ABSTRACT
Objetivo: Evaluar la respuesta antiproteinúrica a un tratamiento multifactorial basado en dosis elevadas de antagonistas de los receptores de la angiotensina II (ARAII) (olmesartán) en pacientes con nefropatías proteinúricas no diabéticas, según tres de los polimorfismos del sistema renina-angiotensina (SRA): inserción/deleción del gen de la enzima convertidora de angiontensina (ECA), M235T del gen del angiotensinógeno y A1166C del receptor AT1 (rAT1) para la angiotensina II. Material y métodos: Se estudiaron 53 pacientes con nefropatía proteinúrica no diabética, con un tiempo medio de evolución de 84,4 ± 15 meses. Género varón en 41 (77,4 %); edad media 49,7 ± 3 años; índice de masa corporal 30 ± 6 kg/m2. Todos recibieron olmesartán (40 mg/12 h) asociado a un promedio de 2,4 ± 1,6 fármacos antihipertensivos durante una mediana de tiempo de 13 meses (rango intercuartil 7-25 meses). Resultados: La presión arterial (PA) sistólica descendió de 145 ± 14 hasta 128 ± 14 mmHg (p < 0,001) y la PA diastólica desde 85 ± 11 a 79 ± 7 mmHg (p < 0,01). La presión de pulso pasó de 53,5 ± 14 a 48 ± 12 mmHg (p < 0,05). La proteinuria se redujo de 2,74 ± 1,6 a 0,9 ± 1 g/24 h (p < 0,001), representando un descenso promedio del 67,1 %. Según los polimorfismos del SRA, la respuesta antiproteinúrica fue: polimorfismo del gen del angiotensiógeno: genotipo TT: 76,8 %; genotipo MM: 67,3 %; genotipo MT: 65,8 %, significativamente mayor (p < 0,05) para genotipo TT respecto de MM y MT. Polimorfismo del gen de la ECA: genotipo DD: 71,4 %; genotipo ID: 60,6 %, genotipo II: 34,8 %, significativamente mayor (p < 0,05) para genotipo DD respecto a ID e II, y asimismo (p < 0,05) para el genotipo ID respecto a II. Polimorfismo del gen del rAT1: genotipo AC: 85,2 %; genotipo CC: 73,7 %; genotipo AA: 62,7 %; significativamente mayor para el genotipo AC (p < 0,05) respecto a AA y CC. Las diferencias entre la proteinuria inicial y final del período de seguimiento fueron significativas (p < 0,01) para las asociaciones genotípicas: DD/AA, DD/MT, DD/MM, DD/TT y DD/AC, si bien la asociación con mayor efecto antiproteinúrico fue DD/AC (89,9 %, p < 0,05 %). Conclusiones: La administración de dosis altas de olmesartán en pacientes con nefropatía proteinúrica no diabética comporta reducciones significativas en la proteinuria. Este descenso fue independiente del control tensional y de otros factores de confusión. Los polimorfismos del SRA pueden modular la respuesta antiproteinúrica al tratamiento con ARAII
Objective: To assess the antiproteinuric response to multifactorial treatment based on high doses of angiotensin II receptor antagonists (ARBs) (olmesartan) in patients with non-diabetic proteinuric nephropathies, according to three renin-angiotensin system (RAS) polymorphisms: insertion/deletion of the angiotensin converting enzyme (ACE) gene, the angiotensinogen gene M235T and the angiotensin II type 1 receptor (AT1R) A1166C. Material and method: We studied 53 patients with non-diabetic proteinuric nephropathy with a mean progression time of 84.4±15 months. 41 were males (77.4%); mean age 49.7±3 years, body mass index 30±6kg/m2. All received olmesartan (40mg/12h) associated with a mean of 2.4±1.6 antihypertensive drugs for a median period of 13 months (interquartile range 7-25 months). Results: Systolic blood pressure (BP) decreased from 145±14mmHg to 128±14mmHg (P<.001) and diastolic BP from 85±11mmHg to 79±7mmHg (P<.01). Pulse pressure decreased from 53.5±14mmHg to 48±12mmHg (P<.05). Proteinuria decreased from 2.74±1.6g/24h to 0.9±1g/24h (P<.001), representing a mean decrease of 67.1%. According to RAS polymorphisms, antiproteinuric response was: angiotensinogen gene polymorphism: genotype TT: 76.8%; genotype MM: 67.3%; genotype MT: 65.8%, significantly higher (P<.05) for genotype TT compared to genotypes MM and MT. Polymorphism of the ACE gene: genotype DD: 71.4%; genotype ID: 60.6%, genotype II: 34.8%, significantly higher (P<.05) for genotype DD compared to genotypes ID and II, and also (P<.05) for genotype ID compared to II. AT1R gene polymorphism: genotype AC: 85.2%; genotype CC: 73.7%; genotype AA: 62.7%; significantly higher for genotype AC (P<.05) compared to genotypes AA and CC. The differences between initial and final proteinuria for the follow-up period were significant (P<.01) for genotypic associations DD/AA, DD/MT, DD/MM, DD/TT and DD/AC, although the association with the highest antiproteinuric effect was DD/AC (89.9%, P<.05%). Conclusions: Administering high doses of olmesartan in patients with non-diabetic proteinuric nephropathy results in significant reductions in proteinuria. This decrease was independent of blood pressure control and other confounding factors. RAS polymorphisms may modulate the antiproteinuric response to treatment with ARBs
Subject(s)
Humans , Genotype , Proteinuria/physiopathology , Renin-Angiotensin System , Antihypertensive Agents/pharmacokinetics , Renal Insufficiency, Chronic/physiopathology , Cardiovascular Diseases/epidemiology , Kidney TransplantationABSTRACT
OBJECTIVE: To assess the antiproteinuric response to multifactorial treatment based on high doses of angiotensin II receptor antagonists (ARBs) (olmesartan) in patients with non-diabetic proteinuric nephropathies, according to three renin-angiotensin system (RAS) polymorphisms: insertion/deletion of the angiotensin converting enzyme (ACE) gene, the angiotensinogen gene M235T and the angiotensin II type 1 receptor (AT1R) A1166C. MATERIAL AND METHOD: We studied 53 patients with non-diabetic proteinuric nephropathy with a mean progression time of 84.4±15 months. 41 were males (77.4%); mean age 49.7±3 years, body mass index 30±6kg/m2. All received olmesartan (40mg/12h) associated with a mean of 2.4±1.6 antihypertensive drugs for a median period of 13 months (interquartile range 7-25 months). RESULTS: Systolic blood pressure (BP) decreased from 145±14mmHg to 128±14mmHg (P<.001) and diastolic BP from 85±11mmHg to 79±7mmHg (P<.01). Pulse pressure decreased from 53.5±14mmHg to 48±12mmHg (P<.05). Proteinuria decreased from 2.74±1.6g/24h to 0.9±1g/24h (P<.001), representing a mean decrease of 67.1%. According to RAS polymorphisms, antiproteinuric response was: angiotensinogen gene polymorphism: genotype TT: 76.8%; genotype MM: 67.3%; genotype MT: 65.8%, significantly higher (P<.05) for genotype TT compared to genotypes MM and MT. Polymorphism of the ACE gene: genotype DD: 71.4%; genotype ID: 60.6%, genotype II: 34.8%, significantly higher (P<.05) for genotype DD compared to genotypes ID and II, and also (P<.05) for genotype ID compared to II. AT1R gene polymorphism: genotype AC: 85.2%; genotype CC: 73.7%; genotype AA: 62.7%; significantly higher for genotype AC (P<.05) compared to genotypes AA and CC. The differences between initial and final proteinuria for the follow-up period were significant (P<.01) for genotypic associations DD/AA, DD/MT, DD/MM, DD/TT and DD/AC, although the association with the highest antiproteinuric effect was DD/AC (89.9%, P<.05%). CONCLUSIONS: Administering high doses of olmesartan in patients with non-diabetic proteinuric nephropathy results in significant reductions in proteinuria. This decrease was independent of blood pressure control and other confounding factors. RAS polymorphisms may modulate the antiproteinuric response to treatment with ARBs.
