Abstract

Administration of N-carbamylglutamate (NCG), an analogue of endogenous N-acetyl-glutamate (an activator of arginine synthesis) has been shown to enhance neonatal growth by increasing circulating arginine levels. However, the effect of NCG on pregnancy remains unknown. This study examined the effects of NCG on pregnancy outcome and evaluated potential mechanisms involved. Reproductive performance, embryo implantation, and concentration of amino acids in serum and uterine flushing, were determined in rats fed control or NCG supplemented diets. Ishikawa cells and JAR cells were used to examine the mechanism by which NCG affects embryo implantation. Dietary NCG supplementation increased serum levels of arginine, onithine, and proline, as well as uterine levels of arginine, glutamine, glutamate, and proline. Additionally, it stimulated LIF expression, and enhanced the activation of signal transduction and activator of transcription 3 (Stat3), protein kinase B (PKB), and 70-kDa ribosomal protein S6 kinase (S6K1) during the periimplantation period, resulting in an increase in litter size but not birth weight. In uterine Ishikawa cells, LIF expression was also enhanced by treatment with arginine and its metabolites. In trophoblast JAR cells, treatment with arginine and its metabolites enhanced Stat3, PKB, and S6K1 activation and facilitated cellular adhesion activity. These effects were abolished by pretreatment with inhibitors of phosphatidylinositol 3-kinase (wortmannin) and mammalian target of rapamycin (rapamycin). The results demonstrate that NCG supplementation enhances pregnancy outcome and have important implications for the pregnancy outcome of mammalian species.

Highlights

  • With unprecedented changes in economic and social development as well as advanced maternal age, low fertility rate has become a global concern [1,2]

  • We reported that dietary NCG supplementation could increase the litter size and the concentration of arginine family of amino acids in serum and uterine flushings in rats

  • The results indicate that the increase in the arginine family of amino acids induced by dietary NCG supplementation enhanced uterine leukemia inhibitory factor antibody (LIF) expression

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Summary

Introduction

With unprecedented changes in economic and social development as well as advanced maternal age, low fertility rate has become a global concern [1,2]. Pregnancy loss is a common complication in human gestation [3] and reduced fertility in farm animals is of critical importance for efficient animal production [4]. Among the many factors that are involved in this process [8], leukemia inhibitory factor antibody (LIF) plays an essential role [9]. One of the initial events during embryo implantation is the adhesion of trophoblast cells to glycoproteins in the extracellular matrix of the uterine epithelium, such as fibronectin, vitronectin, and laminin [10]. LIF has been shown to promote extravillous trophoblast adhesion to fibronectin, vitronectin, and laminin during the first trimester in human pregnancy [11]. Stat is essential for embryo implantation, which can be activated by LIF [12]

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