Makoto Ishizaki scite author profile

We investigated whether captopril, an angiotensin-converting-enzyme inhibitor, would reduce proteinuria in patients with advanced diabetic nephropathy. Captopril (37.5 mg given in divided doses three times daily) was administered to 10 azotemic diabetics with heavy proteinuria. Urinary protein decreased promptly within two weeks (from 10.6 +/- 2.2 to 6.1 +/- 1.4 g per day [mean +/- S.E.M.]; P less than 0.01). The decrease in proteinuria did not coincide with a fall in systemic blood pressure or in the blood glucose concentration. Serum creatinine and potassium values did not change in any of the patients except one. We suggest that captopril caused a decrease in intrarenal hypertension, which contributed to the reduction of urinary protein excretion. The therapeutic value of this intervention remains to be established.

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Lanthanum Carbonate Treatment of Patients with Hyperphosphatemia Undergoing CAPD

Kawanishi¹,

Ishida²,

Ishizaki³

et al. 2008

Perit Dial Int

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Reversal of Transplant Rejection by Monoclonal Antiblast Antibody

et al. 1983

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Makoto Ishizaki

Effect of Captopril on Heavy Proteinuria in Azotemic Diabetics

Lanthanum Carbonate Treatment of Patients with Hyperphosphatemia Undergoing CAPD

Reversal of Transplant Rejection by Monoclonal Antiblast Antibody

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