Abolition of Hypertension-Induced End-Organ Damage by Androgen Receptor Blockade in Transgenic Rats Harboring the Mouse Ren-2 Gene

Baltatu, Ovidiu Constantin; Cayla, Cécile; Iliescu, Radu; Андреев, Д. Н.; Jordan, Cynthia L.; Bäder, Michael

doi:10.1097/01.asn.0000033327.65390.ca

Cited by 50 publications

(48 citation statements)

References 45 publications

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“…31,32 An animal model of hypertension-induced end-organ damage showed significant attenuation of renal damage by androgen receptor blockade with flutamide. 33 In uninephrectomy models, male rats developed greater proteinuria and mesangial sclerosis than did female rats. 34 Testosterone seems to amplify compensatory glomerular and tubular growth, which may promote glomerulosclerosis.…”

Section: Discussionmentioning

confidence: 99%

Development of Focal Segmental Glomerulosclerosis after Anabolic Steroid Abuse

Herlitz¹,

Markowitz²,

Farris³

et al. 2010

Journal of the American Society of Nephrology

156

108

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Anabolic steroid abuse adversely affects the endocrine system, blood lipids, and the liver, but renal injury has not been described. We identified an association of focal segmental glomerulosclerosis (FSGS) and proteinuria in a cohort of 10 bodybuilders (six white and four Hispanic; mean body mass index 34.7) after long-term abuse of anabolic steroids. The clinical presentation included proteinuria (mean 10.1 g/d; range 1.3 to 26.3 g/d) and renal insufficiency (mean serum creatinine 3.0 mg/dl; range 1.3 to 7.8 mg/dl); three (30%) patients presented with nephrotic syndrome. Renal biopsy revealed FSGS in nine patients, four of whom also had glomerulomegaly, and glomerulomegaly alone in one patient. Three biopsies revealed collapsing lesions of FSGS, four had perihilar lesions, and seven showed Ն40% tubular atrophy and interstitial fibrosis. Among eight patients with mean follow-up of 2.2 yr, one progressed to ESRD, the other seven received renin-angiotensin system blockade, and one also received corticosteroids. All seven patients discontinued anabolic steroids, leading to weight loss, stabilization or improvement in serum creatinine, and a reduction in proteinuria. One patient resumed anabolic steroid abuse and suffered relapse of proteinuria and renal insufficiency. We hypothesize that secondary FSGS results from a combination of postadaptive glomerular changes driven by increased lean body mass and potential direct nephrotoxic effects of anabolic steroids. Because of the expected rise in serum creatinine as a result of increased muscle mass in bodybuilders, this complication is likely underrecognized. INDEX CASEThe index case (patient 1) is a 30-yr-old white male professional bodybuilder who had no significant medical history and presented to a local hospital with lower extremity edema. The patient was on no prescription medications, but as part of his bodybuilding regimen, he regularly consumed a highprotein diet (Ͼ550 g/d) and dietary supplements including 10 g/d creatine monohydrate, 1000 mg/d branched-chain amino acids, 10 g/d glutamine, and multivitamins. For more than a decade, he regularly used anabolic androgenic steroids (AASs), including injectable testosterone, methyl-1-testosterone (taken orally), growth hormone, and insulin to augment his bodybuilding. At the time of biopsy, his steroid regimen consisted of growth hormone 4 IU 5 d/wk and testosterone 500 mg intramuscularly twice weekly. In addition, he took 75 mg of ephedrine and 600 mg of caffeine before each workout session.Physical examination revealed a height of 71 inches (180 cm), a weight of 295 pounds (134 kg extremely muscular, highly toned physique (Figure 1). BP was 145/80 mmHg, and there was 2ϩ bilateral lower extremity edema. The patient was found to have a serum creatinine of 2.7 mg/dl, blood urea nitrogen of 24 mg/dl, serum albumin of 1.9 g/dl, total serum protein of 5.7 g/dl, serum cholesterol of 212 mg/dl, hematocrit of 45%, and white blood cell count of 10.3 ϫ 10 9 /L with a normal differential and platelet count of 254 ϫ...

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Section: Discussionmentioning

confidence: 99%

Development of Focal Segmental Glomerulosclerosis after Anabolic Steroid Abuse

Herlitz¹,

Markowitz²,

Farris³

et al. 2010

Journal of the American Society of Nephrology

156

108

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“…Estrogen is known to downregulate both ACE and the AT 1 receptor, as well as increase the expression of the AT 2 receptor and ACE2, which may further attenuate the actions of the ACE-ANG II-AT 1 axis (3,10,17,27,33,56,59). In contrast, testosterone may increase ACE and the AT 1 receptor as well as angiotensinogen (9,27). To our knowledge, the current studies are the first to document the sex-based differential expression of both circulating and tissue ANG II and ANG-(1-7) in any hypertensive strain.…”

Section: Discussionmentioning

confidence: 99%

“…Indeed, the cardioprotective effects of estrogen replacement in mRen (2).Lewis rats, an ANG IIdependent model of hypertension, are consistent with its actions to directly attenuate key components of the RAAS, including angiotensin-converting enzyme (ACE) and the AT 1 receptor (12,40,45), as well as the increase of competing components such as ACE2 and the ANG II type 2 (AT 2 ) receptor or influence other signaling pathways (nitric oxide and prostaglandins) that may converge on the RAAS (3,11,41,60,65). Androgens, however, may also have a significant effect on cardiovascular regulation to increase blood pressure and accelerate renal injury that is associated with alterations of the RAAS, including the increased expression of renin, angiotensinogen, and ACE (6,8,9,47). Furthermore, estrogen may exhibit additional effects on the RAAS, including the stimulation of renin and angiotensinogen that in some instances may promote an increase in blood pressure (12).…”

mentioning

confidence: 99%

Sex differences in circulating and renal angiotensins of hypertensive mRen().Lewis but not normotensive Lewis rats

Pendergrass

Pirro²,

Westwood³

et al. 2008

American Journal of Physiology-Heart and Circulatory Physiology

106

145

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“…For example, renin 2 was reported to be an androgen-responsive gene (66,67). Moreover, overexpression of murine renin 2 in rats resulted in testosteronedependent hypertension (68). Furthermore, the RAAS has been suggested to have a greater impact on blood pressure regulation in males than in females: knocking out the gene encoding ACE1 decreased blood pressure in male but not female mice (69), and in a large population study, genetic linkage of the ACE locus with hypertension was found in men but not in women (70).…”

Section: Figurementioning

confidence: 99%

Genetic modifiers of hypertension in soluble guanylate cyclase α1–deficient mice

Buys¹,

Raher²,

Kirby³

et al. 2012

J. Clin. Invest.

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Nitric oxide (NO) plays an essential role in regulating hypertension and blood flow by inducing relaxation of vascular smooth muscle. Male mice deficient in a NO receptor component, the α1 subunit of soluble guanylate cyclase (sGCα 1 ), are prone to hypertension in some, but not all, mouse strains, suggesting that additional genetic factors contribute to the onset of hypertension. Using linkage analyses, we discovered a quantitative trait locus (QTL) on chromosome 1 that was linked to mean arterial pressure (MAP) in the context of sGCα 1 deficiency. This region is syntenic with previously identified blood pressure-related QTLs in the human and rat genome and contains the genes coding for renin. Hypertension was associated with increased activity of the renin-angiotensin-aldosterone system (RAAS). Further, we found that RAAS inhibition normalized MAP and improved endothelium-dependent vasorelaxation in sGCα 1 -deficient mice. These data identify the RAAS as a blood pressure-modifying mechanism in a setting of impaired NO/cGMP signaling. IntroductionSystemic arterial hypertension is one of the most widespread public health problems in the developed world and the most prevalent modifiable risk factor for cardiovascular disease (CVD) in both women and men (1). The pathogenesis of essential hypertension is multifactorial, and in the vast majority of cases the etiology of hypertension is unknown. Although major advances in the treatment of hypertension have decreased CVD-related deaths over the last decade (2), many of the molecular mechanisms underlying the development of hypertension remain elusive. Genome-wide association studies (GWAS) suggest that there is a substantial heritable component to blood pressure (3, 4). Although GWAS have identified several loci associated with blood pressure in human beings, including loci containing genes that either regulate cGMP levels (4-7) or the renin-angiotensin-aldosterone system (RAAS) (8), many of the genetic factors determining blood pressure and how these factors interact remain to be identified.Renal abnormalities, such as decreased urinary sodium excretion in response to increasing renal perfusion pressure, and increased activity of the RAAS are generally considered to be a major contributor to the development of high blood pressure (9). However, other studies support the idea that hypertension can arise from primary vascular abnormalities (10, 11). The ability of NO to relax vascular smooth muscle and its essential role in the regulation of blood flow are well characterized (12, 13). Ample evidence suggests that altered NO signaling is involved in the pathogenesis of hypertension (14).One of the primary receptors for NO is soluble guanylate cyclase (sGC), a heme-containing enzyme that generates cGMP. The

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Abolition of Hypertension-Induced End-Organ Damage by Androgen Receptor Blockade in Transgenic Rats Harboring the Mouse Ren-2 Gene

Cited by 50 publications

References 45 publications

Development of Focal Segmental Glomerulosclerosis after Anabolic Steroid Abuse

Development of Focal Segmental Glomerulosclerosis after Anabolic Steroid Abuse

Sex differences in circulating and renal angiotensins of hypertensive mRen().Lewis but not normotensive Lewis rats

Genetic modifiers of hypertension in soluble guanylate cyclase α1–deficient mice

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