1-3), beta-defensin (HBD-2)UC/CDDisease activityHNP-1-3 all elevated in IBD patients, while HBD-2 levels normal; serum HNP1-3 levels correlated with disease severity for Crohn's
Kanmura et al[113]Alpha defensin (HNP)UC/CDDisease activityFecal-HNP levels were markedly elevated in both UC and Crohn's, but slightly more so in Crohn's; F-HNP was significantly higher during flares of UC than remission. For UC, HNP levels correlated with Mayo endoscopic score
Cunliffe et al[114]Alpha defensin (HNP 1-3)UC/CDDisease activitySurface epithelial cells strongly immunoreactive for neutrophil defensins and lysozyme were seen in active ulcerative colitis and Crohn's disease (but not normal or inactive IBD) mucosal samples. Many of these cells coexpressed both antimicrobial proteins.
Tran et al[116]CathelicidinUC/CDDisease activityCathelicidin levels were significantly increased in IBD patients and were inversely correlated with CD activity. In moderate to severe IBD, higher cathelicidin levels before treatment correlated with better prognosis.
Krawiec et al[115]CathelicidinUC/CDIBD diagnosis Cathelicidin was significantly increased in patients with ulcerative colitis (1073.39 ± 214.52 ng/mL) and Crohn’s disease (1057.63 ± 176.03 ng/mL) patients compared to controls (890.56 ± 129.37 ng/mL) (P = 0.0003)
Gubatan et al[21]CathelicidinUCDisease activity, clinical relapseIn ulcerative colitis patients, serum 25(OH)D positively correlated with serum and colonic cathelicidin. Higher serum cathelicidin is associated with decreased risk of histologic inflammation and clinical relapse but not independent of 25(OH)D or baseline inflammation
Borkowska et al[118]LactoferrinUC/CDIBD diagnosis, disease activityFecal concentration of lactoferrin in children with IBD was significantly higher than in the controls. The sensitivity and specificity were 80.7% and 92.7%, respectively, and its positive and negative prognostic values were 96.8% and 63.3%, respectively
Sugi et al[119]Lactoferrin, lysozymeUC/CDDisease activityLactoferrin and lysozyme were significantly increased in the active phases of CD and UC relative to inactive. They both correlated with fecal Hb concentration in UC, and with alpha 1-AT concentration in CD
Sidhu et al[120]LactoferrinUC/CDIBD diagnosis, disease activityLactoferrin levels were significantly higher in IBD patients compared with IBS/healthy controls (P < 0.001). The sensitivity, specificity, positive and negative predictive values of lactoferrin in distinguishing active IBD from IBS/healthy controls were 67% and 96%, 87% and 86.8% respectively
Wang et al[121]LactoferrinUC/CDIBD diagnosisFL test has a high sensitivity (82%) and specificity (95%) for the discrimination of patients with IBD against non-IBD patients
Kane et al[122]LactoferrinUC/CDDisease activityFecal lactoferrin was 90% specific for identifying inflammation in patients with active IBD. Elevated fecal lactoferrin was 100% specific in ruling out IBS
Turner et al[123]LactoferrinUCIBD diagnosis Lactoferrin levels significantly were elevated in pediatric UC patients, but were not responsive to change or predictive of response to corticosteroids
Wang et al[132]ElafinCDDisease activity, intestinal stricturesHigh serum elafin levels were associated with a significantly elevated risk of intestinal stricture in CD patients. Serum elafin levels had weak positive correlations with clinical disease activity but not endoscopic disease activity
Zhang et al[133]ElafinUC/CDDisease activityThe expression of elafin mRNA in peripheral blood in active IBD patients is decreased, which may be correlated with the activity of IBD, and negatively correlated with corresponding disease activity score
Motta et al[130]ElafinUC Disease activityStudy identified a previously unrevealed production of elastase 2A (ELA2A) by colonic epithelial cells, which was enhanced in IBD patients. Study demonstrated that ELA2A hyperactivity is sufficient to lead to a leaky epithelial barrier and modified the cytokine gene expression profile with an increase of pro-inflammatory cytokine transcript
Schmid et al[134]Elafin and SLPIUC/CDDisease activity Levels of mRNA and immunostaining of the antiproteases elafin and SLPI were enhanced strongly in inflamed versus noninflamed UC
Frol'ová et al[124]Galectin-3UC/CDDisease activitySerum concentrations were significantly increased in specimen of patients with active and remission-stage ulcerative colitis and Crohn's disease (relative to healthy controls)
Yu et al[125]Galectin-1, -3UC/CDIBD diagnosis Serum level of galectin-1 and -3, but not galectins-2, -4, -7 and -8, were significantly higher in IBD patients than in healthy people. None of the galectins however were able to distinguish active disease from remission in UC or CD
Tibble et al[97]CalprotectinCDIBD diagnosisThe cross-sectional study showed a sensitivity of 96% for calprotectin in discriminating between normal subjects and those with Crohn's disease. With a cutoff point of 30 mg/L fecal calprotectin has 100% sensitivity and 97% specificity in discriminating between active CD and irritable bowel syndrome
Moniuszko et al[100]CalprotectinUC/CDDisease activity, progressionRapid bedside FC test reliably detected disease flares in patients with both UC and CD. FC levels increased even with early signs of inflammations; values were lower in isolated small bowel disease for CD patients
Pous-Serrano et al[101]CalprotectinCDDisease activityFC was the only inflammatory marker significantly associated with the degree of histologic inflammation in surgical specimens
Scheopfer et al[102]CalprotectinCDDisease activityFC correlates more closely with endoscopic disease activity that CRP, blood leukocytes, and CDAI. It was the only marker that reliably discriminated inactive from mild, moderate, and highly active disease, underscoring its value in disease monitoring
Ferreiro-Iglesias et al[103]CalprotectinUC/CDRelapseIn IBD patients under Infliximab maintenance therapy, high FC levels allow predicting relapse within the following 2 mo. Long-term remission is associated with low calprotectin levels
Klingberg et al[104]CalprotectinCDIBD diagnosis, treatment monitoringFC was a useful predictor of the development of CD in patients with ankylosing spondylitis; NSAIDs increase FC levels; FC levels drop following TNF-blocker treatments
Godny et al[109]CalprotectinCDTreatment monitoringFC decreases following successful diet-based treatment of active CD
Karaskova et al[126]HepcidinUC/CDIBD diagnosisSerum hepcidin concentration was significantly decreased in IBD children compared with controls; levels did not differ significantly between patients with CD and UC
Martinelli et al[128]HepcidinUC/CDIBD diagnosis, iron deficiency MonitoringSerum hepcidin was significantly higher in IBD patients with active disease versus healthy and celiac patients. Hepcidin levels corresponded with iron malabsorption and other inflammatory biomarkers like ESR
Aksan et al[129]HepcidinUC/CDResponse to iron supplementationHigher hepcidin and other inflammatory markers correlated with decreased iron absorption follow supplementation
Zollner et al[127]LipocalinCDClinical and endoscopic activity Fecal lipocalin-2 levels of 78.4 and 0.56 μg/g in Crohn’s disease patients for clinical and endoscopic activity, respectively, corresponded well with fecal calprotectin levels in UC patients (R = 0.87, P < 0.001)