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From the * Department of Andrology, Mansoura
University, Mansoura, Egypt; and the
Department of Urology, University of Illinois
at Chicago, Chicago, Illinois.
| Correspondence to: Dr Craig Niederberger, Department of Urology, University of Illinois at Chicago, 515 CSN M/C 955, 840 S Wood St, Chicago, IL 60612 (e-mail: craign{at}uic.edu). |
| Received for publication May 5, 2004; accepted for publication July 6, 2004. |
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Abstract |
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 Top Abstract Patients and MethodsResultsDiscussionConclusionsReferences |
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Key words: Smoking, impotence, color duplex, pharmacocavernosometry, veno-occlusion
In a study of 1290 noninstitutionalized men aged 40–70 years old, impotence was complete in 11% of smokers and only 0.3% of nonsmokers (Feldman et al, 1994). In another study including 4462 Vietnam-era army veterans aged 31–49 years, ED was found in 2.2% of nonsmokers, 2.0% of ex-smokers, and 3.7% of current smokers (Mannino et al, 1994). The authors also found that ED was independent of the number of cigarettes smoked per day and the number of years of smoking. Condra et al (1986) reported that the incidence of ED among heavy smokers is twice that in the general population. In their study on 2010 men, Mirone et al (2002) concluded that the risk of ED is influenced by smoking and that the duration of the habit increases the risk. In a literature review of 18 studies, Dorey (2001) found a detrimental effect of smoking on erectile function and a 1.5 times more likely chance for smokers to suffer ED than nonsmokers.
Studies that investigated the mechanisms through which cigarette smoking causes ED have suggested that tobacco-induced ED is mainly a result of vasculogenic etiology. Rosen et al (1991) proposed that cigarette smoking is an independent risk factor in the development of atherosclerotic lesions in the internal pudendal and common penile arteries of young impotent men. Inhalation of cigarette smoke was found to inhibit smooth muscle relaxation and impair the release of neurovascular mediators (Jeremy et al, 1986). Another report indicated that smoking increases platelet aggregation, inducing catecholamines, and that nicotine and carbon monoxide have a direct toxic effect on vascular endothelium (Bornman and du-Plessis, 1986). Nicotine was also found to interfere with erectile response to the intracavernous injection of vasoactive drugs (Glina et al, 1988). In a comprehensive literature review, McVary et al (2001) posited that clinical and basic science studies provide indirect strong evidence that smoking affects penile erection by impairment of endothelium-dependent smooth muscle relaxation.
Our study was designed to determine the hemodynamic mechanisms through which cigarette smoking, as an independent risk factor, induces ED. The evaluation of the differential effect of cigarette smoking on the arterial and venous components of penile vasculature can be used to localize the pathophysiology of vasculogenic ED in smokers, thus adding to a better understanding of this problem.
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Patients and Methods |
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TopAbstractPatients and MethodsResultsDiscussionConclusionsReferences |
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Nocturnal Penile Tumescence and Rigidity Monitoring
Nocturnal penile tumescence and rigidity (NPTR) monitoring in this study
was performed (1–3 nights) in the sleep unit of the medical center with
the use of the Rigiscan device (Dacomed Corporation, Minneapolis, Minn). To
ensure a restful night's sleep, the patient was asked to avoid napping,
alcohol, and caffeine and to evacuate bladder and bowel prior to going to
sleep. Data were collected each morning. The following criteria were
considered normal: at least 1 nocturnal erection with at least a 2-cm change
in tip circumference and a 3-cm or greater change in base circumference. Also
required for normalcy was a rigidity measurement of at least 70% at tip and
base and duration of greater than 10 minutes.
Pharmacopenile Doppler Ultrasonography
We used a Toshiba color duplex ultrasound unit with a 7 MHz linear
transducer. Each examination commenced with a general penile evaluation for
corporal fibrosis, Peyronie plaques, and bilateral cavernosal artery diameter
(CAD). Next, we performed intracavernosal injection (ICI) with 1 mL of Trimix
(papaverine, prostaglandin E1 [PGE1], and phentolamine combined so that each 1
mL of mixture contained 15 mg papaverine, 5 µg PGE1, and 0.5 mg
phentolamine). Patients with suspected venous leak had a tourniquet placed for
2 minutes around the base of the penis prior to the ICI. The patients were
scanned at 5-minute interval post-ICI to record internal diameters and Doppler
waveforms of the right and left cavernosal arteries. Values for maximal peak
systolic velocity (PSV) and end diastolic velocity (EDV) were obtained for
both arteries during maximal clinical response. Resistive index (RI) was
calculated for each patient by the following formula:
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Redosing Pharmacocavernosometry
In redosing, complete cavernous smooth muscle relaxation was indicated by
demonstration of a linear relationship between the maintenance flow and the
intracorporeal pressure (ICP). If this linear relationship was not
demonstrated in the first redosing pharmacocavernosometry (RPC) setting, we
performed 1 or 2 further measurements with a higher dose of Trimix. Repeated
RPC measurements were separated by 1-week intervals. Briefly, a 21-G butterfly
needle attached to the Cavomat-7000 Device (Weist Medizintechnik, GMBH Munch,
Germany) was inserted into 1 corpora cavernosum. Inserted into the other
corpora cavernosum was a 19-G butterfly needle attached to an automatic saline
infusion pump. The penis was then injected with 1 mL of Trimix. Five minutes
later, saline infusion began and was increased gradually until a predefined
baseline erect ICP of 90 mm Hg was reached. The flow required to achieve this
initial erection ICP was defined as the induction flow (IF). The flow required
to maintain the initial ICP was defined as the maintenance flow (MF).
Different MFs were then calculated at different pressures until a steady MF at
an ICP of 150 mm Hg was obtained. Pressure loss (PL) was calculated by the
following formula: PL = (150 mm Hg) - (ICP reached 30 seconds after flow
arrest)/30. Under the above conditions of complete cavernous smooth muscle
relaxation, we considered the following RPC criteria as indicative of
incompetent penile veno-occlusion: an IF > 30 mL/min, a MF > 5 mL/min,
and a PL > 1.5 mm Hg/s.
Statistical Methods
Statistical comparisons between groups were made with Student's t
tests. P < .05 was considered statistically significant. To
quantify the relative strength of each variable and to determine which
diagnostic parameter was most affected by cigarette smoking, we calculated the
receiver operating characteristic (ROC) curve areas for each variable with
smoking as the outcome. Diagnostic variables more affected by smoking would
thus display an area under the curve (AUC) closer to 1.0. In addition, we have
used the most significant variates from the Wald test of the beta weights to
build a model for the prediction of smoking.
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Results |
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TopAbstractPatients and MethodsResultsDiscussionConclusionsReferences |
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NPTR Results
All patients were monitored with Rigiscan for 3 nights, except those with
normal NPTR results in the first or second nights. We considered the patient
as having normal NPTR if he had at least 1 episode of nocturnal erection of at
least 10 minutes duration with a 2-cm increase in tumescence of the tip and
3-cm increase in tumescence of the base, together with 70% rigidity in the tip
and base. According to the above criteria, 61 patients (86%) in the smoker
group had abnormal NPTR compared with only 21 patients (55%) in the nonsmoker
group (Table 1). The average
base and tip tumescence in the smoker and nonsmoker groups
(Table 2) was 2.17 vs 2.83 cm
and 1.34 vs 1.78 cm, respectively, and the difference was significant for the
base and tip (P = .01). Average penile rigidity
(Table 2) was 45.7 vs 58.6% for
the base and 44.1 vs 55.9% for the tip; again, the difference was
statistically significant (P < .05).
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PPDU Results
We considered PSV < 25 cm/s and RI < 0.9 as abnormal. In the smoking
group, 36 patients (51%) had abnormal PSV compared with 42% in the nonsmoking
group. On calculating the RI, 58 patients (82%) had RI < 0.9 between
smokers compared with 39% of nonsmokers
(Table 1). The average PSV
(indicator of arterial perfusion) in the smoking group was 26.8 cm/s compared
with 31.2 cm/s in the nonsmokers, and the difference was not found to be
statistically significant (P = .19;
Table 2). Another indicator of
penile arterial perfusion is the percent change in the cavernosal artery after
ICI. This percentage was 77.2 vs 86.3% for the smokers and nonsmokers,
respectively; again, the difference was not found to be statistically
significant (P = .14). The RI (indicator of competence of penile
veno-occlusion) was 0.62 for smokers and 0.78 for nonsmokers, and the
difference was significant (P = .001;
Table 2).
RPC Results
We considered MF > 5 mL/min as an indication of disturbed penile
veno-occlusive mechanisms. The average MF among smokers was 20.9 mL/min
compared with 11.7 mL/min among nonsmokers, and the difference was
statistically significant (P = .001;
Table 2). In the smoker group,
63 patients (89%) had an abnormal MF compared with 18 patients (47%) in the
nonsmoker group (Table 1).
ROC Curve Analysis
Using smoking as the outcome, we calculated the AUC for each diagnostic
parameter in order to quantify its strength in relation to smoking
(Table 3). The AUC for those
parameters reflecting venous integrity, namely the MF and RI, was 0.77 and
0.74, respectively, compared with 0.58 for the PSV, which reflects the
integrity of the arterial side. The ROC for the linear regression model with
the use of the 4 most significant variates (base rigidity, tip rigidity, RI,
MF) as input features was 0.857.
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Discussion |
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TopAbstractPatients and MethodsResultsDiscussionConclusionsReferences |
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We used the Rigiscan device to monitor NPTR in our patients to investigate the organic nature of ED in smokers. In the smoking group, only 86% of our patients had abnormal NPTR compared with 55% in the nonsmoking group (Table 1). Of note, the average base rigidity was 45.7% and 58.6% in the smoking and nonsmoking groups, respectively (P < .05; Table 2). Moreover, on performing ROC curve analysis with smoking as the outcome, the AUC value for base rigidity was 0.79 (Table 3). These NPTR figures suggest an organic etiology underlying ED in cigarette smokers. Impairment of NPTR in cigarette smokers was previously reported by Hirshkowitz et al (1992), who indicated that penile rigidity during nocturnal erections was inversely correlated with the number of cigarettes smoked per day. The organic nature of ED in cigarette smoking was also reported by Xie et al (1997), Jeremy and Mikhailidis (1998), and Tan and Philip (1999).
Numerous previous studies have indicated that ED in smokers is mainly due to underlying vascular pathology. Chronic smoking in the rat was found to produce age-independent moderate hypertension and considerable decreases in penile nitric oxide synthetase activity (Xie et al, 1997). Cigarette smoking was determined to be an independent risk factor in the development of atherosclerotic lesions in the internal pudendal and common penile arteries of young impotent men (Rosen et al, 1991). Purvis et al (1996) demonstrated a correlation between the response to intracorporeal injection of PGE1 and tobacco consumption. Another study showed that inhalation of cigarette smoke inhibits smooth muscle relaxation and impairs the release of neurovascular mediators (Jeremy et al, 1986). Using echo-Doppler and ICI, Vidal-Moreno et al (1996) studied the effect of tobacco on penile vascularization and concluded that cigarette smoking causes ED from vascular damage that is as severe as the damage caused by other factors like arteriosclerosis, diabetes, or hypertension. One report indicated that smoking increases platelet aggregation and induces catecholamines and that nicotine and carbon monoxide has a direct toxic effect on vascular endothelium (Bornman and du-Plessis, 1986).
Most previous studies thus demonstrated a strong link between vascular involvement and the development of ED in smokers. However, most of these studies did not indicate whether the arterial or the venous compartment is more involved in tobacco-induced ED. The unique feature of our trial is that we not only investigated the arterial supply of the penis, but we also studied venous drainage by both PPDU and RPC. To make a pathophysiologic distinction, we calculated ROC curve area to quantify the relative strength of the PSV as an indicator of arterial integrity and of both the RI and MF as indicators of competence of the veno-occlusive system.
Interestingly, the difference in the average PSV between the smoking and the nonsmoking groups was not statistically significant (P = .19), whereas the average MF was significantly higher in the smoking group. This result signifies that MF (indicator of venous involvement) is more impaired by smoking than the PSV (indicator of arterial involvement). These results might be explained by the lower average age in our smoking group (44.3 years) compared with that of ED smokers in most other studies. It could be speculated that impairment of venous drainage plays a more significant role in younger ED patients because smoking-induced atherosclerotic changes affecting the arterial system develop over a longer period. The clinical significance of base and tip rigidity, RI, and MF is underscored by the high ROC produced by a logistic regression model that used these parameters as input features.
To our knowledge, this study is the first to investigate the venous system in smokers with the use of the redosing technique of pharmacocavernosometry. Many previous studies indicated that smoking is a cause for penile arterial insufficiency. For example, smoking was shown to decrease the intracavernosal pressure and penile brachial index (Condra et al, 1986; Glina et al, 1988; Morales et al, 1998). Other studies have shown that smoking predisposes men to premature atherosclerosis in the internal pudendal, common penile, and cavernosal arteries (Forsberg et al, 1989; Rosen et al, 1991). Degenerative changes in the corpus cavernosum of smokers was reported by Mersdorf et al (1991). A later ultrastructural study demonstrated a statistically significant reduction in the amount of corporeal smooth muscle, endothelial cells, and elastic fibers in smokers compared with nonsmokers (Yaman et al, 2003). None of these studies investigated the venous system of impotent smokers, which, as evident from our results, is highly involved in the development of ED.
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Conclusions |
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TopAbstractPatients and MethodsResultsDiscussionConclusionsReferences |
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References |
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TopAbstractPatients and MethodsResultsDiscussionConclusionsReferences |
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Condra M, Morales A, Owen J, Surridge D, Fenemore J. Prevalence and significance of tobacco smoking in impotence. Urology. 1986; 6: 495 -499.
Dorey G. Is smoking a cause of erectile dysfunction? A literature review. Br J Nurs. 2001; 10: 455 -465.[Medline]
Feldman H, Goldsein I, Hatzichristou D, Krane R, McKinlay J. Impotence and its medical and psychological correlates: results of the Massachusetts male aging study. J Urol. 1994; 151: 54 -61.[Medline]
Forsberg L, Hederstrom E, Olsson AM. Severe arterial insuffiency in impotence confirmed with an improved angiographic technique: the impact on smoking and other etiologic factors. Eur Urol. 1989; 16: 357 -360.[Medline]
Glina S, Reichelt A, Puech Leao P, Marcondes dos Reis J. Impact of cigarette smoking on papaverine-induced erection. J Urol. 1988;140: 523 -524.[Medline]
Gray RR, Keresteci AG, Louis El, Grossman H, Jewette MS, Rankin JT,
Provan JL. Investigation of impotence by internal pudendal angiography:
experience with 73 cases. Radiology. 1982; 144: 773
-776.
Hirshkowitz M, Karacan I, Howell JW, Arcasoy MO, Williams RL. Nocturnal penile tumescence in cigarette smokers with erectile dysfunction. Urology. 1992;39: 101 -107.[Medline]
Jeremy J, Mikhailidis D. Smoking and erectile dysfunction. J R Soc Health. 1998; 118: 151 -155.[Medline]
Jeremy J, Mikhailidis D, Thompson C, Dandona P. The effect of cigarette smoke and diabetes mellitus on muscarinic stimulation of prostacyclin synthesis by rat penis. Diabetes Res. 1986; 3: 467 -452.[Medline]
Juenemann K, Lue T, Luo J, Benowitz N, Abozeid M, Tanagho E. The effect of cigarette smoking on penile erection. J Urol. 1987;138: 438 -441.[Medline]
Mannino D, Klevens R, Flanders W. Cigarette smoking: an independent
risk factor for impotence. Am J Epidemiol. 1994; 140: 1003
-1008.
McVary KT, Carrier S, Wessells H. Smoking and erectile dysfunction: evidence based analysis. J Urol. 2001; 166: 1624 -1632.[Medline]
Mersdorf A, Goldsmith PC, Diedrichs W, Paulda CA, Lue TF, Fishman IJ, Tanagho EA. Ultrastructural changes in impotent penile tissue: a comparison of 65 patients. J Urol. 1991; 145: 749 -758.[Medline]
Mirone V, Imbimbo C, Bortolotti A, Di Cintio E, Lndoni M, Lavezzari M, Parazzini F. Cigarette smoking as risk factor for erectile dysfunction: results from an Italian epidemiological study. Eur Urol. 2002; 41: 294 -297.[Medline]
Morales JC, Lemourt OM, Perez RJ. Arterial risk factors in sexual impotence. Arch Esp Urol. 1998; 42: 905 -909.
Purvis K, Brekke I, Christiansen E. Determinants of satisfactory rigidty after ICI with PGE1 in men with erectile failure. Int J Impot Res. 1996;8: 9 -16.[Medline]
Rosen M, Greenfield A, Walker T, Grant P, Dubrow J, Bettman M, Fried L, Goldstein I. Cigarette smoking: an independent risk factor for atherosclerosis in the hypogastric-cavernous arterial bed of men with arteriogenic impotence. J Urol. 1991; 145: 759 -763.[Medline]
Safarinejad MR. Prevalence and risk factors for erectile dysfunction in a population-based study in Iran. Int J Impot Res. 2003;15: 246 -252.[Medline]
Shabsigh R, Fishman IJ, Schum C, Dunn JK. Cigarette smoking and other risk factors in vasculogenic impotence. Urology. 1991; 38: 227 -231.[Medline]
Tan RS, Philip PS. Perceptions of and risk factors for andropause. Arch Androl. 1999; 43: 227 -233.[Medline]
Vidal-Moreno JF, Moreno Pardo B, Jimeneze Cruz JF. Assessment of tobacco impact on penile vascularisation with echo-Doppler and intracavernous injection. Actas Urol Esp. 1996; 20: 365 -371.[Medline]
Virag R, Bouilly P, Frydman D. Is impotence an arterial disorder? A study of arterial risk factors in 440 impotent men. Lancet. 1985;26: 181 -184.
Xie Y, Garban H, Ng C, Rajfer J, Gonzalez-Cadavid NF. Effect of long term passive smoking on erectile dysfunction and penile nitric oxide synthetase. J Urol. 1997; 157: 1121 -1126.[Medline]
Yaman O, Yilmaz E, Bozlu M, Anafarta K. Alteration of intracorporeal structures in patients with erectile dysfunction. Urol Int. 2003;71: 87 -90.[Medline]
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