Purpose: CD93 is receiving renewed attention as a biomarker of inflammation. We aimed to evaluate the potential for serum sCD93 to serve as a novel biomarker for allergic inflammation. Materials and Methods: We enrolled 348 subjects with an allergic disease [allergic rhinitis (AR), chronic spontaneous urticaria (CSU), or bronchial asthma (BA)], including 14 steroid-naive BA patients who were serially followed-up. Results: The serum sCD93 levels (ng/mL) in patients with exacerbated AR (mean +/- standard deviation, 153.1 +/- 58.4) were significantly higher than in patients without AR (132.2 +/- 49.0) or with stable AR (122.3 +/- 42.1). Serum sCD93 levels in exacerbated CSU (169.5 +/- 42.8) were also significantly higher than those in non-CSU (132.4 +/- 51.6) and stable CSU (122.8 +/- 36.2). This trend was also seen in BA. Serum levels in patients with ICS-naive BA (161.4 +/- 53.1) were significantly higher than those in healthy controls without BA (112.2 +/- 30.8), low-and medium-dose ICS users. Serum sCD93 levels in high-dose ICS users (72.2 +/- 20.6) were significantly lower than those in low-and medium-dose users. The serum sCD93 levels in steroid-naive patients with BA (195.1 +/- 72.7) decreased after ICS use for 4 weeks (134.4 +/- 42.8) and 8 weeks (100.7 +/- 13.4), serially. Conclusion: Elevated serum sCD93 levels reflected exacerbated status of allergic diseases, including CSU, AR, and asthma. ICS use significantly diminished serum sCD93 levels in steroid-naive patients with BA. This result may suggest sCD93 in serum as a therapeutic marker for allergic inflammation.
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Univ Notre Dame, Eck Inst Global Hlth, Dept Biol Sci, Notre Dame, IN USAUniv Notre Dame, Eck Inst Global Hlth, Dept Biol Sci, Notre Dame, IN USA
Greenlee, Mallary C.
Bohlson, Suzanne S.
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Univ Notre Dame, Eck Inst Global Hlth, Dept Biol Sci, Notre Dame, IN USA
Indiana Univ, Sch Med S Bend, Dept Microbiol & Immunol, South Bend, IN 46615 USAUniv Notre Dame, Eck Inst Global Hlth, Dept Biol Sci, Notre Dame, IN USA