Placenta
Volume 28, Issue 5 , Pages 445-452, May 2007

l-Serine Uptake by Human Placental Microvillous Membrane Vesicles

  • R.M. Lewis

      Affiliations

    • Centre for Developmental Origins of Health and Disease, University of Southampton, Level F (MP887), Princess Anne Hospital, Coxford Road, Southampton SO16 5YA, UK
    • Corresponding Author InformationCorresponding author. Tel.: +44 23 8077 7222x8226; fax: +44 23 8078 6933.
  • ,
  • J. Glazier

      Affiliations

    • The Division of Human Development, The Medical School, University of Manchester, Manchester, UK
  • ,
  • S.L. Greenwood

      Affiliations

    • The Division of Human Development, The Medical School, University of Manchester, Manchester, UK
  • ,
  • E.J. Bennett

      Affiliations

    • Centre for Developmental Origins of Health and Disease, University of Southampton, Level F (MP887), Princess Anne Hospital, Coxford Road, Southampton SO16 5YA, UK
  • ,
  • K.M. Godfrey

      Affiliations

    • Centre for Developmental Origins of Health and Disease, University of Southampton, Level F (MP887), Princess Anne Hospital, Coxford Road, Southampton SO16 5YA, UK
  • ,
  • A.A. Jackson

      Affiliations

    • Institute of Human Nutrition, University of Southampton, Princess Anne Hospital, Coxford Road, Southampton SO16 5YA, UK
  • ,
  • C.P. Sibley

      Affiliations

    • The Division of Human Development, The Medical School, University of Manchester, Manchester, UK
  • ,
  • I.T. Cameron

      Affiliations

    • Centre for Developmental Origins of Health and Disease, University of Southampton, Level F (MP887), Princess Anne Hospital, Coxford Road, Southampton SO16 5YA, UK
  • ,
  • M.A. Hanson

      Affiliations

    • Centre for Developmental Origins of Health and Disease, University of Southampton, Level F (MP887), Princess Anne Hospital, Coxford Road, Southampton SO16 5YA, UK

Accepted 18 June 2006. published online 12 August 2006.

Abstract 

The human fetus requires more glycine than any other amino acid but placental glycine transfer to the fetus is insufficient to meet fetal demand. l-Serine could represent a major metabolic source of glycine for the human fetus but little is known about the kinetics and physiology of l-serine uptake by the human placenta. We have characterised the amino acid transport systems involved in the uptake of l-serine by the microvillous membrane of the human placental syncytiotrophoblast and compared the uptake rates to those of glycine.

l-Serine uptake into microvillous membrane (MVM) vesicles was primarily mediated by system A (MeAIB inhibitable) and system L (BCH inhibitable). Further characterisation using specific substrates of LAT1 and LAT2 found the pattern of l-serine uptake was consistent with that expected for uptake mediated by LAT2. Uptakes were performed with tracer levels of 14C-l-serine, physiological levels of l-serine, or with physiological levels of amino acids. As amino acid concentrations rose, the proportion of uptake by System L decreased while uptake by uncharacterised Na+-independent systems increased.

Uptake of l-serine into MVM vesicles had a Vmax of 2.1±0.4nmol/mg protein/min, which was significantly higher than for glycine (Vmax 1.0±0.2nmol/mg protein/min). This indicates that MVM vesicles have a higher uptake capacity for l-serine than glycine, despite a greater demand for glycine over serine for fetal protein synthesis. Further studies are now required to define the fate of l-serine taken up by the placenta and its importance for the fetus.

Keywords: Placenta, Serine, Glycine, Transport, Amino acid

Abbreviations: MVM, microvillous membrane, BM, basal membrane, SHMT, Serine hydroxymethyltransferase, MeAIB, α-methylamino-isobutyric acid, BCH, 2-norbornanecarboxylic acid

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PII: S0143-4004(06)00170-6

doi:10.1016/j.placenta.2006.06.014

Placenta
Volume 28, Issue 5 , Pages 445-452, May 2007