Renal Glycosuria without Hyperglycemia in Cyclosporine-Treated Rats
Author(s) -
Chang Hwa Lee,
Sua Kim,
Chong Myung Kang,
GheunHo Kim
Publication year - 2012
Publication title -
kidney research and clinical practice
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.152
H-Index - 20
eISSN - 2211-9140
pISSN - 2211-9132
DOI - 10.1016/j.krcp.2012.04.457
Subject(s) - glycosuria , endocrinology , medicine , nephrotoxicity , reabsorption , diabetes mellitus , renal glucose reabsorption , kidney , urine , excretion , urinary system , renal physiology , type 2 diabetes
Background/AimsThe pathogenesis of post-transplant diabetes mellitus is thought to be partly related to the direct toxic effect of cyclosporine on pancreatic β-cells and the resultant decrease in insulin synthesis and secretion. As a result of hyperglycemia , glycosuria may be found in cyclosporine administration. However, mechanism of glycosuria in cyclosporine nephrotoxicity was not clearMethodsCyclosporine was subcutaneously injected to male Sprague-Dawley rats at a daily dose of 7.5mg/kg (n=6) for 6 weeks. Biochemical data were obtained from urine and plasma samples.ResultsCyclosporine treatment caused a remarkable increase in urine volume and a decrease in urine osmolality. Urinary excretion of glucose was remarkably elevated by cyclosporine administration (7±3.0mg/dL versus 12896±3218mg/dL; P < 0.005). Plasma glucose levels at the end of animal experiment were not affected by cyclosporine administration (117 ± 40.6mg/dL versus 114 ±26.0mg/dL; NS). Vehicle-treated controls had a larger final BW than cyclosporine-treated (309±17g versus 275±13g; p < 0.01), steady weight gain was obtained in both groups. We did not find any evidence of generalized proximal tubular dysfunctionConclusionGlycosuria may occur without hyperglycemia in cyclosporine administration. We suggest that cyclosporine may decrease tubular reabsorption of glucose in renal tubular epithelial cells, and then glycosuria could be induced by the altered glucose transporter expressions. We will analyze the glucose transporters in proximal tubule of rat kidney
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