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Indstillinger
Journal of Allergy and Clinical Immunology 2007-Feb

Basophil FcepsilonRI histamine release parallels expression of Src-homology 2-containing inositol phosphatases in chronic idiopathic urticaria.

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Becky M Vonakis
Kavitha Vasagar
Scott P Gibbons
Laura Gober
Patricia M Sterba
Hyeyoun Chang
Sarbjit S Saini
ARTIKEL: 17125820
DOI: 10.1016/j.jaci.2006.09.035
BioSeek: 17125820

Nøgleord

phosphatase

tyrosine

inositol

nældefeber

histamine

Abstrakt

BACKGROUND

Basophils are implicated in the pathogenesis of chronic idiopathic urticaria (CIU). Autoantibodies to the IgE receptor (FcepsilonRI) and serum histamine releasing activity have been detected in some subjects with CIU, although their role in vivo is unclear. Basophils of patients with CIU have altered FcepsilonRI-mediated histamine release (HR); however, the mechanism is unknown. In the basophil FcepsilonRI signaling pathway, protein levels of Src-homology 2-containing-5'-inositol phosphatase (SHIP)-1 are inversely correlated with the release of mediators or releasability. A related phosphatase, SHIP-2, is a negative regulator of monocyte IgG receptor (FcgammaR) signaling . We hypothesized that SHIP levels are altered in CIU basophils.

METHODS

Blood basophils were isolated from cold urticaria, CIU, or normal donors, and FcepsilonRI-dependent and independent HR were quantified. Protein levels of SHIP-1, SHIP-2, spleen tyrosine kinase, and phosphorylated Akt were determined by Western blotting. Subjects' serum was tested for serum histamine releasing activity and anti-FcepsilonRIalpha antibodies.

RESULTS

CIU basophils displayed a bimodal response to anti-IgE activation. One half of CIU subjects' basophils had reductions in anti-IgE-induced HR and were designated nonresponders (CIU NR). CIU NR basophil HR remained diminished at 10-fold to 30-fold higher doses of anti-IgE. CIU anti-IgE responder basophils had HR similar to normal subjects. SHIP-1 and SHIP-2 proteins were increased in CIU NR basophils and were linked to reduced phosphoAkt after anti-IgE stimulation. CIU basophil anti-IgE response was not related to the presence of serologic factors.

CONCLUSIONS

In CIU basophils, the observed changes in FcepsilonRI signaling pathway molecule expression may underlie changes in releasability.

CONCLUSIONS

Patients with CIU can be segregated on the basis of basophil functional phenotype.

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