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Vol. 286, Issue 1, 157-162, July 1998
Physiologisches Institut, Universität Würzburg (A.D.,
S.S., M.G.), D-97070 Würzburg, Germany and
Department of
Physiology, College of Medicine, University of Arizona (W.H.D.),
Tucson, Arizona
Ochratoxin A (OTA) is a widespread nephrotoxin excreted to a
substantial degree via the kidney. Previously we showed
that [3H]OTA can be reabsorbed along the rat nephron
in vivo (). In this
study we investigated in detail the contribution of different nephron
segments to [3H]OTA reabsorption and determined the
possible mechanisms involved by microinfusion and microperfusion
experiments. At pH 6 (~94% of OTA neutral), OTA is reabsorbed in all
nephron segments investigated. The estimated fractional reabsorptions
(FR) at a tubular load of 20 fmol/min are: proximal convoluted tubule
(PCT), 14.8%; proximal straight tubule (PST), 27.4%; ascending limb
of Henle's loop (ALH), 13.6%; distal tubule (DT), 11.6%; collecting
duct (CD), 24.6%; terminal CD, 22.0%. At pH 8 (~10% of OTA
neutral) FR are as follows: PCT, 0%; PST, 25.9%; ALH, 14.0%; DT,
3.2%; CD, 8.2%. Thus, OTA reabsorption in PST and ALH is
pH-independent. Reabsorption in PST but not in DT or CD was inhibited
by sulfobromophthalein, a substrate of the apical organic anion
carrier. L-Phenylalanine did not reduce OTA reabsorption.
After intravenous injection of unlabeled OTA, resulting in a plasma
concentration of ~10
mol/l, the FR of
[3H]OTA during early proximal microinfusion was reduced
slightly. From our results we conclude: 1) OTA can be reabsorbed in all nephron segments investigated. 2) Under physiological conditions the
predominant sites of reabsorption are PST, ALH and terminal CD. 3)
Reabsorption in PST and ALH is not pH-dependent. 4) pH-independent reabsorption in PST is mediated by the apical organic anion transporter (OAT-K1), whereas pH-dependent reabsorption in PCT is mediated by
H+-dipeptide cotransporter(s). 5) Reabsorption also takes
place during natural exposure, i.e., when OTA is present
in plasma and renal tissue. 6) The high FR in ALH and CD explains, at
least in part, the preferential impairment of postproximal functions and the accumulation in renal inner medulla and papilla.
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