Erectile dysfunction (ED) is defined as the consistent or recurrent
inability of a man to attain and /or maintain a penile erection sufficient for sexual activity. Sexual health and function are important determinants of quality of life (QoL). ED and female sexual dysfunction (FSD) are increasingly becoming more important because of an ageing population and newer therapies. As this subject is discussed widely in the media, men and women are seeking guidance. Successful treatment of ED has been demonstrated to improve intimacy, satisfaction, and the sexual aspect of QoL, and relieve symptoms of depression. While in the past ED was a disease treated exclusively by specialists, it has now become a common problem seen by most general practitioners. The rapid developments in the treatment of ED have emphasised the importance of continuing medical education. This concise update on the topic is designed to meet this challenge. Although this article focuses primarily on ED in men, one must remember that one's sexual partner plays an integral role; hence discussion of any intervention should include both partners. Incidence Sexual dysfunction is highly prevalent in men and women. In the Massachusetts Male Aging Study (MMAS), a community-based survey of 1 209 men aged 40-70 years, 52% of the responders reported some degree of erectile difficulty (Fig. 1). Seventeen per cent had mild, 25% moderate and 10% severe ED, with no nocturnal erection and total inability to obtain or maintain an erection during sexual stimulation. In the National Health and Social Life Survey, a nationally representative probability sample of men and women aged 18-59 years, 10.4% of men reported complete ED (similar to the MMAS result (Fig. 2)). Both studies noted a strong correlation between ED and advancing age. Other male sexual dysfunctions, such as premature ejaculation (28.5%) and hypoactive sexual desire (15.8%), were reported in the National Health and Social Life Survey. An additional 17% reported anxiety about sexual performance, and 8% had a lack of pleasure in sex. Long-term predictions based on an ageing population and an increase in risk factors suggest a large increase in the number of men with ED. Also, the prevalence of ED is underestimated because physicians frequently do not question their patients about this disorder. Physiology It is worthwhile first considering the underlying mechanism of normal erection and the pathophysiology of ED. Erection involves the nervous system, vascular system and hormones. The nervous system involves the central, peripheral, sympathetic and parasympathetic nervous systems. Higher centres in the brain, such as the hypothalamus and the limbic system, play an important role in the integration and control of reproductive and sexual functions. Erection occurs in response to tactile, olfactory and audiovisual stimuli. The afferent information is assessed in the forebrain and relayed to the hypothalamus. The efferent pathways from the hypothalamus enter the medial forebrain bundle and project caudally near the lateral part of the substantia nigra into the midbrain tegmental region. It is then conveyed through the dorsal spinal columns to thoracolumbar (sympathetic T11, 12; L1, 2) and sacral autonomic (parasympathetic S2, 3, 4) nuclei. The primary nerve fibres to the penis originate in the dorsal nerve of the penis a branch of the pudendal nerve. This nerve originates from the Onuf nucleus (S2, 3, 4), and forms part of the somatic peripheral nervous system primarily responsible for the sensation from the genitalia and the contraction of bulbocavernosus and ischiocavernosus muscles necessary for a rigid erection. The cavernous nerve of the penis is the other nerve that carries both the nerve of erection (parasympathetic) and the nerve of detumescence (sympathetic). They travel posterolaterally along the prostate and enter the corpora cavernosa and corpus spongiosum by piercing the urogenital diaphragm about 5 mm lateral to the urethral sphincter. They can be damaged during any pelvic or perineal surgery. Sexual stimulation causes the release of neurotransmitters from the cavernous nerve endings and sinusoidal endothelial cells that lead to relaxation of penile smooth muscles and cause erection. The neurotransmitter involved in erection is called nitric oxide (NO) and is formed by the non-adrenergic non-cholinergic (NANC) nerve and endothelial cells. The cholinergic nerve stimulates endothelial cells to form NO and contribute to erection. NO is produced from arginine with the help of the enzyme nitric oxide synthetase (NOS). This, in turn, produces other muscle-relaxing chemicals such as cGMP, which results in the relaxation of smooth muscle of the erectile tissue, producing a dramatic increase in penile blood flow and thus erection (Fig. 3). Erection is maintained as penile venous leak is markedly reduced. This occurs as the venules beneath the rigid tunica albuginea are compressed, resulting in near-total occlusion of venous outflow (Fig. 4). [FIGURE 3 OMITTED] [FIGURE 4 OMITTED] Additional sexual stimulation initiates the bulbocavernous reflex where ischiocavernous muscles forcefully compress the base of the blood-filled corpora cavernosa. At this pressure both the inflow and outflow of blood temporarily cease, causing further rigid erection. Detumescence results from the cessation of neurotransmitter release, breakdown of second messengers (cGMP, cAMP) by PDE-5 (phosphodiesterases), and sympathetic nerve excitation during ejaculation. Contraction of the trabecular smooth muscle reopens the venous channels, allowing the blood to be expelled, which results in flaccidity or detumescence. Pathophysiology and causes of ED ED is essentially a vascular disease, although the aetiology is usually multifactorial. It can be stratified into organic and psychogenic impotence, but most men with organic ED usually have an associated psychogenic component. Many diseases may affect erectile function by altering the nervous, vascular or hormonal systems. Various diseases may produce changes in the smooth muscle tissue of the corpora cavernosa or influence the patient's psychological mood and behaviour. Pure psychogenic ED is an uncommon disorder, although most cases of ED were previously attributed to psychological factors. It is characterised objectively by the presence of good nocturnal and morning erections and negative findings from all other tests. Such men have a history of highly variable erections that can be totally absent on one day but virtually normal on the next day. Diseases associated with ED are summarised in Table I. Evaluation of ED Highly recommended * History directed at aetiology * International Index of Erectile Function (IIEF) (to measure the degree of ED--see Table II) * Physical examination directed at aetiology * Focused neurological examination for S2, 3, 4 reflex arc (anal tone, peri-anal sensation, bulbocavernosus reflex) Recommended * Fasting glucose/HbA1c * Lipid profile * Testosterone if clinically indicated (decreased libido, atrophic testes) Optional * Psychological/psychiatric consultation * Laboratory tests (prolactin, LH, TSH, FBC, urinalysis) Specialised * In-depth psychosexual and relationship evaluation * Psychiatric evaluation * Nocturnal penile tumescence and rigidity tests * Vascular imaging (arterial and venous) * Endocrine * Neurophysiological assessment. The IIEF-5 score is the sum of questions 1-5. The lowest score is 5 and the highest score 25, 22-25 (no ED), 17-21 (mild ED), 12-16 (mild-moderate ED), 8-11 (moderate ED) and 5-7 (severe ED). Management After all the information regarding the patient's status has been gathered, the various options can be discussed. This is best done in the presence of his partner. There are enough options available for every man who wants to be sexually active. Psychogenic ED Patients with obvious psychogenic ED are referred for psychotherapy. Organic ED The diagnosis and treatment of these patients must be goal directed and based on the expectations of the patient and his sexual partner. Other areas to consider are lifestyle changes such as regular exercise, no smoking, healthy diet, moderate alcohol consumption, etc. The patient's medication also needs to be reviewed and changed if it contributes to ED. Patients with organic ED have options, including: * Oral drugs * Vacuum device * Intracavernosal injection * Prosthesis * Reconstruction surgery. Oral drugs 5-phosphodiesterase inhibitors (PDE-5) Sildenafil (Viagra). This is the first oral agent to be well documented as an effective form of treatment. Since its introduction in March 1998, no other therapy for ED has achieved such prominent public recognition. The efficacy of sildenafil has been demonstrated by 21 randomised, double-blind, placebo-controlled studies of up to 6 months' duration, involving more than 3 000 men aged 20-87 years. The long-term efficacy has been shown Big Dick I Want in a 48-month, open-label, non-controlled, flexible-dose study. Sildenafil is a potent inhibitor of PDE5, the enzyme that acts in the corpora to break down cGMP mediated by the secondary neurotransmitter NO, which is primarily responsible for smooth muscle relaxation. This permits the development of an improved and sustainable erection. It has been demonstrated to improve erectile function in diabetic, hypertensive, post-prostatectomy, post-irradiation, spinal cord injury, geriatric and depressive patients. Safety concerns and adverse effects have been studied carefully. The most common are mild headache and upper GI distress which are self-limiting. It is a mild inhibitor of PDE-6 found in the retina, causing blue haze at the periphery of the field of vision, but is not dangerous. Anterior ischaemic optic neuropathy (unilateral blurred vision) has been reported. Sildenafil is absolutely contraindicated in patients taking nitrates (nitroglycerine or isosorbide) as it can potentiate the vasodilatory effect to dangerously low blood pressure levels. Exertion associated with sexual activity has been documented to increase the chances of ischaemic events in patients on nitrates. Co-administration of ketoconazole, erythromycin or cimetidine (CYP4503A4 inhibitor) increases its plasma concentration and rifampicin decreases it; therefore sildenafil requires dose adjustments. This is, however, a feature of all PDE-5 inhibitors. It is available in 3 doses: 25 mg, 50 mg and 100 mg. The starting dose depends on the severity of ED. The dose can be modified after at least 3 tries, although 5-6 tries are advised. It is recommended to take it on an empty stomach 30-60 minutes before sexual intercourse. Sexual stimulation (foreplay and/or audiovisual) is necessary to produce an erection. The half-life of sildenafil is 6-8 hours but the ability to obtain an erection may last up to 24 hours. To refractory patients (after 6 tries), benefit may be obtained by another PDE-5 inhibitor or combination with intracorporeal injection. Vardenafil (Levitra). Its mechanism of action is similar but 9 times more selective than that of sildenafil; it therefore needs a low dose. It is available in 5 mg, 10 mg and 20 mg. It has similar efficacy, side-effects and limitations as sildenafil but is less affected by food; however, a high-fat meal can inhibit absorption. Avoid co-administration with antiarrhythmic drugs that prolong the QT interval (quinidine, procainamide, amiodarone and sotalol). Caution is advised in hepatic impairment, as these patients may develop priapism. Tadalafil (Cialis). This is available in 5 mg, 10 mg and 20 mg doses. Tadalafil, even though chemically unrelated to sildenafil and vardenafil, has a similar mechanism of action, efficacy and side-effects. It has an extended period of responsiveness that can last 36 hours or longer in some men. It can also be ingested without food restriction. It has a PDE-11 effect and can cause back pain. Studies have shown that a single, small daily dose (2.5 mg) has a similar effect to an intermittent dose, which can eliminate the need for careful timing before intercourse. Yohimbine has been available for many years. It acts both centrally and peripherally, but its efficacy has been questioned as it has only done slightly better than placebo, even in well-controlled trials. There is renewed interest in combination therapy with sildenafil or some of the other oral agents. It is safe, with few adverse effects. The dosage is 1 tablet (6 mg) 3 times daily. However, it has limited effectiveness, with a success rate of only 20-25%. Fluoxetine (an SSRI) is effective in psychogenic ED and also helps in cases of premature ejaculatory disorder. The dosage is 20 mg 3 times daily for 4-6 weeks. Androgens This is an option in cases of severe hypogonadism. It improves the libido and overall sense of well-being. It is available in oral, injectable, gel and transdermal preparations. Oral therapy is the least effective, with a small risk of hepatotoxicity. Parenteral therapy will most likely restore testosterone levels, but it has to be injected periodically and is known to have symptomatic trough plasma levels and supernormal peak levels. To manage this, weekly lower doses are recommended. Skin patches deliver a sustained dose and are generally accepted by patients. Androgen creams (Androgel and Testim) are now available for daily topical use, minimising the peaks and trough side-effects of injectables. However, they need daily dosing and are relatively expensive. An elevated serum androgen level has the potential to stimulate prostate growth and there is a risk of activating latent cancer. Therefore periodic prostate examinations and follow-up PSA levels are recommended in all patients. Possible side-effects are fluid retention and liver damage. Others Apomorphine (Uprima), phentolamine (Vasomax), vasodilators (nitroglycerine), pentoxifylline (Trental), trazodone (Desyrel) and others have been tried alone and in combinations, with limited success. Injection therapy This is indicated if oral agents fail or are contraindicated. In 1993 alpha blockers, like papaverine, showed that an erection could be achieved when they were injected directly into the corpora cavernosa. Soon other vasodilators like prostaglandin E1 and phentolamine were introduced. Self injection of these agents, either alone or in combination, achieve erection in a wide variety of ED if the vasculature of the corpus cavernosa is healthy. These agents were available before the introduction of sildenafil and are still used by a select group of men. Alprostadil or Caverject (synthetic PGE1) is most commonly used in doses of 5-40 [micro]g. Papaverine (15-60 mg) and phentolamine (Regitine--mostly used in the combination Trimix preparation--dose of 0.2 mg) are also used. The main adverse effect is priapism or scarring at the injection site. Alprostadil is now available in a gel and a patch and cannot be used in patients on monoamine oxidase inhibitors (MAOIs). The injection technique is important. Vacuum constriction device (VCD) This is another option if first-line therapy fails. Negative pressure is created around the penis with the aid of a cylindrical appliance. This draws blood into the penis, which is trapped with the aid of a constriction ring. It is safe, painless and effective but needs manual dexterity. Adverse effects are mild and well tolerated. Penile implants At one time this was the only option available, but currently it is the last option even though 90% of men who have had the procedure would recommend the procedure to their friends and relatives. It is now considered in those in whom all therapies have failed. Two types, a semi-rigid and a multi-component inflatable system, are available. The semi-rigid prosthesis has two matching cylinders that are implanted into the corpora cavernosa, providing enough rigidity for penetration, and it rarely breaks. The disadvantages are that it stays semi-rigid all the time, requires surgery and the natural erectile mechanism is tampered with to implant the prosthesis. The inflatable devices consist of two silastic or bioflex cylinders inserted into the corpora cavernosa, a pump placed in the scrotum to inflate the cylinders, and a reservoir that is contained either within the cylinders or in a separate reservoir placed beneath the fascia of the lower abdomen. It stays functional for 7-10 years before replacement is necessary. Complications include infection, erosion and painful erection (very low incidences). The newer antibiotic-coated implants have a reduced infection rate. Patient acceptance of these devices is very high, with nearly 100% of patients expressing satisfaction. Reconstructive surgery A penile abnormality--like Peyronie's disease--can be referred for surgical correction. Vascular reconstruction restores natural erection when successful, but it is technically the most difficult surgery and only 50% of patients are potential candidates, e.g. those suffering from trauma and patients less than 30 years of age. Future The development of future medical options will emphasise the restoration of physiological function due to better understanding of the molecular biology of ED. Research involving gene therapy is already showing promise. Vascular endothelial growth factor (VEGF) is produced by vascular smooth muscle, and endothelial and inflammatory cells. It increases the production of NO, which improves endothelial function and blood flow in chronic ischaemic disorders. In animal models, direct intracavernosal injection of recombinant VEGF protein or adenoviral VEGF that contains plasmids has shown dramatic results based on cavernosography. Burchardt et al. identified VEGF 165 as the predominant isoform of the corpora cavernosa. Conclusion While oral PDE-5 inhibitors continue to be the first-line therapy for patients with ED, a significant number do not respond satisfactorily to these agents. Change of PDE-5 inhibitors, evaluation of hormone status, and patient counselling are the first efforts to salvage non-responders. Failure of these measures can be followed by combination pharmacological therapy, intracavernosal injection, a vacuum constriction device, or ultimately penile prosthesis implantation. By following a stepwise approach (see algorithm), the clinician can offer a satisfactory, effective, and safe treatment plan for the majority of men with ED. [ILLUSTRATION OMITTED] Further reading Akash R, Hrishikesh D, Amith P, Sabah S. Case report: association of combined nonarteritic anterior ischemic optic neuropathy (NAION) and obstruction of cilioretinal artery with overdose of Viagra. J Ocul Pharmacol Ther 2005; 21(4): 315-317. Andersson KE. Erectile physiological and pathophysiological pathways involved in erectile dysfunction. J Urol 2003; 170: S6-14.5. Andersson KE, Wagner G. Physiology of penile erection. Physiol Rev 1995; 75(1): 191-236. Baldwin K, Ginsberg P, Harkaway RC. Underreporting of erectile dysfunction among men with unrelated urologic conditions. Int J Impot Res 2003; 15(2): 87-89. Burchardt M, Burchardt T, Anastasiadis AG, et al. Application of angiogenic factors for therapy of erectile dysfunction: protein and DNA transfer of VEGF 165 into the rat penis. Urology 2005; 66(3): 665-670. Carson CC. What to do when initial PDE5 inhibitor therapy fails. Contemporary Urology 2006: 55-65. Christ GJ. The penis as a vascular organ. The importance of corporal smooth muscle tone in the control of erection. Urol Clin North Am 1995; 22(4): 727-745. Derby CA, Araujo AB, Johannes CB, et al. Measurement of erectile dysfunction in population-based studies: the use of a single question self-assessment in the Massachusetts Male Aging Study. Int J Impot Res 2000; 12(4): 197-204. Goldstein I, Lurie AL, Lubisich JP. Bicycle riding, perineal trauma, and erectile dysfunction: data and solutions. Curr Urol Rep 2007; 8(6): 491-497. Feldman HA, Goldstein I, Hatzichristou DG, et al. Impotence and its medical and psychosocial correlates: results of the Massachusetts Male Aging Study. J Urol 1994; 151(1): 54-61. Goldstein I, Lue TF, Padma-Nathan H, et al. Oral sildenafil in the treatment of erectile dysfunction. Sildenafil Study Group. N Engl J Med 1998; 338(20): 1397-1404. Goldstein I, Payton TR, Schechter PJ. A double-blind, placebo-controlled, efficacy and safety study of topical gel formulation of 1% alprostadil (Topiglan) for the in-office treatment of erectile dysfunction. Urology 2001; 57(2): 301-305. Heaton JP, Morales A, Adams MA, et al. Recovery of erectile function by the oral administration of apomorphine. Urology 1995; 45(2): 200-206. Laumann EO, Paik A, Rosen RC. Sexual dysfunction in the United States: prevalence and predictors. JAMA 1999; 281(6): 537-544. Lin CS, Ho HC, Chen KC, et al. Intracavernosal injection of vascular endothelial growth factor induces nitric oxide synthase isoforms. BJU Int 2002; 89(9): 955-960. McKenna KE. Central control of penile erection. Int J Impot Res 1998; 10 Suppl 1: S25-34. Morales A, Gingell C, Collins M, et al. Clinical safety of oral sildenafil citrate (VIAGRA) in the treatment of erectile dysfunction. Int J Impot Res 1998; 10(2): 69-74. Padma-nathan H, Eardley I, Kloner RA, et al. A 4-year update on the safety of sildenafil citrate (Viagra). Urology 2002; 60(2 Suppl 2): 67-90. Rosen RC, et al. Development and evaluation of an abridged, 5-item version of the international index of erectile function (IIEF-5) as a diagnostic tool for erectile dysfunction. Int J Impot Res 1999; 11: 319-326. Schmidt AC. Erectile function in the ageing male. CME 2001; 19(4): 230-234. Schmidt AC. Treatment of erectile dysfunction. The Specialist Forum 2003: 37-55. Williams G, Abbou CC, Amar ET, et al. Efficacy and safety of transurethral alprostadil therapy in men with erectile dysfunction. MUSE Study Group. Br J Urol 1998; 81(6): 889-894 SUNIL SINHA, FCS (Urol) (SA), FRCS (Glasg), HDip (Surg) (SA), MS (Gen Surg) (India), MB BS (India) Senior Specialist, Department of Urology, Groote Schuur Hospital, Cape Town Table I. Classification of ED A. Psychogenic: Depression, widower syndrome, performance anxiety, post-traumatic stress disorder B. Organic I. Vascular diseases: Atherosclerosis, peripheral vascular disease (PVD), myocardial infarction, hypertension, post-radiotherapy of pelvis, long-distance bicycle riders (perineal blood vessel and nerve trauma), drugs related to treatment of vascular disease II. Systemic disease: Diabetes mellitus, hypertension, dyslipidaemia, malignancy and its treatment, idiopathic haemochromatosis, scleroderma, renal failure, cirrhosis III. Neurological disease: Trauma, multiple sclerosis, Guillain-Barre syndrome, stroke, epilepsy, Alzheimer's disease IV. Endocrine disease: Hypogonadism, hypothyroidism, hyperthyroidism, hyperprolactinaemia V. Penile conditions: Peyronie's disease, priapism, epispadias, micropenis, trauma VI. Drugs: Antidepressants (tricyclic antidepressants, tranquillisers), antipsychotics, antihypertensives (thiazide diuretics, beta blockers, calcium-channel blockers, ACE inhibitors, alpha blockers--seldom), antiarrhythmics (digoxin), H2 blockers (cimetidine), antiandrogens (GnRH agonist, ketoconazole, spironolactone) 5-alpha reductase (finasteride), anticholesterol agents, recreational drugs (alcohol, marijuana, cocaine, heroine) VII. Surgery: Brain and spinal cord surgery, aortic surgery, abdomino-perineal resection of the rectum (APR), rectal surgery, prostatectomy VIII. Trauma: Fracture of the pelvis due to nerve and/or vascular damage IX. Radiotherapy Table II. International Index of Erectile Function-5 (IIEF-5)* Over the past 6 months 1 2 3 How do you rate your Very Low Moderate confidence that you low could get and keep an erection? When you had erections Almost Much About with sexual stimulation, never or less than half the how often were your never half the time erections hard enough time for penetration? During sexual inter- Almost Much About course, how often were never or less than half the you able to maintain your never half the time erection after you had time penetrated (entered) your partner? During sexual inter- Extremely Very Difficult course how difficult difficult difficult was it to maintain your erection to the completion of intercourse? When you attempted Much sexual intercourse, how Almost less than About out often was it never or half the half the satisfactory for you? never time time Over the past 6 months 4 5 How do you rate your High Very confidence that you high could get and keep an erection? When you had erections Much Almost with sexual stimulation, more always how often were your than half or erections hard enough the time always for penetration? During sexual inter- Much Almost course, how often were more always you able to maintain your than half or erection after you had the time always penetrated (entered) your partner? During sexual inter- Slightly Not course how difficult difficult difficult was it to maintain your erection to the completion of intercourse? When you attempted Much Almost sexual intercourse, how more always often was it than half or satisfactory for you? the time always * IIEF-5 is an abridged and slightly modified 5-item version of a 15-item IIEF designed for easy use by clinicians. Fig. 1. Prevalence of ED in the MMAS--a community-based survey. Men aged 40 to 70 years No erectile dysfunction (48%) Erectile dysfunction (52%) Complete (10%) Moderate (25%) Mild (17%) Note: Table made from pie chart. Fig. 2 Association between age and prevalence of ED--Mmas (N = 1 209). Complete Ed 40 39% 50 48% 60 57% 70 67% Data from Feldman et al, 1994 Note: Table made from bar graph. https://www.thefreelibrary.com/Erectiledysfunction.-a0204482258
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