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Vol. 54, Issue 6, 1073-1079, December 1998
Institut National de la Santé et de la Recherche
Médicale U425, Neuroimmunopharmacologie Pulmonaire, Faculté
de Pharmacie, 67401 Illkirch Cedex, France
Stem cell factor (SCF) is a major mast cell growth factor that promotes
differentiation and chemotaxis of mast cells and inhibits their
apoptosis. SCF therefore may be involved in diseases associated with an
increased number of tissue mast cells such as asthma, for which the
major treatment is glucocorticoids. In this study, we evaluated the
effect of the glucocorticoid budesonide on the constitutive expression
of SCF by human lung fibroblasts in primary culture. Budesonide (0.1 µM) induced a time-dependent biphasic effect on SCF mRNA
and protein production. A short treatment (2.5-10 hr) induced an
inhibition of SCF protein accumulation (
58% at 2.5 hr) and mRNA
expression (
69% at 2.5 hr), associated with an accelerated decay of
SCF mRNA and with a decrease in SCF gene transcription observed by
nuclear run-on assay. Longer treatment (24-72 hr) led to increases in
SCF protein accumulation (+64% at 48 hr) and mRNA expression (+125%
at 24 hr) as a consequence of transcriptional activation. Similar
effects of a decrease followed by an increase in SCF production were
observed using another glucocorticoid, dexamethasone. Overall, our
results show that glucocorticoids potently regulate SCF expression in
human lung fibroblasts, successively decreasing and increasing SCF mRNA
levels according to treatment duration. Such time-dependent modulation
of SCF levels may explain some current discrepant findings about the
effects of glucocorticoids on SCF production and may have functional
consequences during glucocorticoid treatment, such as asthma therapy.
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