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      Regulation of mast-cell and basophil function and survival by IgE.

      Nature reviews. Immunology
      Animals, Basophils, cytology, drug effects, immunology, Cell Adhesion Molecules, Cell Survival, Cytokines, metabolism, Feedback, Humans, Immunoglobulin E, pharmacology, Mast Cells, Mice, Models, Immunological, Receptors, IgE, chemistry, Signal Transduction

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          Abstract

          Mast cells and basophils are important effector cells in T helper 2 (T(H)2)-cell-dependent, immunoglobulin-E-associated allergic disorders and immune responses to parasites. The crosslinking of IgE that is bound to the high-affinity receptor Fc epsilon RI with multivalent antigen results in the aggregation of Fc epsilon RI and the secretion of products that can have effector, immunoregulatory or autocrine effects. This response can be enhanced markedly in cells that have been exposed to high levels of IgE, which results in the increased surface expression of Fc epsilon RI. Moreover, recent work indicates that monomeric IgE (in the absence of crosslinking) can render mast cells resistant to apoptosis induced by growth-factor deprivation in vitro and, under certain circumstances, can induce the release of cytokines. So, the binding of IgE to Fc epsilon RI might influence mast-cell and basophil survival directly or indirectly, and can also regulate cellular function.

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