Abstract

The major milestones in mouse placental development are well described, but our understanding is limited to how the placenta can adapt to damage or changes in the environment. By using stereology and expression of cell cycle markers, we found that the placenta grows under normal conditions not just by hyperplasia of trophoblast cells but also through extensive polyploidy and cell hypertrophy. In response to feeding a low protein diet to mothers prior to and during pregnancy, to mimic chronic malnutrition, we found that this normal program was altered and that it was influenced by the sex of the conceptus. Male fetuses showed intrauterine growth restriction (IUGR) by embryonic day (E) 18.5, just before term, whereas female fetuses showed IUGR as early as E16.5. This difference was correlated with differences in the size of the labyrinth layer of the placenta, the site of nutrient and gas exchange. Functional changes were implied based on up-regulation of nutrient transporter genes. The junctional zone was also affected, with a reduction in both glycogen trophoblast and spongiotrophoblast cells. These changes were associated with increased expression of Phlda2 and reduced expression of Egfr. Polyploidy, which results from endoreduplication, is a normal feature of trophoblast giant cells (TGC) but also spongiotrophoblast cells. Ploidy was increased in sinusoidal-TGCs and spongiotrophoblast cells, but not parietal-TGCs, in low protein placentas. These results indicate that the placenta undergoes a range of changes in development and function in response to poor maternal diet, many of which we interpret are aimed at mitigating the impacts on fetal and maternal health.

Highlights

  • The placenta is a complex organ that integrates the fetal demand for nutrients with maternal nutrient availability [1], while protecting the health of the mother [2]

  • The number of cells in the chorionic plate decreased by ~4-fold, but this was balanced by the appearance of trophoblast cells in the labyrinth layer as the chorion trophoblast cells differentiate

  • We calculated the trophoblast cellular volume and found that it increased by ~5-fold between E12.5 and E18.5 (Fig 1D). These results indicated that the increase in the volume of the trophoblast cell compartment in the labyrinth after E12.5 was driven by trophoblast cell hypertrophy rather than an increase in trophoblast cell number

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Summary

Objectives

The objectives of our current study were first to describe the patterns of cell proliferation and endoreduplication during the time course of normal gestation and to see how these normal patterns of development and function are affected by a chronic low protein maternal diet

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