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Journal of Lipid Research, Vol 38, 576-584, Copyright © 1997 by Lipid Research, Inc.
Glucosylceramide metabolism is regulated during normal and hormonally stimulated epidermal barrier development in the rat
K Hanley, Y Jiang, WM Holleran, PM Elias, ML Williams and KR Feingold
Department of Dermatology, University of California, San Francisco 94143, USA.
Glucosylceramides, delivered to the stratum corneum interstices by
exocytosis of lamellar body contents, are enzymatically hydrolyzed to
ceramides, which are major components of the lipid lamellar bilayers that
mediate epidermal barrier function. Because this conversion is critical for
permeability barrier homeostasis in the adult animal, in this study we
measured the changes in activities of the enzymes responsible for the
synthesis of glucosylceramide and its conversion to ceramide,
UDP-glucose:ceramide glucosyltransferase (GC synthase) and
beta-glucocerebrosidase (beta-GlcCer'ase), respectively, during fetal
barrier formation. In epidermis from rats of gestational age 17-21 days, GC
synthase activity peaked on day 19, prior to barrier competence, whereas
beta-GlcCer'ase activity rose throughout barrier formation, exhibiting a
5-fold increase over this time period. beta- GlcCer'ase protein rose in
parallel with activity, as did mRNA levels. Enzyme activities in skin
explants from 17-day fetal rats, incubated up to 4 days in hormone- and
serum-free media, paralleled those measured at corresponding time points in
utero. Incubation with hormones that accelerate barrier development had
minimal effects on GC synthase activity, whereas beta-GlcCer'ase activity
was significantly increased after 1 or 2 days in culture. Finally,
inhibition of beta-GlcCer'ase with conduritol B epoxide prevented barrier
development in vitro and was accompanied by abnormalities in the lamellar
bilayer ultrastructure of the stratum corneum. These data indicate that
both synthesis and hydrolysis of glucosylceramide are regulated during
fetal development. Furthermore, the enzymatic hydrolysis of
glucosylceramide to ceramide is essential for fetal barrier ontogenesis.

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Copyright © 1997 by the American Society for Biochemistry and Molecular Biology.
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