Asthma and other allergic diseases are caused by inappropriate immune  responses. Soluble IgE molecules, produced by immune cells known as B  cells, are key immune mediators of these diseases. Therapeutic targeting  of IgE in the blood can neutralize its effects and is an effective  treatment for moderate-to-severe allergic asthma. However, this approach  does not halt IgE production and patients need to be treated  repeatedly. 
But now, a team of researchers, at Genentech Inc., South San  Francisco, has developed a way to specifically eliminate IgE-producing B  cells, providing a potential new long-lasting therapeutic approach to  treating asthma and other allergic diseases.
IgE-producing B cells express on their surface an IgE molecule that  is slightly different to the IgE molecules that they secrete. The team,  led by Lawren Wu, generated a therapeutic molecule known as a monoclonal  antibody that targets the portion of human IgE that is contained in IgE  molecules on the surface of B cells but not in IgE molecules in the  blood. When mice expressing human IgE were treated with this monoclonal  antibody, their levels of IgE in the blood decreased substantially as  did their numbers of IgE-producing B cells.
As the monoclonal antibody provided mice with protection in a model  of allergic asthma, the authors suggest that targeting IgE-producing B  cells using monoclonal antibodies similar to those described in this  study might be of benefit to individuals with asthma and other allergic  diseases.
The research appears in the Journal of Clinical Investigation.

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