Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Enzyme
Compound
Query: UMLS:C0022104 (
irritable bowel syndrome
)
8,033
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Traditionally,
IBD
diagnosis is based on clinical, radiological, endoscopic, and histological criteria. Biomarkers are needed in cases of uncertain diagnosis, or to predict disease course and therapeutic response. No guideline recommends the detection of antibodies (including ASCA and ANCA) for diagnosis or prognosis of
IBD
to date. However, many recent data suggest the potential role of new serological markers (anti-glycan (ACCA, ALCA, AMCA, anti-L and anti-C), anti-
GP2
and anti-GM-CSF Ab). This review focuses on clinical utility of these new serological markers in diagnosis, prognosis and therapeutic monitoring of
IBD
. Literature review of anti-glycan, anti-
GP2
and anti-GM-CSF Ab and their impact on diagnosis, prognosis and prediction of therapeutic response was performed in PubMed/MEDLINE up to June 2014. Anti-glycan, anti-
GP2
and anti-GM-CSF Ab are especially associated with CD and seem to be correlated with complicated disease phenotypes even if results differ between studies. Although anti-glycan Ab and anti-
GP2
Ab have low sensitivity in diagnosis of
IBD
, they could identify a small number of CD patients not detected by other tests such as ASCA. Anti-glycan Abs are associated with a progression to a more severe disease course and a higher risk for
IBD
-related surgery. Anti-
GP2
Ab could particularly contribute to better stratify cases of pouchitis. Anti-GM-CSF Ab seems to be correlated with disease activity and could help predict relapses. These new promising biomarkers could particularly be useful in stratification of patients according to disease phenotype and risk of complications. They could be a valuable aid in prediction of disease course and therapeutic response but more prospective studies are needed.
...
PMID:Systematic review: new serological markers (anti-glycan, anti-GP2, anti-GM-CSF Ab) in the prediction of IBD patient outcomes. 2546 78
The need for reliable biomarkers for distinguishing Crohn disease (CD) from ulcerative colitis (UC) is increasing. This study aimed at evaluating the diagnostic potential of anti-
GP2
antibodies as a biomarker in Chinese patients with CD. In addition, a variety of autoantibodies, including anti-saccharomyces cerevisiae antibodies (ASCA), perinuclear anti-neutrophil cytoplasmic antibodies (PANCA), anti-intestinal goblet cell autoantibodies (GAB), and anti-pancreatic autoantibodies (PAB), were evaluated.A total of 91 subjects were prospectively enrolled in this study, including 35 patients with CD, 35 patients with UC, 13 patients with non-
IBD
gastrointestinal diseases as disease controls (non-
IBD
DC), and 8 healthy controls (HC). The diagnosis of
IBD
was determined based on the Lennard-Jones criteria, and the clinical phenotypes of the
IBD
patients were determined based on the Montreal Classification.Anti-
GP2
IgG antibodies were significantly elevated in patients with CD, compared with patients with UC (P = 0.0038), HC (P = 0.0055), and non-
IBD
DC (P = 0.0063). The prevalence of anti-
GP2
IgG, anti-
GP2
IgA and anti-
GP2
IgA, or IgG antibodies in patients with CD was 40.0%, 37.1%, and 54.3%, respectively, which were higher than those in non-
IBD
DC (anti-
GP2
IgG, 15.4%; anti-
GP2
IgA, 7.7%; and anti-
GP2
IgA or IgG, 23.1%) and those in patients with UC (anti-
GP2
IgG, 11.4%; anti-
GP2
IgA, 2.9%; and anti-
GP2
IgA or IgG, 14.3%). For distinguishing CD from UC, the sensitivity, specificity, positive predictive value (PPV) and positive likelihood ratios (LR+) were 40%, 88.6%, 77.8%, and 3.51 for anti-
GP2
IgG, 37.1%, 97.1%, 92.9%, and 13.0 for anti-
GP2
IgA, and 54.3%, 85.3%, 79.2%, and 3.69 for anti-
GP2
IgA or IgG. For CD diagnosis, the combination of anti-
GP2
antibodies with ASCA IgA increased the sensitivity to 68.6% with moderate loss of specificity to 74.3%. Spearman's rank of order revealed a significantly positive correlation of anti-
GP2
IgG with ileocolonic location of disease (L3) (P = 0.043) and a negative correlation of anti-
GP2
IgA with biologic therapy (P = 0.012).Our findings suggest that anti-
GP2
antibodies could serve as a biomarker for distinguishing patients with CD from patients with UC, and the combination of anti-
GP2
antibodies with ASCA IgA may improve the predictive power.
...
PMID:Diagnostic Potential of Zymogen Granule Glycoprotein 2 Antibodies as Serologic Biomarkers in Chinese Patients With Crohn Disease. 3126 10
