In 1994, we reported a 3.4 +/- 0.8 year follow-up of the eight patients who experienced remission of nephrotic syndrome during the Collaborative Study Group-sponsored, multicenter trial of captopril therapy in patients with type 1 diabetes with nephropathy (Captopril Study). Of the 409 patients randomized to treatment on the Captopril Study, 108 had nephrotic syndrome (24-hour proteinuria greater than or equal to 3.5 g of protein) at baseline. Of these 108 patients, 8 experienced remission of nephrotic syndrome (proteinuria less than or equal to 1.0 g/24 h of protein). Remission was significantly associated with captopril therapy and control of systolic blood pressure. The present study describes the status of these eight patients during a follow-up of 7.7 +/- 0.3 years. Since our previous report, one patient has been lost to follow-up and one patient progressed to end-stage renal disease (ESRD) 3.7 years after completion of the Captopril Study. The remaining six patients remain in remission of nephrotic syndrome (mean 24-hour proteinuria, 1.03 +/- 0.3 g of protein) and have stable serum creatinine levels (mean, 1.58 +/- 0.3 mg/dL) and body weights (mean, 69.8 +/- 5.3 kg). Of the six patients, one has discontinued angiotensin-converting enzyme inhibitor (ACEI) therapy because of hypotension. Excluding the patient who progressed to ESRD, the current mean systolic brood pressure is 135 +/- 6 mm Hg and mean diastolic blood pressure is 78 +/- 4 mm Hg. We conclude that long-term remission of nephrotic syndrome and preservation of renal function is achievable in some patients with type 1 diabetes. Control of blood pressure and ACEI therapy appear to be important in achieving long-term remission. (C) 1999 by the National Kidney Foundation, Inc.
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Inst Canc Res, Div Genet & Epidemiol, London, England
Inst Canc Res, Div Breast Canc Res, London, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Swerdlow, Anthony J.
Jones, Michael E.
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Inst Canc Res, Div Genet & Epidemiol, London, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Jones, Michael E.
Slater, Stefan D.
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80 Whitehouse Rd, Edinburgh, ScotlandInst Canc Res, Div Genet & Epidemiol, London, England
Slater, Stefan D.
Burden, Andrew C. F.
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Top Orchard, Broadhembury, Honiton, Devon, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Burden, Andrew C. F.
Botha, Johannes L.
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Meanwood, Leeds, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Botha, Johannes L.
Waugh, Norman R.
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Univ Warwick, Div Hlth Sci, Coventry, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Waugh, Norman R.
Morris, Andrew D.
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Hlth Data Res UK, London, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Morris, Andrew D.
Gatling, Wendy
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Poole Hosp NHS Trust, Dept Diabet, Poole, Dorset, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Gatling, Wendy
Gillespie, Kathleen M.
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Univ Bristol, Bristol Med Sch, Diabet & Metab, Bristol, EnglandInst Canc Res, Div Genet & Epidemiol, London, England
Gillespie, Kathleen M.
Patterson, Christopher C.
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Queens Univ, Dept Epidemiol & Publ Hlth, Belfast, North IrelandInst Canc Res, Div Genet & Epidemiol, London, England
Patterson, Christopher C.
Schoemaker, Minouk J.
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Global Database Studies, Real World Solut IQVIA, Amsterdam, NetherlandsInst Canc Res, Div Genet & Epidemiol, London, England