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J Biol Chem, Vol. 273, Issue 23, 14545-14549, June 5, 1998
Cholecystokinin Decreases Intestinal Hexose Absorption by a
Parallel Reduction in SGLT1 Abundance in the Brush-Border
Membrane
Andrew J.
Hirsh and
Christopher I.
Cheeseman
From the Membrane Transport Group, Department of Physiology,
University of Alberta, Edmonton, Alberta T6G 2H7, Canada
The dual lumenaly and vascularly perfused small
intestine was used to determine the mechanism by which cholecystokinin
octapeptide (CCK-8) decreases the rate of glucose absorption. With
CCK-8 in the vascular perfusate the rate of
3-O-methyl-D-glucose absorption decreased,
whereas the rate of D-fructose absorption was unaffected. The substrate pool size within the tissue during steady-state transport, in the presence and absence of CCK-8, was estimated by
compartmental analysis of the
3-O-methyl-D-glucose washout into the vascular
bed. When CCK-8 was included in the vascular perfusate, the absorptive
cell pool size decreased when compared with untreated tissue. Both the
steady-state hexose absorption data and the washout studies indicated
that the locus of action of CCK-8 was the SGLT1 transporter located in
the brush-border membrane. The SGLT1 protein abundance in isolated
brush-border membranes, as quantified by Western blotting, showed a
decrease that paralleled the decrease in the steady-state transport
rate induced by CCK-8. These results indicate that CCK-8 diminishes the
rate of intestinal hexose absorption by decreasing SGLT1 protein abundance in the brush-border membrane of the rat jejunum and therefore
provides evidence for acute enteric hormonal regulation of the rate of
glucose absorption across the small intestine.
Copyright © 1998 by The American Society for Biochemistry and Molecular Biology, Inc.

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Copyright © 1998 by the American Society for Biochemistry and Molecular Biology.
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