›› 2002, Vol. 22 ›› Issue (2): 78-82.

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Establishment of Diabetic Nephropathy Model in Rat

  

  1. Shanghai Institute of Materia Medica,Chinese Academy of Science,Shanghai 200031, China
  • Received:2002-01-23 Online:2002-01-25 Published:2013-03-19

Abstract: Type I diabetes mellitus were made in Wistar rats by intravenous injection of 35 mg/kg streptozotocin freshly dissolved in citrate-buffered saline solution. Stable moderate hyperglycemia was maintained throughout the duration of the experiment,without receiving any insulin injection. Body weights were markedly reduced at 1 week after induction of the diabetes and maintained throughout the experiment in the untreated diabetic rats,whereas non-diabetic control rats gained weight during the 5-month follow-up. Blood pressure (BP) and renal function data at 5 months after induction of diabetes were summarized.The untreated uninephrectomized diabetic rats developed hypertension with mean arterial pressure (MAP) of 128±2 mmHg under anesthesia. Renal vascular resistance (RVR) was markedly elevated·in the untreated diabetic rats as compared to that in controls (P<0.001),leading to a significant lower renal plasma flow (RPF)(P<0.01).Glomerular filtration rate (GFR) was comparable between untreated diabetic rats and controls.Thus,Filtration fraction (FF) rose significantly (P<0.001).Urine flow rate was also markedly increased in the untreated diabetic rats.Un-treated diabetic rats showed a significant increase in urinary protein excretion as early as 4 weeks after induction of the disease (36.8±3.6 vs. 21. 5±1.7,P<0.01 in control rats at week 4) , with a substantial progressive increase of this value over time. A ratio of the heart weight to the body weight was 3. 5±0.1 to 2.4±0.1 (P<0.001) and the left kidney weight to the body weight was 9.9±0.7 to 3. 9±0.1 (P<0.001).Both ra-tios were markedly higher in untreated diabetic rats as compared to those in controls. Thus, the STZ-injected uninephrectomized rats developed overt diabetic nephropathy,as evidenced by the development of hypertension,progressive proteinuria and renal dys-function.

Key words: Wistar rats, Type I diabetes mellitus, Nephropathy, Hyperglycemia, Urinary protein