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Strategy to estimate risk progression of chronic kidney disease, cardiovascular risk, and referral to nephrology:: the EPIRCE Study

  • Autores: Pilar Gayoso Diz, Alfonso Otero González, M. Xosé Rodríguez Álvarez, Fernando García López, Arturo González Quintela, Ángel L. Martín De Francisco
  • Localización: Nefrología: publicación oficial de la Sociedad Española de Nefrología, ISSN 0211-6995, Vol. 33, Nº. 2, 2013, págs. 223-230
  • Idioma: inglés
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  • Resumen
    • Background:

      Although the prevalence of chronic kidney disease (CKD) is 10�14%, several prospective studies note a low rate of progression to end-stage renal disease (ESRD) in stages 3 and 4. A correct classification of risk of progression, based on demonstrated predictive factors, would allow better management of CKD. Recent studies have demonstrated the high predictive value of a classification that combines estimated (e) glomerular filtration rate (GFR) and urine albumin�creatinine ratio (ACR). We estimated the clinical risk of progression to ESRD and cardiovascular mortality predicted by the combined variable of eGFR and ACR in the Spanish general population.

      Materials and Methods:

      This study was a cross- sectional evaluation in the Epirce sample, representative of Spanish population older than 20 years. GFR was estimated using MDRD and CKD-EPI formulas; microalbuminuria was considered to be an ACR 20�200 mg/g (men) or 30�300 mg/g (women) and macroalbuminuria was indicated beyond these limits. Population- weighted prevalence of risk of progression of CKD to ESRD was estimated.

      Results:

      With MDRD, 1.4% of the adult Spanish population was at moderate risk of progression to ESRD, 0.1% at high risk, and 12.3% at low risk. With CKD-EPI, the moderate risk ratio rose to 1.7% and low risk to 12.6%, but high risk remained stable.

      Conclusions:

      The addition of ACR to eGFR best classifies the population at risk for renal impairment relative to Kidney/Disease Outcomes Quality Initiative grades 3 and 4. Estimating GFR with CKD-EPI modifies the distribution of low and moderate risk


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