Am. J. Respir. Cell Mol. Biol., Vol 11, No. 3, 09 1994, 251-261.
Ontogeny and regulation of platelet-derived growth factor gene expression in distal fetal rat lung epithelial cells
S Buch, D Jassal, I Cannigia, J Edelson, R Han, J Liu, K Tanswell and M Post
MRC Group in Lung Development, Hospital for Sick Children Research Institute, Toronto, Ontario, Canada.
Using flow cytometry, thymidine uptake into DNA, and expression of two
growth-related genes, histone 3 and c-myc, we found an increase in the
proportion of distal lung epithelial cells in the G0/G1 phase of the cell
cycle with advancing gestation. Since our previous studies had demonstrated
that platelet-derived growth factor (PDGF) is essential for the progression
of these cells from the G0/G1 to the S phase of cell cycle, we investigated
the gene and protein expression of PDGF- related genes (PDGF-A, PDGF-B,
alpha-receptor, and beta-receptor) in distal fetal lung epithelial cells.
The cells transcribed all the PDGF- related genes and translated the PDGF-A
and PDGF-B mRNAs into protein, as demonstrated by immunocytochemistry and
immunoprecipitation. To explore an autocrine role for PDGF in distal fetal
lung epithelial cells, intervention studies using PDGF-A and -B
chain-specific antisense oligodeoxynucleotides (ODN) were carried out.
Antisense PDGF- B ODN, but not antisense PDGF-A ODN, significantly reduced
the DNA synthesis of these cells. The inhibitory effect of antisense PDGF-B
ODN on DNA synthesis was reversed by the addition of exogenous PDGF-BB,
which supports an autocrine role in the DNA synthesis of these cells. We
also examined the expression of PDGF genes in distal fetal lung epithelial
cells during late gestation. PDGF-A chain and beta-receptor gene
expressions declined with advancing gestation, whereas expression of
message for PDGF-B chain and alpha-receptor increased. The increases in
message for PDGF-B chain and alpha-receptor with advancing gestation were
due to a greater rate of transcription, whereas the developmental decrease
of PDGF-A chain and beta-receptor mRNAs was caused by a decrease in RNA
stability. Taken together with the ODN data, these results suggest that the
G0/G1 cell cycle arrest of distal lung epithelial cells during late fetal
gestation is due to a decrease in PDGF beta-receptor expression by the
cells.
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Copyright © 1994 American Thoracic Society.
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