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Vol. 67. Núm. 2.
Páginas 181-183 (febrero 2012)
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Vol. 67. Núm. 2.
Páginas 181-183 (febrero 2012)
RAPID COMMUNICATION
Open Access
Prevalence of erectile dysfunction in chronic renal disease patients on conservative treatment
Visitas
908
José Fernando Pereira MesquitaI,
Autor para correspondencia
jfpmesquita@uol.com.br

Tel.: 55 32 3231-2129
, Thiago Faria RamosII, Felipe Pereira MesquitaII, José Murillo Bastos NettoIII, Marcus Gomes BastosIV, André Avarese de FigueiredoV
I Faculdade de Medicina da Universidade Federal de Juiz de Fora, Curso de Pós Graduação em Saúde Brasileira, Juiz de Fora/MG, Brasil
II Faculdade de Medicina da Universidade Federal de Juiz de Fora, Juiz de Fora/MG, Brasil
III Faculdade de Medicina da Universidade Federal de Juiz de Fora, Departamento Materno Infantil e da Residência Médica em Urologia, Juiz de Fora/MG, Brasil
IV Faculdade de Medicina da Universidade Federal de Juiz de Fora Departamento de Clínica Médica, Juiz de Fora/MG, Brasil
V Universidade Federal de Juiz de Fora, Departamento de Anatomia do Instituto de Ciências Biológicas, Juiz de Fora/MG, Brasil
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INTRODUCTION

Erectile dysfunction (ED), the inability to maintain sufficient penile erection for satisfactory sexual performance, is highly prevalent in the general population, affecting almost 50% of men in the 40-70 years age range, which corresponds to approximately 150 million men worldwide (1,2). More recently, ED has been considered a manifestation of a functional and/or structural abnormality affecting penile circulation as part of a more generalized vascular disorder (2).

Erectile dysfunction, therefore, has been associated with signs of generalized arterial disease, as it frequently coexists with diseases with a high component of endothelial dysfunction, such as coronary artery disease, idiopathic systemic arterial hypertension, atherosclerosis, and end-stage chronic kidney disease (ESCKD). ED is also associated with cardiovascular disease risk factors, such as diabetes mellitus, dyslipidemia, and smoking (1–3).

Erectile dysfunction prevalence rates in men with chronic kidney disease (CKD) may reach 70-80%, with similar rates having been reported for those with ESCKD. A number of factors have been implicated in the development of ED in these patients, including the actual presence of a chronic disease, drugs, increased parathyroid hormone (PTH) serum levels, zinc deficiency, decreased testosterone serum levels, increased serum prolactin levels, and psychological factors (3,4).

MATERIALS AND METHODS

This study assessed the prevalence rate of ED in stage 3, 4, and 5 CKD outpatients and sought to identify the associations among ED, CKD stage, and comorbidities. ED was graded according to the International Index of Erectile Function (IIEF), which was validated for use in Portuguese (5).

We assessed 81 patients with a mean age of 61.7±11.6 years (range: 21-84). The results included an estimated ED rate of 70%, significance level of 0.05, presumed error margin of 5%, and a population of 163 elements. The study databank was statistically analyzed with SPSS 13.0 software. For descriptive and bivariate analyses, only the valid cases were used. Logistic regression was used to characterize the relative weight of several variables studied on outcomes among the group of interviewed subjects. This study was approved by the ethics committee of the University Hospital of the Federal University of Juiz de Fora. During the history-taking visit, each subject received an explanation of the study and the shared patient/researcher responsibility in the study's success. Informed consent authorizing data collection was then obtained.

RESULTS

The prevalence of erectile dysfunction among those individuals aged 61 years or older was 85.1% compared with 66.7% of those ranging from 21 to 60 years in age (p = 0.052). The sample size may not have been sufficiently large to demonstrate a significant difference between the groups, as indicated in the literature. The prevalence of ED was 76.5% (62 patients), with 72.3% classified as stage 3 CKD, 81.5% as stage 4 CKD, and 85.7% as stage 5 CKD, although no statistically significant difference was found. Nineteen patients (23.5%) had no ED; 24 (29.6%) had mild ED; 15 (18.5%) had mild/moderate ED; 13 (16%) had moderate ED; and 10 (12.3%) had severe ED. Our study did not demonstrate any association between ED and most comorbidities considered to impart important cardiovascular risk, except diabetes mellitus, which reached significance as both a cause (p = 0.004) of kidney disease and comorbidity (p = 0.006; Tables 1 and 2).

Table 1.

Bivariate analysis of the association between erectile dysfunction and diabetes mellitus.

Variable    With dysfunctionN (%)  p-value 
Diabetes    mellitus  YES  29 (93.6)  0.004* 
  NO  33 (66.0)   
Table 2.

Bivariate analysis of the association between erectile dysfunction and other variables.

Variables  % with Erectile Dysfunction  p-value 
DM2  93.5  0.006 * 
Caucasian  77.2  0.832 
Smoker (current or former)  78.9  0.631 
SAH1  77.6  0.367 
Dyslipidemia  71.4  0.619 
CAD3  85.7  0.549 
PVD4  100  0.125 
Stroke5  66.7  0.553 
ACEI5  79.3  0.351 
ARB6  76.3  0.964 
CCB7  69.4  0.177 
Diuretics  77.6  0.619 
ALPHA-ADREN8  83.3  0.683 
BETA-BLOCK9  82.8  0.324 
Vasodilator  100  0.256 
Nitrate  100  0.329 

p-value<0.05.

1-Systemic Arterial Hypertension; 2-Diabetes Mellitus; 3-Coronary Artery Disease; 4-Peripheral Vascular Disease; 5-Angiotensin-converting Enzyme Inhibitor; 6-Angiotensin Receptor Blocker; 7-Calcium-Channel Blocker; 8-Alpha-adrenergics; 9-Beta-blocker.

Of the 81 patients assessed, 59 were aware of their CKD for 60 months at most. Among these patients, 86.4% had ED, while 50% of those aware of their CKD for longer than 61 months had ED (p = 0.001). Sixty-three patients were followed-up as outpatients for 60 months at most; 82.5% had ED compared with 55.6% of those followed up for longer than 61 months (p = 0.017; Table 3).

Table 3.

Bivariate analysis of the association among erectile dysfunction, the length of disease and the length of follow-up.

Variable    With dysfunction  p-value 
Length of disease  Less than 60 months  51(86.4)  0.001* 
  Equal to or more than61 months  11(50)   
Length of follow-up  Less than 60 months  52(82.5)  0.017* 
  Equal to or more than61 months  10(55.6)   

p-value<0.05.

The logistic regression model revealed that among subjects with ED, those with diabetes mellitus were 4.05 times more likely to have ED than non-diabetic subjects (p = 0.048). However, subjects aware of their CKD for a period of less than 60 months were 3.5 times more likely to have ED than those who were aware of their CKD for longer periods (p = 0.012; Table 4).

Table 4.

Logistic regression model for the association between erectile dysfunction, diabetes mellitus and the duration of chronic kidney disease.

VariableOdds ratio  p-value  CI (95%) 
Diabetes Mellitus  Yes  4.05  0.048*  1.017 – 25.085 
  No     
Length of Disease  Less than 60 months  3.50  0.012*  1.400 – 14.489 
  Equal to or more than 61 months     

Analysis in relation to the “with erectile dysfunction” group of individuals.

p-value<0.05.

DISCUSSION

The high prevalence of ED (76.5%) among CKD patients is compatible with published reports (4). The prevalence of ED among those who were aware of their CKD for less than 60 months was higher than that among subjects who were aware of their CKD for 61 months or more. The former group was 3.5 times more likely to have ED (p = 0.012; CI 1.4–14.489). These data may indicate greater clinical, metabolic, and inflammatory imbalances among those who were more recently aware of their CKD and consequently had shorter follow-up times, a condition that theoretically favors a higher prevalence of ED (4),. Therefore, this trend may also reflect a major public health issue, because these patients are likely to require specialized treatment. This study found a 93.6% ED prevalence rate among 31 patients with diabetes mellitus as a cause of their CKD, compared with a 66% ED prevalence rate among non-diabetic subjects (p = 0.004). For those with diabetes mellitus as a comorbidity, the prevalence of ED was 93,5%, which is in agreement with the literature (3,4). Diabetic patients were 4.05 times more likely to have ED compared with non-diabetic subjects.

In conclusion, our study found a high prevalence rate of ED among CKD patients on conservative treatment. There was a strong association with diabetes mellitus, either as a cause of the renal disease or as a comorbidity, and disease duration. We understand that inflammation, which is common in these patients (6–8), may account for the high prevalence rate of ED in this study. The presence of inflammation may point to the possibility of an early diagnosis of a generalized endothelial disease that is amenable to screening at the first nephrological consultation through a simple but efficient clinical approach.

The utilization of 5-phosphodiesterase inhibitors represents a novel therapeutic approach used to improve endothelial function (10). When administered daily to CKD patients, this treatment can prevent or delay the development of kidney disease as a consequence of reduced inflammation in the endothelium.

AUTHOR CONTRIBUTIONS

Mesquita JFP was the researcher in charge of gathering and analyzing data as well as orienting students involved with this work; he is an expert on Brazilian healthcare. Ramos T and Mesquita FP are medical students from Faculdade de Medicina da Universidade Federal de Juiz de Fora who are in charge of interviewing patients and obtaining data. Netto JMB and Bastos MG are co-advisors on this study. Figueiredo AA is an advisor on this study.

ACKNOWLEDGMENTS

This study was supported by the IMEPEN Foundation (Instituto Mineiro de Ensino e Pesquisa em Nefrologia) through the efforts of physicians, nurses, social assistants, psychologists, nutritionists, and supporting staff.

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No potential conflict of interest was reported.

Copyright © 2012. CLINICS
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