LAT1-dependent placental methionine uptake is a key player in fetal programming of metabolic disease.

Schröder, Mariana; Fuenzalida, Barbara; Yi, Nan; Shahnawaz, Saira; Gertsch, Jürg; Pellegata, Daniele; Ontsouka, Edgar; Leiva, Andrea; Gutiérrez, Jaime; Müller, Martin; Brocco, Marcela A; Albrecht, Christiane (2024). LAT1-dependent placental methionine uptake is a key player in fetal programming of metabolic disease. Metabolism : clinical and experimental, 153, p. 155793. Elsevier 10.1016/j.metabol.2024.155793

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The Developmental Origins of Health and Disease hypothesis sustains that exposure to different stressors during prenatal development prepares the offspring for the challenges to be encountered after birth. We studied the gestational period as a particularly vulnerable window where different stressors can have strong implications for fetal programming of the offspring's life-long metabolic status via alterations of specific placentally expressed nutrient transporters. To study this mechanism, we used a murine prenatal stress model, human preeclampsia, early miscarriage, and healthy placental tissue samples, in addition to in vitro models of placental cells. In stressed mice, placental overexpression of L-type amino acid transporter 1 (Lat1) and subsequent global placental DNA hypermethylation was accompanied by fetal and adult hypothalamic dysregulation in global DNA methylation and gene expression as well as long-term metabolic abnormalities exclusively in female offspring. In human preeclampsia, early miscarriage, and under hypoxic conditions, placental LAT1 was significantly upregulated, leading to increased methionine uptake and global DNA hypermethylation. Remarkably, subgroups of healthy term placentas with high expression of stress-related genes present increased levels of placental LAT1 mRNA and protein, DNA and RNA hypermethylation, increased methionine uptake capacity, one-carbon metabolic pathway disruption, higher methionine concentration in the placenta and transport to the fetus specifically in girls. Since LAT1 mediates the intracellular accumulation of methionine, global DNA methylation, and one-carbon metabolism in the placenta, our findings hint at a major sex-specific global response to a variety of prenatal stressors affecting placental function, epigenetic programming, and life-long metabolic disease and provide a much-needed insight into early-life factors predisposing females/women to metabolic disorders.

Item Type:	Journal Article (Original Article)
Division/Institute:	04 Faculty of Medicine > Pre-clinic Human Medicine > Institute of Biochemistry and Molecular Medicine
UniBE Contributor:	Schröder, Mariana, Fuenzalida Saavedra, Barbara Marlene, Yi, Nan, Pellegata, Daniele, Ontsouka, Corneille Edgar, Albrecht, Christiane
Subjects:	500 Science > 570 Life sciences; biology 600 Technology > 610 Medicine & health
ISSN:	1532-8600
Publisher:	Elsevier
Language:	English
Submitter:	Pubmed Import
Date Deposited:	01 Feb 2024 15:30
Last Modified:	04 Mar 2024 00:15
Publisher DOI:	10.1016/j.metabol.2024.155793
PubMed ID:	38295946
Uncontrolled Keywords:	Environmental stress Fetal programming Metabolic disease Miscarriage Placenta Preeclampsia Sex differences
BORIS DOI:	10.48350/192325
URI:	https://boris.unibe.ch/id/eprint/192325

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