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1 inhibits surfactant component expression
and epithelial cell maturation in cultured human fetal lung
1 Pulmonary and Critical Care
Division,
Transforming growth factor-
1 (TGF-
1) is a
multifunctional cytokine shown to play a critical role in organ
morphogenesis, development, growth regulation, cellular
differentiation, gene expression, and tissue remodeling after injury.
We examined the effect of exogenously administered TGF-
1 on the
expression of surfactant proteins (SPs) and lipids, fatty acid
synthetase, and ultrastructural morphology in human fetal lung cultured
for 5 days with and without dexamethasone (10 nM). Expression of the type II cell-specific marker surfactant proprotein C (proSP-C), studied
by [35S]Met
incorporation and immunoprecipitation, increased sevenfold with
dexamethasone treatment. TGF-
1 (0.1-100 ng/ml) in the presence of dexamethasone inhibited 21-kDa proSP-C expression in a
dose-dependent manner (maximal inhibition 31% of control level at 100 ng/ml). There was no change in
[35S]Met incorporation
into total protein in any of the treatment groups vs. the control
group. In immunoblotting experiments, TGF-
1 blocked culture-induced
accumulation of SP-A and SP-B. Under the same conditions, TGF-
1
reduced mRNA content for SP-A, SP-B, and SP-C to 20, 38, and 41%,
respectively, of matched control groups but did not affect levels of
-actin mRNA. SP transcription rates after 24 h of exposure to
TGF-
1 were reduced to a similar extent (20-50% of control
level). In both control and dexamethasone-treated explants, TGF-
1
(10 ng/ml) also decreased fatty acid synthetase mRNA, protein, and
enzyme activity and the rate of
[3H]choline
incorporation into phosphatidylcholine. By electron microscopy,
well-differentiated type II cells lining potential air spaces were
present in explants cultured with dexamethasone, whereas exposure to
TGF-
1 with or without dexamethasone resulted in epithelial cells
lacking lamellar bodies. We conclude that exogenous TGF-
1 disrupts
culture-induced maturation of fetal lung epithelial cells and inhibits
expression of surfactant components through effects on gene
transcription.
transforming growth factor-
1; human fetal lung explants; surfactant proteins; fatty acid synthetase; dexamethasone
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