IL-9 Stimulates Release of Chemotactic Factors from Human Bronchial Epithelial Cells

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IL-9 Stimulates Release of Chemotactic Factors from Human Bronchial Epithelial Cells

Frédéric F. Little, William W. Cruikshank, and David M. Center

The Pulmonary Center, Boston University School of Medicine, Boston, Massachusetts

Interleukin (IL)-9 is a T helper 2 cytokine implicated as a candidate gene and contributor to human asthma. We hypothesizedthat the inflammatory potential of bronchial epithelium is affectedby its local environment and explored this hypothesis with respectto the effect of IL-9 on bronchial epithelium. We investigatedthe response of primary and immortalized human bronchial epithelialcells to IL-9 stimulation with respect to the release of T-cellchemoattractant factors. In response to IL-9, the HBE4-E6/E7 cellline, but not BEAS-2B cells, released the T-cell chemoattractantsIL-16 and regulated on activation, normal T cells expressed andsecreted (RANTES) in a dose-dependent fashion. We found a similardose response to IL-9 in primary cells from bronchial brushingsof healthy subjects and that nearly all of the T-cell chemoattractionwas attributable to IL-16 and RANTES. Reverse transcriptase/polymerasechain reaction of BEAS-2B, HBE4-E6/E7, and primary cells fromtwo subjects revealed messenger RNA for IL-9 receptor (IL-9R) $alpha$ but not in BEAS-2B cells. Fluorescence-activated cell sorteranalysis of HBE4-E6/E7 and primary cells confirmed surface expressionof the IL-9 receptor. Costimulation of both cell types with IL-9and antibody to either $gamma$ -common chain or IL-9R $alpha$ completely blockedthe release of T-cell chemoattractant activity, confirming theprimary role of a functioning IL-9 receptor for IL-9 signalingin HBE4-E6/E7 and primary bronchial epithelial cells. We concludethat IL-9 is a stimulus for airway epithelial cell release ofT-cell chemoattractant factors, which in turn may modulate theimmune response in allergic airwayinflammation.

Abbreviations: bronchial hyperresponsiveness, BHR; bovine serum albumin, BSA; complementary DNA, cDNA; ethylenediaminetetraaceticacid, EDTA; fluorescein-activated cell scanner, FACS; gamma-commonchain, $gamma$ -c; enzyme-linked immunosorbent assay, ELISA; immunoglobulin,Ig; interleukin, IL; interleukin-9 receptor, IL-9R; messengerRNA, mRNA; phosphate-buffered saline, PBS; polymerase chain reaction,PCR; phycoerythrin, PE; regulated on activation, normal T cellsexpressed and secreted, RANTES; reverse transcriptase/polymerasechain reaction, RT-PCR; standard error of the mean, SEM; T helper,Th.

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