Inhibition of TGF-β3 restores the invasive capability of extravillous trophoblasts in preeclamptic pregnancies
Isabella Caniggia, … , Martin Post, Stephen J. Lye
Isabella Caniggia, … , Martin Post, Stephen J. Lye
Published June 15, 1999
Citation Information: J Clin Invest. 1999;103(12):1641-1650. https://doi.org/10.1172/JCI6380.
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Article

Inhibition of TGF-β3 restores the invasive capability of extravillous trophoblasts in preeclamptic pregnancies

Abstract

Preeclampsia, the major cause of maternal morbidity and mortality in developed countries, is associated with abnormalities of placenta function due to shallow invasion of the maternal decidua by trophoblasts. Data suggest that TGF-β may play a role in inhibiting trophoblast outgrowth or invasion, or both. We report that placental TGF-β3 expression is high in early pregnancy but falls at around 9 weeks’ gestation. This pattern is inversely correlated with trophoblast outgrowth and fibronectin synthesis, markers of early trophoblast differentiation toward an invasive phenotype. We demonstrate that TGF-β3 is overexpressed in preeclamptic placentae. In contrast to control placentae, explants from preeclamptic pregnancies fail to exhibit spontaneous invasion in vitro. Significantly, antisense-induced inhibition of TGF-β3 expression, and inhibition of TGF-β3 activity with antibodies, induces the formation of columns of trophoblast cells, which migrate out of the explant into the underlying Matrigel. To our knowledge, this is the first demonstration that the hypoinvasive placental phenotype characteristic of preeclampsia can be essentially normalized in vitro by biochemical manipulation. We speculate that a failure to downregulate expression of TGF-β3 at around 9 weeks’ gestation results in shallow trophoblast invasion and predisposes the pregnancy to preeclampsia.

Authors

Isabella Caniggia, Sorina Grisaru-Gravnosky, Maciej Kuliszewsky, Martin Post, Stephen J. Lye

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Immunoperoxidase staining of TGF-β1, TGF-β2, and TGF-β3 was performed in...
Immunoperoxidase staining of TGF-β1, TGF-β2, and TGF-β3 was performed in placental sections from normal pregnancies and pregnancies complicated by preeclampsia. Sections of both normal and preeclamptic placental tissue of 29 weeks’ gestation show low/absent TGF-β1 immunoreactivity in cells of the chorionic villi. Sections of both normal and preeclamptic placental tissue of 32 weeks’ gestation show positive TGF-β2 immunoreactivity in the syncytium of the chorionic villi (ST, arrow). Sections of normal placental tissue of 31 weeks’ gestation show low/absent TGF-β3 immunoreactivity in cells of the chorionic villi. Sections of preeclamptic placental tissue of the same gestation show strong TGF-β3 immunoreactivity viewed by brown staining in the syncytiotrophoblast (ST, arrow) and in stromal cells (S) of the chorionic villi. Control experiments were performed using antiserum preabsorbed with an excess of peptide. ×100. Immunostaining for TGF-β1, TGF-β2 , and TGF-β3 was repeated in 5 different preeclamptic and age-matched control placentae ranging from 27 to 34 weeks’ gestation.