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Cultured Human Fibroblasts Express Constitutive IL-16 mRNA: Cytokine Induction of Active IL-16 Protein Synthesis Through a Caspase-3-Dependent Mechanism¹

Daniela Sciaky^*, William Brazer, David M. Center, William W. Cruikshank and Terry J. Smith^2,*,

^* Division of Molecular and Cellular Medicine, Department of Medicine, and Department of Biochemistry and Molecular Biology, Albany Medical College, and the Samuel S. Stratton Veterans Administration Medical Center, Albany, NY 12208; and Pulmonary Center, Boston University School of Medicine, Boston, MA 02118

Human fibroblasts can express numerous regulatory molecules that influence immune function. IL-16, a ligand for CD4, is a chemoattractant molecule expressed by lymphocytes, eosinophils, mast cells, and lung epithelium. It appears that the sole target for IL-16 is the CD4-bearing cell. Here we demonstrate that fibroblasts from several tissues can express IL-16 mRNA and protein as well as IL-16-dependent chemoattractant activity. The transcript is expressed abundantly under basal culture conditions as a 2.5-kb band on Northern analysis, similar to that observed in lymphocytes. IL-16 protein and activity are undetectable in fibroblast cultures under these same control conditions. However, when treated with proinflammatory cytokines such as IL-1ß, they express very high levels of IL-16 protein and chemoattractant activity, a substantial component of which can be blocked with IL-16-neutralizing Abs. The amount of IL-16 protein released into the medium is 3- to 4-fold greater, on a per cell basis, than that observed in lymphocytes. The induction of IL-16 protein by IL-1ß can be attenuated with specific inhibition of caspase-3, which could be detected in IL-1ß-treated fibroblasts. IL-1ß also induces RANTES mRNA, protein, and activity, and most of the chemoattractant activity released from fibroblasts not derived from IL-16 can be attributed to RANTES. Human fibroblasts appear to be an important source of IL-16 and through expression of this molecule may have key roles in the recruitment of CD4⁺ cells to sites of inflammation. IL-16 expression and the mechanism involved in its regulation appear to be cell type specific.

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