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Review

Role of androgens in cardiovascular pathology

Dimitry A Chistiakov1 Department of Neurochemistry, Division of Basic and Applied Neurobiology, Serbsky Federal Medical Research Center of Psychiatry and Narcology, Moscow, Russia
,
Veronika A Myasoedova2 Laboratory of Angiopathology, Institute of General Pathology and Pathophysiology, Moscow, Russia, [email protected]
,
Alexandra A Melnichenko2 Laboratory of Angiopathology, Institute of General Pathology and Pathophysiology, Moscow, Russia, [email protected]
,
Andrey V Grechko3 Federal Scientific Clinical Center for Resuscitation and Rehabilitation, Moscow, Russia
&
Alexander N Orekhov2 Laboratory of Angiopathology, Institute of General Pathology and Pathophysiology, Moscow, Russia, [email protected];4 Institute for Atherosclerosis Research, Skolkovo Innovative Center, Moscow, Russia, [email protected]Correspondence[email protected]
Pages 283-290 | Published online: 15 Oct 2018

Abstract

Cardiovascular effects of android hormones in normal and pathological conditions can lead to either positive or negative effects. The reason for this variation is unknown, but may be influenced by gender-specific effects of androids, heterogeneity of the vascular endothelium, differential expression of the androgen receptor in endothelial cells (ECs) and route of androgen administration. Generally, androgenic hormones are beneficial for ECs because these hormones induce nitric oxide production, proliferation, motility, and growth of ECs and inhibit inflammatory activation and induction of procoagulant, and adhesive properties in ECs. This indeed prevents endothelial dysfunction, an essential initial step in the development of vascular pathologies, including atherosclerosis. However, androgens can also activate endothelial production of some vasoconstrictors, which can have detrimental effects on the vascular endothelium. Androgens also activate proliferation, migration, and recruitment of endothelial progenitor cells (EPCs), thereby contributing to vascular repair and restoration of the endothelial layer. In this paper, we consider effects of androgen hormones on EC and EPC function in physiological and pathological conditions.

Introduction

Androgens are a group of steroid hormones mostly represented by steroids produced by the testes and adrenal cortex. The main examples of androgens include testosterone, androstenedione, dehydroepiandrosterone(DHEA), and dehydroepiandrosterone sulfate. Androgens play a key role in the establishment and maintenance of male properties in vertebrates, including sex activity and formation of secondary sex features in males.

In cardiovascular pathology, males have a higher risk of developing the disease during the reproductive period in comparison with females of the same age.Citation1 The sex-related difference in resistance to cardiovascular disease was hypothesized to be related to the cardioprotective role of estrogen hormones in females and harmful effects of androgen steroids in males.Citation2 This hypothesis was not initially supported by large-scale follow-up studies.Citation3 In contrast, many studies indicated the positive role of androgens in cardiovascular protection.Citation1 Furthermore, follow-up clinical studies showed that plasma concentrations of androgens were associated with various independent cardiovascular risk factors and mortality from cardiovascular pathology.Citation1,Citation4Citation6 For example, decrease in blood testosterone was found to show a positive correlation with the elevation of arterial stiffness (an independent marker of cardiovascular pathology).Citation7 In a recent meta-analysis, cardiovascular risk, in men with coronary artery disease (CAD) and heart failure who took testosterone as a drug compared with the control (placebo) group, was decreased.Citation8 Androgen steroids were found to attenuate atherogenesis in males via several mechanisms, including modulatory effects on lesion progression and plaque vulnerability to thrombosis,Citation9 decreasing fat accumulation in the arterial intima media,Citation10 and reducing carotid intima media thickness.Citation11 Treatment with testosterone was shown to induce arterial vasorelaxation in males affected with CAD.Citation12,Citation13 In a randomized clinical trial, administration of testosterone in low doses was found to significantly improve cardiac function in men with stable angina when compared with the placebo group.Citation14 Treatment of hypogonadal men with testosterone led to reduced levels of inflammatory cytokines, decreased concentrations of total cholesterol but elevated interleukin (IL)-10, an anti-inflammatory cytokine.Citation9 Compared with the placebo group, regular injections of testosterone had beneficial effects on hypogonadal men affected with ischemic heart disease by improving mood and decreasing levels of total cholesterol and tumor necrosis factor (TNF)-α, a pro-inflammatory cytokine.Citation15 In cardiometabolic pathology, androgens exhibit pleiotropic positive effects by improving glucose metabolism,Citation16 serum lipid profile,Citation17 and hemostasis,Citation18 and inducing vasodilation.Citation13 Androgens are known to target muscle cells by promoting their growth and cardiomyocytes can respond to testosterone by increasing the cell size leading to cardiac hypertrophy.Citation19 In the vascular system, endothelial cells (ECs) and endothelial progenitor cells (EPCs) are primary targets of favorable actions of androgen hormones through the vascular lumen. We will discuss below the action of androgens on the cardiovascular system after reviewing the general role of androgens in physiological conditions.

Biogenesis and biological actions of androgenic hormones

In mammals, two androgen hormones, testosterone and dihydrotestosterone (DHT) play a major role.Citation20 Both hormones interact with the single androgen receptor (AR). It has been found that testosterone binds to the AR with a stronger affinity than DHT.Citation21 Testosterone is the major sex hormone in males and is mainly produced by testes. Its synthesis is quite complicated and is converted from cholesterol by the action of five enzymes. Testosterone can then be transformed to DHT by 5α-reductase (5αRD) isozymes and the aromatase cytochrome P-450.Citation22 Testosterone is crucial in the control of catabolic reactions and general androgenic actions in males.Citation23 DHT is hardly involved in penis and prostate formation.Citation24

In the cerebral arteries, ECs produce receptors that bind steroid hormones and steroid-metabolizing enzymes. For example, estrogen receptor (ER)α, 5αRD isoform 2, and aromatase were found to be expressed by cerebral endothelium. Aromatase transforms testosterone to 17β-estradiol, a female sex hormone, thereby affecting the local equilibrium between androgens and estrogens in the brain.Citation25 It has been shown that the function of brain vessels can be influenced by local steroid hormones as well as by circulating steroids.Citation26

AR mainly mediates the physiological effects of androgenic steroids. The binding of an androgen to AR leads to structural changes in the receptor molecule and causes the dissociation of chaperons that are bound to the inactive receptor. This induces AR dimerization, nuclear trafficking, and receptor activation through phosphorylation and promotion of transcriptional activity.Citation27 Described above was the DNA-dependent pathway of the androgen-mediated control of gene expression. The non-genomic mechanism of the action of androgens involves the modulation of numerous signaling pathways. One of them is the stimulation of cyclic adenosine monophosphate and protein kinase-A (PKA) via the sex hormone binding globulin (SHBG)/SHBG receptor complex.Citation28 This way leads to the elevation of cytoplasmic Ca2+ concentration. Indeed, increase in intracellular Ca2+ results in the stimulation of several signaling pathways, such as the PKA-dependent pathway,Citation29 the protein kinase-C-mediated mechanism,Citation30 and mitogen-activated protein kinases (MAPKs),Citation31 that finally induce the activation of AR and other transcription factors. The DNA-dependent pathway is slow to take effect, requiring several hours, while the non-DNA-dependent mechanism is much faster (taking only seconds or minutes) and can lead to posttranslational modulation of AR and other transcriptional factors. Additionally, AR can be stimulated by several growth factors including insulin-like growth factor-1 and epithelial growth factor. Because androgen-dependent non-genomic modifications are not involved in gene expression, these modifications can be manifested quickly. Cell type and AR ligands modulate the physiological action of androgen hormones to select genomic or non-genomic mechanisms of action.Citation32

Role of androgen hormones in ECs

Endothelial dysfunction is the initial stage in multiple cardiovascular disorders such as atherosclerosis and atherothrombosis. The prevalence of vasoconstrictors or vasodilators results in the promotion of the arterial stiffness.Citation33 In this context, the presence and viability of EPCs was considered an essential factor for productive vascular repair and recovery of the endothelial layer after vessel denudation.Citation34 Deficiency and loss of function of EPCs were observed to be inversely associated with various cardiovascular risk factors, while higher levels of EPCs correlate with decreased mortality from cardiovascular events.Citation35

The deficiency of EPCs reduces the regenerative potential of vascular endothelium and can lead to the progression of cardiovascular pathology. Since androgens generally have a protective role on ECs, androgen administration may prove beneficial for the improvement of endothelial function and prevention of atherosclerosis.

Role of androgens and estrogens on proliferation of ECs

Androgens, such as testosterone and DHT, are involved in controlling EC proliferation and function.Citation36 In cultured human ECs, administration of DHT was shown to increase cell growth, stimulate MAPKs and creatine kinase.Citation37,Citation38 Treatment with flutamide, an antagonist of AR, inhibited DHT actions, suggesting the involvement of AR-associated pathway. In a primary culture of aortic ECs, androgens were shown to induce EC proliferation and viability through AR/vascular endothelial growth factor (VEGF)-dependent and cyclin-dependent mechanisms.Citation39 In cultured ECs, the activation of VEGF synthesis was followed by the stimulation of cyclin expression and finally resulted in cell proliferation.Citation39 In ECs of female rats, testosterone can bind to AR and stimulate nitric oxide (NO) production that in turn potentiates EC growth.Citation40 Therefore, androgens support EC growth and proliferation that are important for endothelial repair in vascular damage and/or endothelial dysfunction, ie, are the important factors of cardiovascular disease.

In vascular beds, the population of ECs is rather heterogeneous and depends on the location.Citation41 For example, AR is not expressed in microvessels of certain tissues, such as skin or prostate, thereby preventing androgen-dependent EC proliferation through primary binding to AR.Citation42 However, androgens are able to influence the function of those cells in a paracrine manner through the stimulation of liberation of VEGF. A recent study showed that DHT could induce VEGF production by prostate cancer cells that in turn activated proliferation of ECs.Citation43 This effect could be defeated by estrogens.Citation44 The mechanism of VEGF induction in cancer cells may be important for the formation of tumor neovessels and further tumor propagation. However, vascular endothelium expresses both AR and ER. Indeed, the function of ECs can be modulated by both androgens and estrogens. Estrogens exhibit the opposite effects on EC proliferation, supporting the quiescence of endothelium through the inhibition of cyclin A production and inducing the transformation of testosterone to 17α-estradiol, a female hormone.Citation44,Citation45

According to recent findings, VEGF can act on ECs in both autocrine and paracrine fashions. For instance, estrogens are able to influence the effects of androgens on cell growth in ECs that do not express AR in a paracrine manner.Citation43 However, other androgen/estrogen-dependent vasoactive agents that explain the complexity of vasodilatory/vasoconstrictor effects of sex hormones on vascular endothelium, may exist.Citation39

Effects of androgens on proliferation of EPCs

Androgen hormones also stimulate the function of EPCs. Bone marrow-derived EPCs were shown to be involved in vessel remodeling, vasculogenesis, and reparation of endothelial denudation in injured vascular regions.Citation33,Citation46 Decreased EPC numbers in the cardiovascular system correlate with elevated cardiovascular risk, while increased EPC counts correlate with decreased risk of cardiovascular mortality.Citation35,Citation47 Furthermore, cell therapy with EPCs was shown to have beneficial effects on people with cardiovascular disease.Citation48,Citation49 Increased circulating EPC numbers were found to correlate with higher blood levels of androgens.Citation49,Citation50

Some studies also showed that patients with central hypogonadism, a syndrome characterized by low production of sex hormones, had decreased levels of EPCs.Citation51,Citation52 Treatment with testosterone can improve the state of men with central hypogonadism.Citation53

Expression of AR was found in human EPCs. The binding of androgen hormones to the AR activates EPC proliferation and migration.Citation51 Androgen steroids control the proliferation of EPCs via the PI3K/Akt signaling.Citation53 Androgen-dependent stimulation of EC and EPC proliferation may, therefore, be suggestive of the cardioprotective effects of these hormones through the stimulation of vascular repair.Citation53

Effects of androgens on the vascular tone

The role of ECs in the regulation of vascular tone is crucial. Androgens cause arterial vasodilation by inducing relaxation of vascular smooth muscle cells (VSMCs) and also contribute to vasorelaxation through the induction of NO formation by ECs.Citation54 It was shown that in cultured ECs, DHEA stimulated endothelial NO production by up-regulating expression of endothelial NO synthase (eNOS) and ERK1/2 signaling.Citation55 In the ERK1/2-dependent pathway, DHEA regulates G protein-coupled receptors-ERK1/2-MAPK signaling to activate eNOS protein production. DHEA also increases the duration of eNOS expression.Citation56

In human umbilical vein endothelial cells (HUVECs), testosterone and DHT were observed to rapidly stimulate NO release in a dose-dependent manner through the activation of PI3K/Akt and ERK1/2 mechanisms. Androgen-dependent NO production was inhibited by flutamide, an AR-antagonist, indicating that stimulatory effects of androgens on ECs are mediated by the AR.Citation57 Identical effects of androgen hormones were also observed in cultured human arterial ECs.Citation58

To stimulate endothelial NO production, testosterone activates release of Ca2+ from the endoplasmic reticulum that then increases eNOS activity and NO generation. NO, in turn, causes elevated cyclic guanosine monophosphate (cGMP) production by up-regulation of guanylate cyclase. In turn, cGMP decreases Ca2+ influx to VSMCs leading to vasodilation. In addition, testosterone up-regulates the liberation of endothelium-derived hyperpolarizing factor, a vasodilator, which blocks the activity of Ca2+ channels and activates large-conductance K+ channels. Finally, this results in VSMC hyperpolarization and relaxation.Citation59

Data about the involvement of androgens in vasorelaxation through mediating the activity of cyclooxygenases are still contradictory.Citation60Citation62 It was demonstrated that testosterone-dependent vasodilation involves the activation of eNOS, inducible NO synthase, and increased production of prostacyclin.Citation61 Testosterone up-regulates cyclooxygenase-2, which in turn leads to increased prostacyclin formation. However, thromboxane A2 does not contribute to androgen-dependent vasorelaxation.Citation63 Androgens can also stimulate relaxation of vessels through induction of hydrogen sulphide (H2S) via an AR-HSP90-cystathionine-γ lyase pathway.Citation64 Cystathionine-γ lyase can produce H2S from amino acid L-cysteine. H2S is a physiologically active gas that is involved in cell signaling causing various biological effects including vasorelaxation.Citation65 Decrease in cystathionine-γ lyase activity and insufficient production of H2S by HUVECs was shown to be associated with preeclampsia.Citation66

Androgens can also induce vasoconstriction by up-regulation of the synthesis of arachidonic acid intermediates, including thromboxane A2 and 20-hydroxyeicosatetraenoic acid.Citation60,Citation62 Androgenic steroids can also modulate production of endothelin-1 (ET-1), an endothelium-derived vasoactive molecule that increases blood pressure. In postmenopausal women, a direct correlation was shown between blood levels of testosterone, ET-1, and vascular tone.Citation67 Female-to-male transsexuals who are treated with high doses of testosterone have increased ET levels.Citation68 However, in hypogonadal men, plasma ET is increased and tends to decrease after treatment with testosterone, suggesting that androgen hormones can reduce ET-1 formation.Citation69,Citation70

Effects of androgens on the myocardium

The growth-promoting effect of androgens on muscle cells is currently well known.Citation71 Anabolic androgens are used in clinical practice to accelerate healing of wounds, promote skeletal muscle growth, and treat cachexia. Due to their effects on skeletal muscles, these hormones are often misused, for instance, by bodybuilders. High doses of anabolic androgens can induce pathological processes, most importantly, cardiac hypertrophy.Citation72 Moreover, animal studies have provided evidence that supra-physiological doses of testosterone induce cardiac fibrosis and apoptosis.Citation73 Antiandrogenic therapy was shown to be beneficial for the treatment of induced cardiac hypertrophy in model rodents.Citation74 However, at physiological levels, androgens are more likely to have a protective effect on the myocardium: testosterone deficiency was shown to be associated with cardiovascular risk in humans, while treatment with testosterone had beneficial effects.Citation75

Treatment of aging males with physiological testosterone doses is known to have positive effects on the lipid profile, thus protecting them from atherosclerosis-related cardiovascular disease.Citation76 Indeed, androgen dysregulation associated with aging generally results in altered lipid metabolism, increased body fat and obesity that represent well-known risk factors of cardiovascular disease, and in many instances, can be attenuated by testosterone replacement therapy.Citation77 Direct protective effects of testosterone on cardiomyocytes were studied in animal models. For instance, testosterone could protect rat myocardium from ischemia/reperfusion injury through stimulation of α(1)-AR.Citation78 The protective effects of androgens can also be conveyed in an AR-independent manner, as was shown in a mouse model, where physiological doses of testosterone attenuated aging of cardiomyocytes.Citation79

In summary, it can be concluded that androgens at physiological levels appear to have a protective effect on the myocardium and cardiovascular system in general. The precise mechanisms of these effects remain to be studied in detail, but it is likely that it is pleiotropic and includes both direct pathways mediated by AR and indirect actions via improving lipid profile, reducing hypertension, fat deposition, chronic inflammation and other cardiovascular risk factors.

The role of androgenic hormones in endothelial inflammatory responses

Endothelial inflammatory activation and dysfunction are involved in the initial steps of vascular impairment, including further atherogenesis. Androgenic hormones were shown to act as pro-inflammatory and anti-inflammatory messengers in circulation.Citation54 Many studies show that increase of plasma levels of android hormones is associated with elevated levels of inflammatory signaling molecules in humans.Citation80Citation82 Correlation between endothelial expression of adhesion molecules, such as vascular cell adhesion molecule-1 (VCAM-1) and endothelial selectin, and testosterone levels was shown by several studies.Citation83Citation86 Therefore, these findings suggest that increased concentrations of androgenic steroids can enhance the adhesion of monocytes to ECs, an initial stage of vascular inflammation that can lead to the atherogenic changes in arterial vessels.

On the other hand, androgens exhibit anti-inflammatory properties through induction of endothelial vasodilation and production of anti-inflammatory cytokines, such as IL-10. Moreover, exposure of cultured human ECs to DHT or testosterone resulted in attenuated TNF-α/lipopolysaccharide -dependent inflammation and caused down-regulation of inflammatory molecules such as IL-6, VCAM-1, chemokine ligand 2, and caspases.Citation87 In cultured HUVECs, androgens were shown to suppress expression of caspase-3 and -9, and activity of p38/MAPK, and indeed decrease apoptosis of ECs induced by hydrogen peroxide (H2O2).Citation83,Citation84,Citation88 It is difficult to explain these conflicting results, but the discrepancy can be influenced by the origin of ECs, donor’s sex, and a variety of signaling pathways influenced by androids. In a recent review attempting to summarize available knowledge, it was suggested that androgen dysregulation is likely to convey its deleterious effects on the cardiovascular system via a chronic inflammatory process, which is dependent on different signaling pathways, including nuclear factor-κB, and tightly linked to changes of lipid metabolism and increased blood pressure.Citation89

Anti-thrombotic actions of androgens

Quiescent ECs secrete a number of molecules involved in hemostasis and thrombosis such as plasminogen activator inhibitor type 1 (PAI-I), tissue plasminogen activator (t-PA), and tissue factor pathway inhibitor (TFPI). All these proteins are involved in the breakdown of blood clots, thereby indicating the anti-coagulant state of ECs in normal conditions. In elderly people, decreased plasma testosterone was shown to be associated with reduced TFPI levels and accelerated hemostatic response.Citation90 Furthermore, serum testosterone was shown to directly correlate with t-PA but inversely correlate with PAI-I and factor VII.Citation91,Citation92 In cultured HUVECs, stimulatory effects of testosterone on TFPI and t-PA expression levels were observed.Citation93 In summary, these results indicate that androids show anti-thrombotic properties, thereby possessing the cardioprotective function.

Effects of testosterone replacement therapy

Testosterone replacement therapy (TRT) of hypogonadal and aging men was introduced into clinical practice a long time ago. In normal physiological concentrations, testosterone as a therapeutic agent shows favorable vasculoprotective effects,Citation94 which have also been discussed above. Nevertheless, some clinical studies have reported adverse cardiovascular side effects of TRT in elderly men with low testosterone levels and various comorbidities.Citation95,Citation96 For instance, treatment of old men fragility with testosterone was found to increase the frequency of cardiovascular events and overall cardiovascular mortality in the elderly. These results, however, were questioned by the scientific community.Citation97 Indeed, the retrospective design of the studies did not allow for proper comparison between groups, and the studied populations did not allow for generalization of the safety results. More studies are needed to properly evaluate the safety of TRT and risk/benefit balance of this therapeutic approach. Despite the fact that some clinical trials showed unfavorable effects of testosterone treatment, the majority of studies demonstrated beneficial role of therapy with androgen hormones on the cardiovascular health that is broadly appreciated.

Conclusion

Androgenic steroid hormones act through genomic and non-genomic mechanisms and significantly influence the function of ECs and their progenitors. These hormones are involved in the regulation of the vascular tone, proliferation, mobility, adhesion, and anti-thrombotic properties of vascular endothelium. Androgens also participate in important pathogenic mechanisms such as atherogenesis and vascular inflammation. Many studies indicate that androgens play a vasculoprotective role through the anti-inflammatory, anti-apoptotic, and vasodilatory actions on endothelium and VSMCs and recruitment of EPCs essential for vascular repair. However, there are studies that report the adverse vascular effects of androgens, for example, via induction of several vasoconstrictors. The causes of these disparities are obscure, but can involve the heterogeneity of the vascular endothelium and gender-specific effects of androgens. In addition, significant spatial and temporal changes in AR expression observed in ECs and their progenitors can also contribute to the opposite effects of androgens on vascular endothelium.

Author contributions

All authors contributed toward drafting and critically revising the paper and agree to be accountable for all aspects of the work.

Acknowledgments

The work was supported by the Russian Science Foundation (grant no. # 18-15-00254).

Disclosure

The authors report no conflicts of interest in this work.

References

  • NettleshipJEJonesRDChannerKSJonesTHTestosterone and coronary artery diseaseFront Horm Res2009379110719011291
  • KannelWBHjortlandMCMcnamaraPMGordonTMenopause and risk of cardiovascular disease: the Framingham studyAnn Intern Med1976854447452970770
  • HendrixSLWassertheil-SmollerSJohnsonKCEffects of Conjugated Equine Estrogen on Stroke in the Women’s Health InitiativeCirculation2006113202425243416702472
  • SmithMRAndrogen deprivation therapy for prostate cancer: new concepts and concernsCurr Opin Endocrinol Diabetes Obes200714324725417940447
  • KintzelPEChaseSLSchultzLMO’RourkeTJIncreased Risk of Metabolic Syndrome, Diabetes Mellitus, and Cardiovascular Disease in Men Receiving Androgen Deprivation Therapy for Prostate CancerPharmacotherapy200828121511152219025432
  • TivestenAVandenputLLabrieFLow serum testosterone and estradiol predict mortality in elderly menJ Clin Endocrinol Metab20099472482248819401373
  • DockeryFBulpittCJDonaldsonMFernandezSRajkumarCThe Relationship Between Androgens and Arterial Stiffness in Older MenJ Am Geriatr Soc200351111627163214687394
  • MorgentalerAMinerMMCaliberMGuayATKheraMTraishAMTestosterone Therapy and Cardiovascular Risk: Advances and ControversiesMayo Clin Proc201590222425125636998
  • MalkinCPughPJJonesRDJonesTHChannerKSTestosterone as a protective factor against atherosclerosis--immunomodulation and influence upon plaque development and stabilityJ Endocrinol2003178337338012967330
  • AlexandersenPHaarboJByrjalsenILawaetzHChristiansenCNatural Androgens Inhibit Male Atherosclerosis : A Study in Castrated, Cholesterol-Fed RabbitsCirc Res199984781381910205149
  • ChanYXKnuimanMWHungJTestosterone, dihydrotestosterone and estradiol are differentially associated with carotid intima-media thickness and the presence of carotid plaque in men with and without coronary artery diseaseEndocr J201562977778626073868
  • RosanoGMCLeonardoFPagnottaPAcute Anti-Ischemic Effect of Testosterone in Men With Coronary Artery DiseaseCirculation199999131666167010190874
  • KangS-MJangYKimJi-YJiKEffect of oral administration of testosterone on brachial arterial vasoreactivity in men with coronary artery diseaseAm J Cardiol200289786286411909577
  • EnglishKMSteedsRPJonesTHDiverMJChannerKSLow-dose transdermal testosterone therapy improves angina threshold in men with chronic stable angina: A randomized, double-blind, placebo-controlled studyCirculation2000102161906191111034937
  • MalkinCJPughPJMorrisPDTestosterone replacement in hypogonadal men with angina improves ischaemic threshold and quality of lifeHeart200490887187615253956
  • HakAEWittemanJCde JongFHGeerlingsMIHofmanAPolsHALow levels of endogenous androgens increase the risk of atherosclerosis in elderly men: the Rotterdam studyJ Clin Endocrinol Metab20028783632363912161487
  • SvartbergJvon MühlenDMathiesenEJoakimsenOBønaaKHStensland-BuggeELow testosterone levels are associated with carotid atherosclerosis in menJ Intern Med2006259657658216704558
  • GyllenborgJRasmussenSLBorch-JohnsenKHeitmannBLSkakkebaekNEJuulACardiovascular risk factors in men: The role of gonadal steroids and sex hormone-binding globulinMetabolism200150888288811474474
  • DuranJOyarceCPavezMGSK-3β/NFAT Signaling Is Involved in Testosterone-Induced Cardiac Myocyte HypertrophyPLoS One20161112e016825527977752
  • ZhuYSKatzMDImperato-McginleyJNatural potent androgens: lessons from human genetic modelsBaillieres Clin Endocrinol Metab1998121831139890063
  • ZhuYSMolecular Basis of Steroid Action in the ProstateCellscience200514275516971966
  • SultanCLumbrosoSParisFDisorders of Androgen ActionSemin Reprod Med200220321722812428202
  • YoshidaSIkedaYAiharaK-IchiAiharaKRoles of the Androgen – Androgen Receptor System in Vascular AngiogenesisJ Atheroscler Thromb201623325726526522430
  • AmoryJKAnawaltBDMatsumotoAMThe effect of 5alpha-reductase inhibition with dutasteride and finasteride on bone mineral density, serum lipoproteins, hemoglobin, prostate specific antigen and sexual function in healthy young menJ Urol2008α9:2333α9:2338
  • GonzalesRJAnsarSDucklesSPKrauseDNAndrogenic/estrogenic balance in the male rat cerebral circulation: metabolic enzymes and sex steroid receptorsJ Cereb Blood Flow Metab200727111841185217406656
  • KrauseDNDucklesSPGonzalesRJLocal oestrogenic/androgenic balance in the cerebral vasculatureActa Physiol20112031181186
  • ArandaAPascualANuclear Hormone Receptors and Gene ExpressionPhysiol Rev20018131269130411427696
  • KahnSMHrybDJNakhlaAMRomasNARosnerWSex hormone-binding globulin is synthesized in target cells. Sex hormone-binding globulin is synthesized in target cellsJ Endocrinol200217511312012379495
  • BagchiGWuJFrenchJKimJMoniriNHDaakaYAndrogens Transduce the G s-Mediated Activation of Protein Kinase A in Prostate CellsCancer Res20086893225323118451148
  • ChristianHCRollsNJMorrisJFNongenomic actions of testosterone on a subset of lactotrophs in the male rat pituitaryEndocrinology200014193111311910965881
  • GatsonJWKaurPSinghMDihydrotestosterone differentially modulates the mitogen-activated protein kinase and the phosphoinositide 3-kinase/Akt pathways through the nuclear and novel membrane androgen receptor in C6 cellsEndocrinology200614742028203416410299
  • KimSBKannoAOzawaTTaoHUmezawaYNongenomic Activity of Ligands in the Association of Androgen Receptor with SRCACS Chem Biol20072748449217602621
  • GatesPEStrainWDShoreACHuman endothelial function and microvascular ageingExp Physiol200994331131619042980
  • FadiniGPAgostiniCSartoreSAvogaroAEndothelial progenitor cells in the natural history of atherosclerosisAtherosclerosis20071941465417493626
  • WernerNKosiolSSchieglTCirculating Endothelial Progenitor Cells and Cardiovascular OutcomesN Engl J Med Overseas Ed2005353109991007
  • Torres-EstayVCarreñoDVSan FranciscoIFSotomayorPGodoyASSmithGJAndrogen receptor in human endothelial cellsJ Endocrinol20152243R131R13725563353
  • SomjenDKohenFJaffeAAmir-ZaltsmanYKnollESternNEffects of gonadal steroids and their antagonists on DNA synthesis in human vascular cellsHypertension199832139459674635
  • SomjenDKohenFGayerBKulikTKnollESternNRole of putative membrane receptors in the effect of androgens on human vascular cell growth. Role of putative membrane receptors in the effect of androgens on human vascular cell growthJ Endocrinol20041809710614709148
  • CaiJHongYWengCTanCImperato-McginleyJZhuY-SAndrogen stimulates endothelial cell proliferation via an androgen receptor/VEGF/cyclin A-mediated mechanismAm J Physiol Heart Circ Physiol20113004H1210H122121257919
  • CampeloAECutiniPHMassheimerVLChristianHCRollsNJMorrisJFTestosterone modulates platelet aggregation and endothelial cell growth through nitric oxide pathway. Nongenomic actions of testosterone on a subset of lactotrophs in the male rat pituitaryEndocrinology20001413111311910965881
  • AirdWCEndothelial cell heterogeneityCrit Care Med200331SupplementS221S23012682444
  • PrinsGSBirchLGreeneGLAndrogen Receptor Localization in Different Cell Types of the Adult Rat Prostate*Endocrinology19911296318731991954898
  • WenJZhaoYLiJSuppression of DHT-induced paracrine stimulation of endothelial cell growth by estrogens via prostate cancer cellsProstate201373101069108123423946
  • WengCCaiJWenJDifferential effects of estrogen receptor ligands on regulation of dihydrotestosterone-induced cell proliferation in endothelial and prostate cancer cellsInt J Oncol201342132733723135751
  • QiaoYZhangZ-KCaiL-QTanCImperato-McginleyJLZhuY-S17α-estradiol inhibits LAPC-4 prostatic tumor cell proliferation in cell cultures and tumor growth in xenograft animalsProstate200767161719172817879940
  • BalakumarPKaurTSinghMPotential target sites to modulate vascular endothelial dysfunction: Current perspectives and future directionsToxicology20082451–2496418242815
  • HillJMZalosGHalcoxJPJCirculating Endothelial Progenitor Cells, Vascular Function, and Cardiovascular RiskN Engl J Med Overseas Ed20033487593600
  • WernerLDeutschVBarshackIMillerHKerenGGeorgeJTransfer of endothelial progenitor cells improves myocardial performance in rats with dilated cardiomyopathy induced following experimental myocarditisJ Mol Cell Cardiol200539469169716125196
  • Flores-RamírezRUribe-LongoriaARangel-FuentesMMIntracoronary infusion of CD133+ endothelial progenitor cells improves heart function and quality of life in patients with chronic post-infarct heart insufficiencyCardiovasc Revasc Med2010112727820347795
  • WangXXZhangFRShangYPTransplantation of autologous endothelial progenitor cells may be beneficial in patients with idiopathic pulmonary arterial hypertension: a pilot randomized controlled trialJ Am Coll Cardiol200749141566157117418297
  • ForestaCCarettaNLanaAReduced number of circulating endothelial progenitor cells in hypogonadal menJ Clin Endocrinol Metab200691114599460216926245
  • LiaoCHWuYNLinFYTsaiWKLiuSPChiangHSTestosterone replacement therapy can increase circulating endothelial progenitor cell number in men with late onset hypogonadismAndrology20131456356923653307
  • LiuRDingLYuM-HMhYEffects of dihydrotestosterone on adhesion and proliferation via PI3-K/Akt signaling in endothelial progenitor cellsEndocrine201446363464324190051
  • KellyDMJonesTHTestosterone: a vascular hormone in health and diseaseJ Endocrinol20132173R47R7123549841
  • WilliamsMRDawoodTLingSDehydroepiandrosterone increases endothelial cell proliferation in vitro and improves endothelial function in vivo by mechanisms independent of androgen and estrogen receptorsJ Clin Endocrinol Metab20048994708471515356084
  • SimonciniTMannellaPFornariLVaroneGCarusoAGenazzaniARDehydroepiandrosterone Modulates Endothelial Nitric Oxide Synthesis Via Direct Genomic and Nongenomic MechanismsEndocrinology200314483449345512865324
  • GogliaLTosiVSanchezAMEndothelial regulation of eNOS, PAI-1 and t-PA by testosterone and dihydrotestosterone in vitro and in vivoMol Hum Reprod2010161076176920547636
  • YuJAkishitaMEtoMAndrogen Receptor-Dependent Activation of Endothelial Nitric Oxide Synthase in Vascular Endothelial Cells: Role of Phosphatidylinositol 3-Kinase/Akt PathwayEndocrinology201015141822182820194727
  • WynneFLKhalilRATestosterone and coronary vascular tone: Implications in coronary artery diseaseJ Endocrinol Invest200326218118612739749
  • WongSLLeungFPLauCWCyclooxygenase-2-Derived Pros-taglandin F2 Mediates Endothelium-Dependent Contractions in the Aortae of Hamsters With Increased Impact During AgingCirc Res2009104222823519096033
  • MarrachelliVGMirandaFJCentenoJMRole of NO-synthases and cyclooxygenases in the hyperreactivity of male rabbit carotid artery to testosterone under experimental diabetesPharmacol Res2010611627019573602
  • WuCCSchwartzmanMLThe role of 20-HETE in androgen-mediated hypertensionProstaglandins Other Lipid Mediat2011961–4455321722750
  • CaugheyGEClelandLGPenglisPSGambleJRJamesMJRoles of cyclooxygenase (COX)-1 and COX-2 in prostanoid production by human endothelial cells: selective up-regulation of prostacyclin synthesis by COX-2J Immunol200116752831283811509629
  • BrancaleoneVVelleccoVMatassaDSCrucial role of androgen receptor in vascular H 2 S biosynthesis induced by testosteroneBr J Pharmacol201517261505151524750035
  • WangMGuoZWangSThe Effect of Certain Conditions in the Regulation of Cystathionine γ-Lyase by Exogenous Hydrogen Sulfide in Mammalian CellsBiochem Genet2013517–850351323515848
  • WangKAhmadSCaiMDysregulation of hydrogen sulfide producing enzyme cystathionine γ-lyase contributes to maternal hypertension and placental abnormalities in preeclampsiaCirculation2013127252514252223704251
  • MaturanaMABredaVLhullierFSpritzerPMRelationship between endogenous testosterone and cardiovascular risk in early postmenopausal womenMetabolism200857796196518555838
  • PoldermanKHStehouwerCDvan KampGJDekkerGAVerheugtFWGoorenLJInfluence of sex hormones on plasma endothelin levelsAnn Intern Med199311864294328439117
  • KumanovPTomovaAKirilovGDakovskaLSchinkovAIncreased plasma endothelin levels in patients with male hypogonadismAndrologia2002341293311996179
  • KumanovPTomovaAKirilovGTestosterone replacement therapy in male hypogonadism is not associated with increase of endothelin-1 levelsInt J Androl2007301414716879620
  • WyceABaiYNagpalSThompsonCCResearch Resource: The androgen receptor modulates expression of genes with critical roles in muscle development and functionMol Endocrinol20102481665167420610535
  • PirompolPTeekabutVWeerachatyanukulWBupha-IntrTWattana-permpoolJSupra-physiological dose of testosterone induces pathological cardiac hypertrophyJ Endocrinol20162291132326850730
  • PapamitsouTBarlagiannisDPapaliagkasVKotanidouEDermentzo-poulou-TheodoridouMTestosterone-induced hypertrophy, fibrosis and apoptosis of cardiac cells--an ultrastructural and immunohistochemical studyMed Sci Monit2011179BR266BR27321873939
  • ZwadloCSchmidtmannESzaroszykMAntiandrogenic therapy with finasteride attenuates cardiac hypertrophy and left ventricular dysfunctionCirculation2015131121071108125632043
  • YeapBBAndrogens and cardiovascular diseaseCurr Opin Endocrinol Diabetes Obes201017326927620186051
  • RosanoGMCornoldiAFiniMEffects of androgens on the cardiovascular systemJ Endocrinol Invest2005283 Suppl3238
  • AllanCAStraussBJGMclachlanRIBody composition, metabolic syndrome and testosterone in ageing menInt J Impot Res200719544845717554396
  • TsangSWuSLiuJWongTMTestosterone protects rat hearts against ischaemic insults by enhancing the effects of α1 -adrenoceptor stimulationBr J Pharmacol2008153469370918157169
  • ZhangLLeiDZhuGPHongLWuSZPhysiological testosterone retards cardiomyocyte aging in Tfm mice via androgen receptor-independent pathwayChin Med Sci J2013282889423806370
  • LiuPYDeathAKHandelsmanDJAndrogens and cardiovascular diseaseEndocr Rev200324331334012788802
  • WuFCvon EckardsteinAAndrogens and coronary artery diseaseEndocr Rev200324218321712700179
  • GonzalesRJAnsarSDucklesSPKrauseDNAndrogenic/estrogenic balance in the male rat cerebral circulation: metabolic enzymes and sex steroid receptorsAm J Physiol Heart Circ Physiol2005289H57858515764681
  • HatakeyamaHNishizawaMNakagawaANakanoSKigoshiTUchidaKTestosterone inhibits tumor necrosis factor-α-induced vascular cell adhesion molecule-1 expression in human aortic endothelial cellsFEBS Lett20025301–312913212387879
  • ZhangXWangLYJiangTYEffects of testosterone and 17-beta-estradiol on TNF-alpha-induced E-selectin and VCAM-1 expression in endothelial cells. Analysis of the underlying receptor pathwaysLife Sci2002711152912020745
  • DeathAKMcgrathKCSaderMADihydrotestosterone promotes vascular cell adhesion molecule-1 expression in male human endothelial cells via a nuclear factor-kappaB-dependent pathwayEndocrinology200414541889189714684616
  • AnnibaliniGAgostiniDCalcabriniCEffects of sex hormones on inflammatory response in male and female vascular endothelial cellsJ Endocrinol Invest201437986186924947177
  • NorataGDTibollaGSeccomandiPMPolettiACatapanoALDihydrotestosterone decreases tumor necrosis factor-alpha and lipo-polysaccharide-induced inflammatory response in human endothelial cellsJ Clin Endocrinol Metab200691254655416317058
  • XuZRHuLChengLFQianYYangYMDihydrotestosterone protects human vascular endothelial cells from H(2)O(2)-induced apoptosis through inhibition of caspase-3, caspase-9 and p38 MAPKEur J Pharmacol20106432–325425920599910
  • MorettiCLanzollaGMorettiMGnessiLCarminaEAndrogens and Hypertension in Men and Women: a Unifying ViewCurr Hypertens Rep20171954428455674
  • AgledahlIBrodinESvartbergJHansenJBPlasma free tissue factor pathway inhibitor (TFPI) levels and TF-induced thrombin generation ex vivo in men with low testosterone levelsThromb Haemost2009101347147719277407
  • PhillipsGBPinkernellBHJingTYThe association of hypotestos-teronemia with coronary artery disease in menArterioscler Thromb Vasc Biol1994145701706
  • PughPJChannerKSParryHDownesTJoneTHBio-available testosterone levels fall acutely following myocardial infarction in men: association with fibrinolytic factorsEndocr Res200228316117312489566
  • JinHLinJFuLPhysiological testosterone stimulates tissue plasminogen activator and tissue factor pathway inhibitor and inhibits plasminogen activator inhibitor type 1 release in endothelial cellsBiochem Cell Biol200785224625117534406
  • BorstSEShusterJJZouBCardiovascular risks and elevation of serum DHT vary by route of testosterone administration: a systematic review and meta-analysisBMC Med201412121125428524
  • BasariaSCovielloADTravisonTGAdverse Events Associated with Testosterone AdministrationN Engl J Med Overseas Ed20103632109122
  • VigenRO’DonnellCIBarónAEAssociation of testosterone therapy with mortality, myocardial infarction, and stroke in men with low testosterone levelsJAMA2013310171829183624193080
  • MorgentalerALunenfeldBTestosterone and cardiovascular risk: world’s experts take unprecedented action to correct misinformationThe Aging Male2014172636524797617
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