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1 Department of Medicine, University of Illinois at Chicago and Westside Veterans Affairs Medical Center, Chicago, Illinois 60612; and 2 University of California-Irvine, Veterans Affairs Medical Center, Long Beach, California 90822
Previous studies from our laboratory have
demonstrated the existence of a folate transporter in the human colonic
apical membranes. The current studies were undertaken to examine the
possible presence and function of a folate carrier in the human colonic
basolateral membrane vesicles (BLMV). BLMV were purified from mucosal
scrapings of colons of organ donors by a Percoll-density gradient
centrifugation technique, and uptake studies were performed using a
rapid filtration technique. Our results on [3H]Pte-Glu
uptake are summarized as follows: 1) uptake was sensitive to
osmolarity of the incubation medium; 2) Na+
removal from the incubation medium did not affect folate uptake into
BLMV; 3) uptake was significantly increased with decreasing incubation buffer pH from 8 to 4; 4) uptake demonstrated
saturation kinetics with an apparent Michaelis constant of 9.6 ± 0.48 µM and a maximal velocity of 8.10 ± 0.36 pmol · mg
protein
1 · 10 s
1; 5)
uptake was markedly inhibited by the structural analog methotrexate (inhibitory constant = 8.28 ± 1.0 µM); 6)
uptake into BLMV demonstrated a trans-stimulation
phenomenon; 7) anion exchange inhibitors DIDS and SITS
significantly inhibited folate uptake; and 8) uptake was
potential-insensitive, as voltage clamping of vesicles or making them
inside positive with K+/valinomycin failed to influence
folate uptake. Western blot analysis using purified human colonic
basolateral membrane preparations and specific polyclonal antibodies
against the human reduced folate carrier (hRFC) has shown expression of
the hRFC protein at this membrane domain. These data demonstrate the
existence of a pH-dependent, DIDS-sensitive, electroneutral,
carrier-mediated mechanism for folate transport across the human
colonic basolateral membranes.
human colon; colonic folate uptake; uptake mechanism; colonic membrane vesicles
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