E-ISSN : 2757-7163
Materials and Methods: Twenty-five patients who applied to the radiology clinic were included in the study. All patients have only hyperlipidemia as a risk factor of ED. The patients were evaluated in terms of ED by using International Index of Erectile Function (IIEF) form. Before and after oral treatment with daily doses of 10 mg atorvastatin, all parameters were measured. Paired t-test was used to compare vascular velocities between lipid profiles and Erectile Function Domain Scores (EFDS) and IIEFs, before and after treatment separately.
Results: Cholesterol levels of 96% of patients were higher than 200 mg/dl and 52% of them had abnormal penile Doppler ultrasonography (PDU) findings. Patients with abnormal PDU findings had lower cholesterol levels than those with normal PDU findings. Significant differences existed between patients with normal and abnormal PDU in the high triglyceride group as for pre-, and post-treatment values . Pre-, and post-treatment EFD and IIEF scores were comparable.
Conclusion: It can be said that a relationship exists between hyperlipidemia and erectile dysfunction. Therefore, lipid profile of a patient admitted with ED may be analyzed routinely
There is usually a multifactorial etiology. Many psychological, neurological, endocrinological, vascular, pharmacological, traumatic, iatrogenic factors have been described as etiologic factors. Potential risk factors are smoking, advanced age, alcohol addiction, hypertension, hyperlipidemia, diabetes mellitus (DM), depression, vascular diseases, some drugs and some surgical procedures and operations.
Penile erection is a complex physiologic and hemodynamic process that requires an intact arterial blood flow and a venocclusive mechanism in the corpus cavernosum. This process is related to the integration between central and peripheral nervous systems as well as the ratio of the trabecular smooth muscle to the connective tissue in the corpus cavernosum [2].
The most important and most common diagnostic test used in vascular ED is penile color Doppler ultrasonography (US). After an intracavernosal injection of a vasoactive substance (papaverine, prostaglandin E1, etc.), increase in penile artery diameter, blood flow velocity, systolic velocity and end-diastolic velocity can be measured and especially arterial and indirectly venous system can be evaluated in penile color Doppler US.
Penile erection is achieved thanks to adequate arterial distribution. The main cause of arteriolar insufficiency is atherosclerosis but it can also be caused by trauma or congenital anomalies. Atherosclerotic lesions are characterized by smooth muscle proliferation and accumulation of lipid in the vessel wall. Hypercholesterolemia, smoking, DM, exposure to radiation and perineal trauma are risk factors that can be associated with ED [3]. The presence of hypercholesterolemia increases lipid storage in vascular lesions, resulting in atherosclerosis and consequent blockage of blood flow.
Use of high-resolution ultrasonography and quantitative Doppler spectral analysis technique in the evaluation of vasculogenic ED was first described by Lue et al. in 1985 [4]. The cavernous artery exhibits very pronounced gray scale changes after injection of an intracavernosal vasoactive agent. The leading change among these alterations is the increase in arterial diameter. As reported in many studies, the expected increase in the diameter of cavernous arteries varies between 70-100% [5]. Measurements of maximal systolic velocity (MSV), end- diastolic velocity (EDV), acceleration (A), acceleration time (AT) and resistive index (RI) (RI= MSV-EDV / MSV) have been used to demonstrate the hemodynamic status of the cavernous artery.
Post-injection MSV measurement in arteriogenic ED are the most commonly used parameter in assessing arterial insufficiency. Collins and Lewandowski found average MSV as 26.8 cm/sec in patients responding to intracavernous papaverine injection [6]. Most of the studies have accepted MSV values above 30-40 cm/sec as normal [7–10].
In cases of venogenic ED excessive venous leakage occurs from corpus cavernosum, In a patient with increased diastolic velocity, venocclusive mechanism is presumably insufficient. The EDV value, which can be considered significant for the assessment of venous leakage, has been reported to be over 5 cm/sec in many studies [8,11].
The aim of this study is to compare PDU, IIEF, EFDS results before and after atorvastatin treatment in hyperlipidemic patients with ED.
Threshold levels of total cholesterol (200≤ mg/dl), and triglyceride (179≤ mg/dl) were as indicated. The patients whose cholesterol or triglyceride values were higher than the determined levels were evaluated as hyperlipidemic cases.
The patients were also evaluated in terms of erectile function. IIEF form which was validated by Turkish Andrology Association, was used in face to face interview sessions. By this means, EFD and IIEF scores were estimated for each patients. Sum of the scores obtained from all questions in the IIEF form was accepted as the IIEF score, and the total score of the 1,2,3,4,5 and 15 questions as the EFD score.
After intracavernosal injecting 60 mg papaverine HCl, all patients underwent Doppler US at 0, 5th, 10th, 15th and 30th minutes, and MSV and EDV values were estimated for each patient. MSV of ≥ 30cm/sec and EDV of ≥ 5 cm/sec were evaluated as normal threshold values . The patients with MSVs, and EDVs lower than these threshold values were evaluated as having arterial failure and venocclusive deficiency, respectively.
Erectile response was evaluated as below:
Grade 0: No erectile response
Grade 1: Elongation in penile shaft
Grade 2: Mild tumescence
Grade 3: Enough tumescence and erection angle is less than 90 degrees
Grade 4: Enough tumescence and erection angle is greater than 90 degrees (rigid erection)
After oral 10 mg atorvastatin treatment for a month, all parameters were measured again. Paired -t test was used to make comparisons between vascular velocities, lipid profiles, EFDS and IIEF, before and after treatment separately. For statistical analysis IBM SPSS Statistics v25 software is used.
Cholesterol levels of 96% of the patients were higher than 200 mg/dl and 52% of them had abnormal PDU findings. Interestingly, patients with abnormal PDU findings had lower cholesterol levels than those with normal PDU resuls, without significant differences between these patients (p>0.05) (Table 1). Even so, both groups responded to the treatment perfectly.
Ninety-seven percent of the patients had higher triglyceride levels, and as is the case with hypercholesterolemia patients 52% of the patients had abnormal PDU findings. Before treatment there was a significant difference between the groups (p<0.05). They significantly responded to the treatment (Table 2).
Both EFD and IIEF scores were similar before treatment, in both patient groups with normal and abnormal PDUs. However, atorvastatin treatment improved their erectile functions (Table 3-4).
Rogers JH and Kaiser FE, emphasized the similar changes in the vessels of ED patients with coronary artery disease and/or hyperlipidemia. Similar obstructive lesions starting from the aortic bifurcation to the distal internal pudendal artery were more common. Hyperlipidemia and its resultant macrosvascular atherosclerosis were also more frequent in patients with ED [17,18]. Gholami SS et al. determined that a high fat diet causes ED with accompanying neurological and vascular changes in hypercholesterolemic rats. All rats had less nerve content and endothelial cells but higher smooth muscle cells than rats with normal cholesterol levels. In rats treated with colosterol plus phosphate buffered saline electron microscopy showed; denuded andothelial lining of sinusoids covered by multiple platelets, hypermyelination and severe atrophy of axons, a significant decrease in the number and size of nonmyelinated axons, dysregulation of smooth muscle cells with insufficient myofilaments and foamy cytoplasm. [19]. Li R et al. investigated this issue in 14 rats. They found decreased smooth muscle/collagen ratio, increased fibrosis, increased apoptosis and decreased autophagy in penile tissue of hyperlipidemic rats in as little as six months. As a conclusion they said that hyperlipidemia might decrease erectile function in rats by causing cavernosal fibrosis [20]. Qiu X et al. showed reduced nitric oxide synthase (nNOS) positive nerves, reduced endothelium, and increased cavernous smooth muscle in penile tissues of hyperlipidemic rats. They interpreted the results and associated the mechanism of ED with, decreased number of nNOS-positive nerves and an attenuated endothelium all of which can adversely affect erectile function due to reduced bioavailability of nitric oxide. They also added that the attenuated endothelium causes smooth muscle to lose their contractile ability as the cells become synthetic. According to this study, both structural changes could possibly explain why men with hyperlipidemia, have higher risk of ED [21]. Kobat M et al. stated that , in men without coronary artery disease, circulating soluble oxidized low-density lipoprotein receptor levels play a role in oxidized LDL-induced damage, which is associated with ED [22].
Both statistical frequency and the above-mentioned literature above make hyperlipidemia important for the ED etiology. Now, we have some relevant histopathologic and laboratory data. Some structural changes that diminish the elasticity of penil micro tissue and structural and/or physiologic deficits of neurons seem responsible for the lack of erection.
We aimed to investigate the correlation between the lipid profile and penile vascular Doppler US findings of ED patients. In our results, we were not able to find any effect of total cholesterol level on ED. However, Saltzman et al. administrated atorvastatin treatment to ED patients, and decrease in lipid levels occurred, the patients improved and showed a good dissese progression [23]. In addition, Wei M et al. calculated that each 1 mmol/L increase in total cholesterol levelss was associated with 1.32-fold greater risk of ED. Likewise, every 1 mmol/L decrease in high-density lipoprotein levels resulted in a 2.6-fold increase in ED risk [24]. Discordance of our results with the literature may be related with our lower patient counts. It is hard to say "there is no relation between total cholesterol level and ED development" before performing a similar study in a larger group.
In our study triglyceride levels, were significantly higher among the patients with abnormal PDU findings. In the literature, the main trend is accepting risk factors of triglyceride and coronary artery disease (CAD) as predictors of ED. In a study on 3390 male participants, Corona G et al. found that high triglyceride levels were related with ED [25]. Atahan et al. determined that lipoprotein A and triglyceride levels were higher in both peripheral and cavernosal samples of vasculogenic ED group than in non-vasculogenic ED group. However, there weren"t any significant differences in other groups [26]. Kim SC et al. found that low- density lipoprotein (LDL) was higher in ED patients, however, triglyceride and cholesterol levels didn"t significantly change [27]. Pinnock et al. interpreted high cholesterol and triglyceride levels as the predictor of ED [28]. So, increased triglyceride levels in our study are correlated with the literature data. Also, response of the patients to the atorvastatin treatment, supports that triglyceride and cholesterol levels are related to ED. Both in normal and abnormal PDU groups, there was significant resolution of symptoms after atorvastatin treatment. EFD and IIEF scores were significantly elevated. However, in recent studies long- term statin usage has been held responsible for ED as a result of decreased testosterone levels in hyperlipidemic patients. Corona et al. determined in statin users that testosterone levels were getting lower while follicle stimulating hormone levels were getting higher. They presumed that statin usage might trigger primary hypogonadism and they suggested the clinicians should query the ED patients with low testosterone levels, in terms of statin usage [29]. In contrast, Mondul AM et al. could not determine any negative effect of statin usage on serum sex steroid levels [30]. Further studies are needed to reveal this issue.
Ethics Committee Approval: The study was approved by Ankara Numune Training and Research Hospital Ethical Committee, Cankaya, Ankara, Turkey.
Informed Consent: An informed consent was obtained from all the patients.
Publication: The results of the study were not published in full or in part in form of abstracts.
Peer-review: Externally peer-reviewed.
Authorship Contributions: Any contribution was not made by any individual not listed as an author. Concept – M.T., U.O., M.C., H.A.; Design – M.T., U.O., M.C., H.A.; Supervision – M.T., U.O., M.C., H.A.; Resources – M.T., U.O., M.C., H.A.; Materials – M.T., U.O., M.C., H.A.; Data Collection and/or Processing – M.T., U.O., M.C., H.A.; Analysis and/or Interpretation – M.T., U.O., M.C., H.A.; Literature Search – M.T., U.O., M.C., H.A.; Writing Manuscript – M.T., U.O., M.C., H.A.; Critical Review – M.T., U.O., M.C., H.A.
Conflict of Interest: The authors declare that they have no conflict of interest.
Financial Disclosure: The authors have declared that they did not receive any financial support for the realization of this study.
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