Abstract
Abstract In contrast to the general model of cytokine-induced
JAK/STAT signaling, tyrosine phosphorylation of the IL-5R ß
chain seems to be dispensable for STAT activation in cells
overexpressing exogenous STAT proteins. In this study we
expressed IL-5 receptor mutants in 293 cells and studied IL-5-
induced endogenous STAT-dependent transcription. Our results
indicate that: (a) tyrosine phosphorylation
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