Your search keyword '"Chaves, H."' showing total 6 results

1. I Brazilian position statement on arterial hypertension and diabetes mellitus.

Author

Alessi A, Bonfim AV, Brandão AA, Feitosa A, Amodeo C, Alves CR, Brasil DP, Souza Ddo S, Barbosa E, Consolim-Colombo FM, Borelli F, Fonseca FH, Lopes HF, Chaves H, Bortolotto LA, Martin LC, Scala LC, Mota-Gomes MA, Malachias MV, Izar MC, Fonseca MI, Neves MF, Morais NS, Passarelli O Jr, Jardim PC, Toscano PR, Miranda RD, Franco R, Betti RT, Pedrosa RP, Povoa R, Carneiro SB, Jardim T, and Barroso WK

Subjects

Blood Glucose, Blood Pressure, Brain Diseases etiology, Brazil, Diabetes Complications therapy, Dyslipidemias drug therapy, Heart Diseases etiology, Humans, Hypertension therapy, Kidney Diseases etiology, Peripheral Arterial Disease etiology, Risk Factors, Societies, Medical, Diabetes Mellitus therapy, Hypertension complications

Published

2013

2. [IV Brazilian Guideline for Dyslipidemia and Atherosclerosis prevention: Department of Atherosclerosis of Brazilian Society of Cardiology].

Author

Sposito AC, Caramelli B, Fonseca FA, Bertolami MC, Afiune Neto A, Souza AD, Lottenberg AM, Chacra AP, Faludi AA, Loures-Vale AA, Carvalho AC, Duncan B, Gelonese B, Polanczyk C, Rodrigues Sobrinho CR, Scherr C, Karla C, Armaganijan D, Moriguchi E, Saraiva F, Pichetti G, Xavier HT, Chaves H, Borges JL, Diament J, Guimarães JI, Nicolau JC, dos Santos JE, de Lima JJ, Vieira JL, Novazzi JP, Faria Neto JR, Torres KP, Pinto Lde A, Bricarello L, Bodanese LC, Introcaso L, Malachias MV, Izar MC, Magalhães ME, Schmidt MI, Scartezini M, Nobre M, Foppa M, Forti NA, Berwanger O, Gebara OC, Coelho OR, Maranhão RC, dos Santos Filho RD, Costa RP, Barreto S, Kaiser S, Ihara S, Carvalho Td, Martinez TL, Relvas WG, and Salgado W

Subjects

Adult, Age Distribution, Aged, Cholesterol blood, Clofibric Acid therapeutic use, Coronary Artery Disease etiology, Coronary Artery Disease physiopathology, Diet, Female, Humans, Hyperlipidemias complications, Hyperlipidemias physiopathology, Hypolipidemic Agents therapeutic use, Lipid Metabolism drug effects, Male, Metabolic Syndrome complications, Middle Aged, Naphthalenes therapeutic use, Risk Factors, Sex Distribution, Smoking adverse effects, Triglycerides blood, Coronary Artery Disease prevention & control, Hyperlipidemias therapy, Lipid Metabolism physiology

Published

2007

3. [IV Guideline for ambulatory blood pressure monitoring. II Guideline for home blood pressure monitoring. IV ABPM/II HBPM].

Author

Alessi A, Brandão AA, Pierin A, Feitosa AM, Machado CA, de Moraes Forjaz CL, Atie CS, Giorgi DM, Mion D Jr, Rosa EC, Nobre F, Silva GV, Chaves H Jr, Pascoal IJ, Guimarães JI, Santello JL, Ribeiro JM, Praxedes JN, Ortega KC, da Costa LS, Bortolotto LA, Gomes MA, Wajngarten M, Gus M, Kohlmann O Jr, Jardim PC, Geleilete TJ, and Koch V

Subjects

Blood Pressure Determination standards, Humans, Blood Pressure Monitoring, Ambulatory standards, Self Care standards

Published

2005

4. [Multicenter National Study for the evaluation of the efficacy and tolerance of nifedipine oral release osmotic system in mild to moderate hypertension].

Author

Amodeo C, Brandão AP, Giorge DM, Mion Júnior D, Lima Júnior E, Nobre F, Chaves H, de Andradre J, Ayoub JC, and Ribeiro JM

Subjects

Administration, Oral, Aged, Aged, 80 and over, Blood Pressure drug effects, Blood Pressure Monitoring, Ambulatory, Female, Humans, Male, Middle Aged, Hypertension drug therapy, Nifedipine therapeutic use

Abstract

Purpose: Evaluation of the efficacy and tolerability of nifedipine oros in patients with mild to moderate essential hypertension without major target organ damage and the anti-hypertensive effect along the 24 hours., Methods: Two hundred and three patients were studied. After two weeks placebo running period single dose of nifedipine oros (30 mg/day) was administered for 8 weeks. At the end of the 4th week, the non-responders (diastolic blood pressure > 90 mmHg or reduction in diastolic pressure < 10 mmHg), had the dosage increased to 60 mg/day. Laboratory tests and 24h blood pressure monitoring (60 patients) were performed at the beginning and at the end of the study., Results: One hundred and ninety one patients completed the study. Fifty nine percent were considered responders at the end of the 4th week with nifedipine oros 30 mg/day and 41% needed dosage increment to 60 mg/day. At the end of the 8th week, all patients were considered responders to nifedipine oros. The blood pressure control extended throughout the 24h of the day. The most common adverse events were edema (14.6%) and headache (12.4%). Good and very good tolerability were informed by 85% of the patients., Conclusion: Nifedipine oros was able to control blood pressure efficaciously along the 24h period without important side effects. The possibility of once day dosage, increases the patient adherence to anti-hypertensive therapy.

Published

1995

5. [A Brazilian multicenter study to evaluate the clinical effectiveness and tolerance of isradipine SRO using ambulatory monitoring of arterial pressure in the treatment of mild and moderate arterial hypertension].

Author

Magliano MF, Amodeo C, Mion Júnior D, Francischetti E, Lima Júnior E, Nobre F, Chaves H, Ribeiro JM, Spritzer N, and Jardim PC

Subjects

Adult, Aged, Blood Pressure drug effects, Blood Pressure Determination, Female, Humans, Hypertension physiopathology, Male, Middle Aged, Monitoring, Physiologic, Hypertension drug therapy, Isradipine administration & dosage

Abstract

Purpose: To evaluate clinical efficacy and tolerability of isradipine SRO (I.SRO), 5 mg O.D. in essential hypertensives., Methods: Eighty-three of 87 selected outpatients with a mean age of 51.3 years (ranging from 25 to 65), 33 male, 48 white, 29 black and others of different races, who had clinical supine and orthostatic diastolic blood pressure (DBP) > or = 95 mmHg and < or = 115 mmHg underwent the study. After a three-week wash-out period, patients received I.SRO 5 mg O.D. at 8:00 am for a six-week period (phase I). After this phase, patients received I.SRO 5 mg O.D. at 8:00 pm for a six-week period (phase II). The patients had a follow-up with an interval of three weeks and the ambulatorial blood pressure monitoring (ABPM) for 24 hours was performed with a SpaceLabs 90207 or Del Mar Avionics devices after the wash-out period and at the end of phases I and II. Measurements were performed at 15-min intervals during the day (6 am to 10 pm) and at 30-min intervals during the night (10 pm to 6 am)., Results: a) Heart rate did not show significant changes during the treatment period (phases I and II) when compared with the wash-out period; b) causal blood pressure: at the end of both treatment periods (phases I and II) there were statistically significant decreases (p < 0.001) in supine SBP and DBP compared with wash-out values. The mean SBP decreased from 161.6 +/- 14 to 144.3 +/- 13 mmHg (phase I) and to 141.8 +/- 13 mmHg (phase II). The mean DBP decreased from 103.4 +/- 6 to 91.2 +/- 7 (phase I) and to 89.1 +/- 8 (phase II); c) ABPM: the mean systolic 24-h ambulatory blood pressure was significantly reduced (p < 0.001) from 148.8 +/- 17 to 137.2 +/- 15 mmHg (phase I) and to 133.4 +/- 13 mmHg (phase II). The mean diastolic 24-h ambulatory blood pressure was significantly decreased (p < 0.001) from 94.3 +/- 9 to 87.0 +/- 9 (phase I) and to 85.8 +/- 8 mmHg (phase II). The mean daytime and nighttime, systolic and diastolic 24-h ambulatory blood pressure were: wash-out--152.3 +/- 17, 140.2 +/- 21, 97.4 +/- 9, 86.8 +/- 13; phase I--139.9 +/- 15, 130.0 +/- 17, 89.3 +/- 9, 81.3 +/- 10; phase II--136.7 +/- 13, 125.3 +/- 15, 88.5 +/- 8, 79.1 +/- 10, respectively. Blood pressure load (percentage of systolic blood pressure values > 140 mmHg or of diastolic blood pressure values > 90 mmHg) was significantly reduced from 62.2/62% (SBP/DBP), on the was-out, to 37.9/39.9% (SBP/DBP) on phase I and to 32.3/34.3% (SBP/DBP) on phase II; d) side effects: most frequently related were palpitations (2.3%), headache (1.1%), flush (1%) and ankle oedema (1%). They were in general, mild-to-moderate and disappeared after the first 3 weeks of treatment. Only two patients were withdrawn because of headache (one of them with previous diagnosis of migraine)., Conclusion: I.SRO, given by oral route, in the dosage of 5 mg O.D. as monotherapy, was effective and well tolerated, promoted significant reduction on 24-h ambulatory blood pressure attenuating the early morning rise and did not interfere with the circadian rhythm of blood pressure. No significant differences were detected in the BP lowering effect when I.SRO was given during the morning or evening. These results may indicate that the drug is as suitable as one of the first choice for treating mild and moderate hypertensive patients.

Published

1993

6. [Fosinopril in a daily single dose in mild and moderate hypertension. Brazilian multicenter study].

Author

Mion Júnior D, Lima Júnior E, Almeida FA, Chaves H, Rocha JC, Nicolau JC, Saragoça M, Spritzer N, Kohlmann Júnior O, and Luna RL

Subjects

Adolescent, Adult, Aged, Blood Pressure drug effects, Brazil, Drug Administration Schedule, Female, Fosinopril therapeutic use, Humans, Male, Middle Aged, Time Factors, Fosinopril administration & dosage, Hypertension drug therapy

Abstract

Purpose: To evaluate during 12 weeks the effectiveness and safety of once-a-day fosinopril (10 or 20 mg/day comparative to placebo) in mild to moderate hypertensives according to an open design comparative to placebo., Methods: One hundred and nineteen patients were studied; 52 +/- 11 years (mean +/- sd) range 18 a 76 years, 86 women and 33 men, 57% whites, 26% blacks and 17% mulattos, 71 mild hypertensives (95 < or = diastolic pressure < or = 104mmHg) e 48 moderate hypertensives (101 < diastolic pressure < or = 115mmHg)., Results: There was a significant reduction in systolic/diastolic pressure on the 6th week of treatment (from 161 +/- 16/103 +/- 7 before to 148 +/- 16/94 +/- 9mmHg on the 6th week). On the 12th week of treatment there was an additional significant reduction in systolic/diastolic pressure (from 148 +/- 16/94 +/- 9 on the 6th week to 145 +/- 17/89 +/- 8mmHg on the 12th week). There was a "favorable" response in 71% of the patients on the 12th week; 62% showed diastolic pressure < or = 90mmHg and 9% presented diastolic reduction > or = 10mmHg. There was no difference in the normalization rates between whites and non-whites, mild and moderate hypertensive, obese and non-obese patients, under or above 50 years of age and those patients from no drug-treatment to those on 3 drug before the study. There was no clinically relevant changes in laboratory evaluations before and at the end of the study. The number of adverse reactions was reduced in comparison with previous treatment., Conclusion: Fosinopril, according to our and others data, is effective and safe for the treatment of mild to moderate hypertensives, in whites or non-whites, obese or non-obese, younger or older than 50 years and receiving 0 or 3 drugs before the study.

Published

1993