Author
Abdul Traish
Bio: Abdul Traish is an academic researcher from Boston University. The author has contributed to research in topics: Androgen & Erectile dysfunction. The author has an hindex of 9, co-authored 14 publications receiving 1063 citations.
Papers
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Rutgers University1, Indiana University2, Cedars-Sinai Medical Center3, Monash University4, Royal Melbourne Hospital5, Boston Medical Center6, Lahey Hospital & Medical Center7, Columbia University8, Yale University9, McGill University10, George Washington University11, Prince Henry's Institute of Medical Research12, Harvard University13, Boston University14
TL;DR: A new definition of androgen insufficiency in women has been proposed along with consensus-based guidelines for clinical assessment and diagnosis and a simplified management algorithm for women with low androgen in the presence of clinical symptoms and normal estrogen status has also been proposed.
431 citations
TL;DR: This review focuses on the multidirectional impact of low testosterone associated with obesity and the metabolic syndrome and its effects on erectile dysfunction and CVD risk in men with type 2 diabetes.
Abstract: Men with obesity, the metabolic syndrome, and type 2 diabetes have low total and free testosterone and low sex hormone–binding globulin (SHBG). Conversely, the presence of low testosterone and/or SHBG predicts the development of metabolic syndrome and type 2 diabetes. Visceral adiposity present in men with low testosterone, the metabolic syndrome, and/or type 2 diabetes acts through proinflammatory factors. These inflammatory markers contribute to vascular endothelial dysfunction with adverse sequelae such as increased cardiovascular disease (CVD) risk and erectile dysfunction. This review focuses on the multidirectional impact of low testosterone associated with obesity and the metabolic syndrome and its effects on erectile dysfunction and CVD risk in men with type 2 diabetes. Whenever possible in this review, we will cite recent reports (after 2005) and meta-analyses.
### Epidemiological studies of low testosterone, obesity, metabolic status, and erectile dysfunction
Epidemiological studies support a bidirectional relationship between serum testosterone and obesity as well as between testosterone and the metabolic syndrome. Low serum total testosterone predicts the development of central obesity and accumulation of intra-abdominal fat (1–3). Also, low total and free testosterone and SHBG levels are associated with an increased risk of developing the metabolic syndrome, independent of age and obesity (1–3). Lowering serum T levels in older men with prostate cancer treated with androgen deprivation therapy increases body fat mass (4). Conversely, high BMI, central adiposity, and the metabolic syndrome are associated with and predict low serum total and to a lesser extent free testosterone and SHBG levels (1–3,5). Because obesity suppresses SHBG and as a result total testosterone concentrations, alterations in SHBG confound the relationship between testosterone and obesity.
Low total testosterone or SHBG levels are associated with type 2 diabetes, independent of age, race, obesity, and criteria for diagnosis of diabetes (6,7). In longitudinal studies, low serum total and free testosterone …
309 citations
TL;DR: It is shown that Hch and atherosclerosis-induced chronic cavernosal arterial insufficiency, beyond decreasing cavernosal perfusion pressure, also adversely affect smooth muscle relaxation mechanisms in cavernosal tissue.
85 citations
TL;DR: A global and integral understanding of the biologic aspects of female sexual function requires investigation of the vascular, neurologic (central and peripheral), and structural components of this extremely complex physiologic process.
82 citations
TL;DR: Digoxin associated alteration of human erectile function may be explained, in part, by inhibition of corporeal smooth muscle sodium pump activity, which promotes contraction and impedes nitric oxide induced relaxation.
62 citations
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TL;DR: The molecular and clinical under-standing of erectile function continues to gain ground at a particularly fast rate and the understanding of the nitric oxide pathway has aided not only in the molecular understand of the tumescence but also greatly in the therapy of erectILE dysfunction.
582 citations
TL;DR: The literature reviewed for this guideline straddles both empirical and pathophysiology-based eras, and some of the reported positive responses to treatment may reflect the natural course of priapism rather than a true treatment success.
539 citations
Journal Article•
TL;DR: Dopamine receptors in central nervous centers participating in the initiation of erection have been targeted for the treatment of ED, and Apomorphine, administered sublingually, is the first of such drugs.
Abstract: Erection is basically a spinal reflex that can be initiated by recruitment of penile afferents, but also by visual, olfactory, and imaginary stimuli. The reflex involves both autonomic and somatic efferents and is modulated by supraspinal influences. Several central transmitters involved in the erectile control have been identified. Dopamine, acetylcholine, nitric oxide (NO), and peptides, such as oxytocin and adrenocorticotropic/alpha-melanocyte-stimulating hormone, seem to have a facilitatory role, whereas serotonin may be either facilitatory or inhibitory, and enkephalins are inhibitory. Peripherally, the balance between contractant and relaxant factors controls the degree of contraction of the smooth muscle of the corpora cavernosa and determines the functional state of the penis. Noradrenaline contracts both corpus cavernosum and penile vessels via stimulation of alpha(1)-adrenoceptors. Neurogenic NO is considered the most important factor for relaxation of penile vessels and corpus cavernosum. The role of other mediators released from nerves or endothelium has not been definitely established. Erectile dysfunction (ED) may be due to inability of penile smooth muscles to relax. This inability can have multiple causes. However, patients with ED respond well to the pharmacological treatments that are currently available. The drugs used are able to substitute, partially or completely, the malfunctioning endogenous mechanisms that control penile erection. Most drugs have a direct action on penile tissue facilitating penile smooth muscle relaxation, including prostaglandin E(1), NO donors, phosphodiesterase inhibitors, and alpha-adrenoceptor antagonists. Dopamine receptors in central nervous centers participating in the initiation of erection have been targeted for the treatment of ED. Apomorphine, administered sublingually, is the first of such drugs.
524 citations
TL;DR: In this paper, a cross-sectional study of 1423 women aged 18 to 75 years, who were randomly recruited via the electoral roll in Victoria, Australia, from April 2002 to August 2003, was conducted to determine whether women with low self-reported sexual desire and sexual satisfaction are more likely to have low serum androgen levels than women without self-report low sexual desire or sexual satisfaction.
Abstract: ContextIt has been proposed that low sexual desire and sexual dysfunction are
associated with low blood testosterone levels in women. However, evidence
to support this is lacking.ObjectiveTo determine whether women with low self-reported sexual desire and
sexual satisfaction are more likely to have low serum androgen levels than
women without self-reported low sexual desire and sexual satisfaction.Design, Setting, and ParticipantsA community-based, cross-sectional study of 1423 women aged 18 to 75
years, who were randomly recruited via the electoral roll in Victoria, Australia,
from April 2002 to August 2003. Women were excluded from the analysis if they
took psychiatric medication, had abnormal thyroid function, documented polycystic
ovarian syndrome, or were younger than 45 years and using oral contraception.Main Outcome MeasuresDomain scores of the Profile of Female Sexual Function (PFSF) and serum
levels of total and free testosterone, androstenedione, and dehydroepiandrosterone
sulfate.ResultsA total of 1021 individuals were included in the final analysis. No
clinically significant relationships between having a low score for any PFSF
domain and having a low serum total or free testosterone or androstenedione
level was demonstrated. A low domain score for sexual responsiveness for women
aged 45 years or older was associated with higher odds of having a serum dehydroepiandrosterone
sulfate level below the 10th percentile for this age group (odds ratio [OR],
3.90; 95% confidence interval [CI], 1.54-9.81; P = .004).
For women aged 18 to 44 years, having a low domain score for sexual desire
(OR, 3.86; 95% CI, 1.27-11.67; P = .02),
sexual arousal (OR, 6.39; 95% CI, 2.30-17.73; P<.001),
and sexual responsiveness (OR, 6.59; 95% CI, 2.37-18.34; P<.001) was associated with having a dehydroepiandrosterone sulfate
level below the 10th percentile.ConclusionsNo single androgen level is predictive of low female sexual function,
and the majority of women with low dehydroepiandrosterone sulfate levels did
not have low sexual function.
458 citations
TL;DR: The new field of intracrinology or local formation of sex steroids from DHEA in target tissues has permitted major advances in the treatment of the two most frequent cancers, namely breast and prostate cancer, while its potential use as a physiological HRT could well provide a physiological balance of androgens and estrogens, thus offering exciting possibilities for women's health at menopause.
Abstract: Dehydroepiandrosterone (DHEA) is not a hormone but it is a very important prohormone secreted in large amounts by the adrenals in humans and other primates, but not in lower species. It is secreted in larger quantities than cortisol and is present in the blood at concentrations only second to cholesterol. All the enzymes required to transform DHEA into androgens and/or estrogens are expressed in a cell-specific manner in a large series of peripheral target tissues, thus permitting all androgen-sensitive and estrogen-sensitive tissues to make locally and control the intracellular levels of sex steroids according to local needs. This new field of endocrinology has been called intracrinology. In women, after menopause, all estrogens and almost all androgens are made locally in peripheral tissues from DHEA which indirectly exerts effects, among others, on bone formation, adiposity, muscle, insulin and glucose metabolism, skin, libido and well-being. In men, where the secretion of androgens by the testicles continues for life, the contribution of DHEA to androgens has been best evaluated in the prostate where about 50% of androgens are made locally from DHEA. Such knowledge has led to the development of combined androgen blockade (CAB), a treatment which adds a pure anti-androgen to medical (GnRH agonist) or surgical castration in order to block the access of the androgens made locally to the androgen receptor. In fact, CAB has been the first treatment demonstrated to prolong life in advanced prostate cancer while recent data indicate that it can permit long-term control and probably cure in at least 90% of cases of localized prostate cancer. The new field of intracrinology or local formation of sex steroids from DHEA in target tissues has permitted major advances in the treatment of the two most frequent cancers, namely breast and prostate cancer, while its potential use as a physiological HRT could well provide a physiological balance of androgens and estrogens, thus offering exciting possibilities for women's health at menopause.
447 citations