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Vol. 281, Issue 3, 1457-1462, 1997
and Fibronectin, and
Lipid Peroxidation Induced by High Glucose in Cultured Mesangial
Cells1
Department of Pharmacology, Yonsei University College of Medicine,
Seoul 120-752, Korea
Oxidative stress has been proposed as the basis for the pathogenesis of
diabetic nephropathy. Rebamipide is a novel antiulcer drug that has, in
addition, oxygen radical scavenging activity. Our study examines
whether rebamipide could ameliorate the pathophysiology associated with
experimental diabetes in vivo, such as microalbuminuria, and
to reverse the increased production of transforming growth factor-
1 and fibronectin in SV-40 transformed murine
mesangial cells in culture that were stimulated with high glucose.
Chronic administration of rebamipide (100 mg/kg/day, p.o., for 3 wk) to rats, in which diabetes was previously induced by the i.v. injection of
streptozotocin 50 mg/kg, reversed hyperglycemia, which would contribute
to prevent the increases in urinary excretion rates of albumin and
lipid peroxides observed in this experimental model. Rebamipide, at
this dose level, did not cause any discernible effect on age-matched
control rats. Rebamipide 2 mM was as effective as 20 mM of
dimethylthiourea, a known hydroxyl radical scavenger, in inhibiting the
increase in lipid peroxides, transforming growth factor-
1, fibronectin mRNAs and proteins induced by
incubation of cultured mesangial cells with high glucose. Our data
suggest that rebamipide attenuates high glucose-induced nephropathy,
which is attributable, in part, to its antioxidative property and, in part, to its effect on reversing hyperglycemia.
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