Development of β-cell mass in fetuses of rats deprived of protein and/or energy in last trimester of pregnancy

Author:

Bertin Eric1,Gangnerau Marie-Noëlle1,Bellon Georges2,Bailbé Danièle1,Arbelot De Vacqueur Annick3,Portha Bernard1

Affiliation:

1. Laboratoire de Physiopathologie de la Nutrition, Centre National de la Recherche Scientifique-UMR 7059, Université Paris 7/D. DIDEROT, 75251 Paris Cedex 05;

2. Laboratoire de Biochimie, Hôpital Robert Debré, 51092 Reims Cedex; and

3. Centre de Recherche Merck-Lipha, 91385 Chilly-Mazarin Cedex, France

Abstract

Fetal malnutrition is now proposed as a risk factor of later obesity and type II diabetes. We previously analyzed the long-term impact of reduced protein and/or energy intake strictly limited to the last week of pregnancy in Wistar rats. Three protocols of gestational malnutrition were used: 1) low-protein isocaloric diet (5 instead of 15%) with pair feeding to the mothers receiving the control diet, 2) restricted diet (50% of control diet), and 3) low protein-restricted diet (50% of low-protein diet). Only isolated protein restriction induced a long-term β-cell mass decrease. In the present study, we used the same protocols of food restriction to analyze their short-term impact (on day 21.5 of pregnancy) on β-cell mass development. A 50% β-cell mass decrease was present in the three restricted groups, but low-protein diet, either associated or not to energy restriction, increased fetal β-cell insulin content. Among all the parameters analyzed to further explain our results, we found that the fetal plasma level of taurine was lowered by low-protein diet and was the main predictor of the fetal plasma insulin level ( r = 0.63, P < 0.01). In conclusion, rat fetuses exposed to protein and/or energy restriction during the third part of pregnancy have a similar dramatic decrease in β-cell mass, and their ability to recover β-cell mass development retardation depends on the type of malnutrition used. Moreover, our results support the hypothesis that taurine might play an important role in fetal β-cell mass function.

Publisher

American Physiological Society

Subject

Physiology (medical),Physiology

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