B-cell isotype control in atopy and asthma assessed with cDNA array technology

Author:

Brutsche Martin H.1,Brutsche Ingrid Carlen1,Wood Peter2,Mogulkoc Nesrin3,Custovic Adnan3,Egan Jim3,Woodcock Ashley3

Affiliation:

1. Pulmonology, University Hospital of Basel, CH-4031 Basel, Switzerland;

2. Department of Biological Sciences, University of Manchester, Manchester M13 9WL, United Kingdom

3. North West Lung Research Centre, South Manchester University Hospital Wythenshawe, Manchester M23 9LT; and

Abstract

B-cell isotype switching and the production of IgE is regulated by a variety of gene products through different mechanisms. A better understanding of these processes has the potential to identify markers of disease and new therapeutic targets. The aim of the study was to investigate human B-cell isotype control and IgE production in atopy and asthma with cDNA array technology. Eighteen atopic asthmatic, eight atopic nonasthmatic, and fourteen healthy control subjects were included. Peripheral blood mononuclear cells were separated by gradient centrifugation, mRNA was purified, and the reverse-transcribed probes were hybridized to cDNA membranes. Group differences were assessed with the Mann-Whitney U-test. Twenty-three of seventy-eight tested IgE-related genes had significantly altered expression in atopy and asthma compared with that in the healthy subjects. The differentially expressed genes include surface molecules involved in T- and B-cell interaction and activation, cytokines, intracellular signaling products, and transcription factors. In conclusion, both atopic nonasthmatic and atopic asthmatic individuals had activated proinflammatory pathways, a minimal requirement for B-cell isotype switching, and a clear net pro-IgE cytokine climate.

Publisher

American Physiological Society

Subject

Cell Biology,Physiology (medical),Pulmonary and Respiratory Medicine,Physiology

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