Rosa Miquel Rodríguez1, Sergio Luis-Lima2, Juan Manuel Fernandez3, María Vanesa Pérez Gómez2, Beatriz González Toledo2, Marian Cobo1, Patricia Delgado-Mallén1, Beatriz Escamilla1, Cristina Oramas Marco4, Sara Estupiñán1, Coriolano Cruz Perera5, Natalia Negrín Mena5, Laura Díaz Martín4,6, Sergio Pitti Reyes7, Ibrahim Hernández González7, Federico González-Rinne5, Alejandra González-Delgado8, Carmen Ferrer-Moure8, Begoña López-Botet Zulueta2, Armando Torres1,9,10, Jose Carlos Rodriguez Pérez3,11, Flavio Gaspari4, Alberto Ortiz2,6, Esteban Porrini12,13,14,15. 1. Nephrology Department, Hospital Universitario de Canarias, Tenerife, Spain. 2. Department of Nephrology and Hypertension, IIS-Fundación Jimenez Díaz, UAM, Madrid, Spain. 3. Nephrology Department, Hospital Universitario Dr Negrín, Las Palmas, Spain. 4. Laboratory of Renal Function, Faculty of Medicine, University of La Laguna, La Laguna, Spain. 5. Research Unit, Hospital Universitario de Canarias, Calle Ofra s/n 38023 La Laguna, Tenerife, Spain. 6. Red de Investigación Renal (REDINREN), Instituto Carlos III-FEDER, 28040, Madrid, Spain. 7. Radiology Unit, Hospital Universitario de Canarias, Tenerife, Spain. 8. Central Laboratory, Hospital Universitario de Canarias, Tenerife, Spain. 9. Internal Medicine Department, Faculty of Medicine, Universidad de La Laguna, Tenerife, Spain. 10. Instituto de Tecnología Biomédicas, ITB, Universidad de La Laguna, La Laguna, Spain. 11. University of Las Palmas de Gran Canaria, Las Palmas de Gran Canaria, Spain. 12. Research Unit, Hospital Universitario de Canarias, Calle Ofra s/n 38023 La Laguna, Tenerife, Spain. esteban.l.porrini@gmail.com. 13. Internal Medicine Department, Faculty of Medicine, Universidad de La Laguna, Tenerife, Spain. esteban.l.porrini@gmail.com. 14. Instituto de Tecnología Biomédicas, ITB, Universidad de La Laguna, La Laguna, Spain. esteban.l.porrini@gmail.com. 15. Laboratory of Renal Function, Faculty of Medicine, University of La Laguna, La Laguna, Spain. esteban.l.porrini@gmail.com.
Abstract
BACKGROUND: Autosomal dominant polycystic kidney disease (ADPKD) causes about 10% of cases of end stage renal disease. Disease progression rate is heterogeneous. Tolvaptan is presently the only specific therapeutic option to slow kidney function decline in adults at risk of rapidly progressing ADPKD with chronic kidney disease (CKD) stages 1-4. Thus, a reliable evaluation of kidney function in patients with ADPKD is needed. METHODS: We evaluated the agreement between measured (mGFR) and estimated glomerular filtration rate (eGFR) by 61 formulas based on creatinine and/or cystatin-C (eGFR) in 226 ADPKD patients with diverse GFR values, from predialysis to glomerular hyperfiltration. Also, we evaluated whether incorrect categorization of CKD using eGFR may interfere with the indication and/or reimbursement of Tolvaptan treatment. RESULTS: No formula showed acceptable agreement with mGFR. Total Deviation Index averaged about 50% for eGFR based on creatinine and/or cystatin-C, indicating that 90% of the estimations of GFR showed bounds of error of 50% when compared with mGFR. In 1 out of 4 cases with mGFR < 30 ml/min, eGFR provided estimations above this threshold. Also, in half of the cases with mGFR between 30 and 40 ml/min, formulas estimated values < 30 ml/min. CONCLUSIONS: The evaluation of renal function with formulas in ADPKD patients is unreliable. Extreme deviation from real renal function is quite frequent. The consequences of this error deserve attention, especially in rapid progressors who may benefit from starting treatment with tolvaptan and in whom specific GFR thresholds are needed for the indication or reimbursement. Whenever possible, mGFR is recommended.
BACKGROUND: Autosomal dominant polycystic kidney disease (ADPKD) causes about 10% of cases of end stage renal disease. Disease progression rate is heterogeneous. Tolvaptan is presently the only specific therapeutic option to slow kidney function decline in adults at risk of rapidly progressing ADPKD with chronic kidney disease (CKD) stages 1-4. Thus, a reliable evaluation of kidney function in patients with ADPKD is needed. METHODS: We evaluated the agreement between measured (mGFR) and estimated glomerular filtration rate (eGFR) by 61 formulas based on creatinine and/or cystatin-C (eGFR) in 226 ADPKD patients with diverse GFR values, from predialysis to glomerular hyperfiltration. Also, we evaluated whether incorrect categorization of CKD using eGFR may interfere with the indication and/or reimbursement of Tolvaptan treatment. RESULTS: No formula showed acceptable agreement with mGFR. Total Deviation Index averaged about 50% for eGFR based on creatinine and/or cystatin-C, indicating that 90% of the estimations of GFR showed bounds of error of 50% when compared with mGFR. In 1 out of 4 cases with mGFR < 30 ml/min, eGFR provided estimations above this threshold. Also, in half of the cases with mGFR between 30 and 40 ml/min, formulas estimated values < 30 ml/min. CONCLUSIONS: The evaluation of renal function with formulas in ADPKD patients is unreliable. Extreme deviation from real renal function is quite frequent. The consequences of this error deserve attention, especially in rapid progressors who may benefit from starting treatment with tolvaptan and in whom specific GFR thresholds are needed for the indication or reimbursement. Whenever possible, mGFR is recommended.
Authors: Edwin M Spithoven; Esther Meijer; Wendy E Boertien; Steef J Sinkeler; Hilde Tent; Paul E de Jong; Gerjan Navis; Ron T Gansevoort Journal: Am J Kidney Dis Date: 2013-05-25 Impact factor: 8.860
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