Expression of cavernous transforming growth factor‐<i>β</i><sub>1</sub> and its Type II Receptor in patients with erectile dysfunction

Ryu, Ji‐Kan; Han, Jee‐Young; Chu, Young‐Chae; Song, Sun U.; Lee, Kwan-Hee; Yoon, Sang Min; Suh, Jun‐Kyu; Kim, Seong‐Jin

doi:10.1046/j.0105-6263.2003.00447.x

Cited by 41 publications

(52 citation statements)

References 31 publications

(27 reference statements)

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“…Furthermore, it was reported that p42/44 kinase is a downstream effector of the transforming growth factor-beta 1 (TGF-b1) signaling pathway (He et al 2010). TGF-b1 expression is increased in aging trabecular fibroblasts and reported to be the main stimulator of collagen synthesis, inducing cavernosal fibrosis and promoting ED (Ferrini et al 2007;Ryu et al 2004). We hypothesize that increased p42/44 activation in aged ECM component may be a downstream event of the TGF-b1 pathway, adding a new piece in the complex puzzle of aging CC signaling events.…”

Section: Discussionmentioning

confidence: 88%

Erectile tissue molecular alterations with aging—differential activation of the p42/44 MAP Kinase pathway

Castela

Soares

Rocha

et al. 2010

AGE

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Erectile dysfunction (ED) is a common problem in aged men; however, the molecular events involved in aging ED remain unclear. To better characterize the effects of aging in the penis, we evaluated cavernosal tissue remodeling capability and the downstream activation of the intracellular signaling mediator mitogen-activated protein p42/44 kinase (p42/44 MAPK). We used male Wistar rats, which were divided in groups of 2, 6, 12, 18, and 24 months old. Penile tissues were harvested and processed for protein isolation and immunohistochemical analysis. Cavernosal viability was assessed by TUNEL assay, and proliferation was analyzed by immunohistochemical detection of proliferating cell nuclear antigen (PCNA). Immunolocalization of the activated form of p42/44 MAPK was evaluated by immunofluorescence, and changes in its phosphorylation status were quantified by western blotting. p42/44 phosphorylation profile was also assessed in situ in human young and elderly cavernosal samples. With the advancement of age, experimental cavernosal tissue remodeling was affected by an age-dependent unbalance between the rate of apoptosis and proliferation, in all erectile components. Moreover, this turnover alteration was accompanied by significant modifications in the activation profile of the downstream effector p42/44 MAPK. In the youngest corporeal samples, p42/44 was mostly activated at perivascular sites, potentially mediating cell survival/proliferation. However, in elderly experimental erectile tissue, p42/44 phosphorylation shifted to trabecular fibroblasts, indicating a potential role in extracellular matrix (ECM) production. More importantly, the same differential pattern of p42/44 activation was observed in human young and aged cavernosal fragments, suggesting a distinct function of this protein with aging. We provided evidence for the first time that with the advancement of age, there is a differential activation of p42/44 MAPK in cavernosal tissue, which may promote ECM expansion and fibrosis, therefore compromising erectile function in the elderly.

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Section: Discussionmentioning

confidence: 88%

Erectile tissue molecular alterations with aging—differential activation of the p42/44 MAP Kinase pathway

Castela

Soares

Rocha

et al. 2010

AGE

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“…[32][33][34] Clinical studies have shown that cavernosal TGFbeta1 expression is significantly greater in vasculogenic ED patients than in the control subjects or psychogenic ED patients. 35 TGF-beta1 type II receptor expression was also found to be significantly greater in vasculogenic ED compared with control subjects and patients with psychogenic and neurogenic ED. 35 Patients with vascular risk factors such as hyperlipidemia and atherosclerosis were found to have significantly greater degrees of cavernosal fibrosis than those without these conditions.…”

Section: Changes In Tgf-beta Expressionmentioning

confidence: 82%

“…35 TGF-beta1 type II receptor expression was also found to be significantly greater in vasculogenic ED compared with control subjects and patients with psychogenic and neurogenic ED. 35 Patients with vascular risk factors such as hyperlipidemia and atherosclerosis were found to have significantly greater degrees of cavernosal fibrosis than those without these conditions. 35 Furthermore, this study has shown that the abundance of collagen fibers closely correlates with both TGF-beta1 and TGF-beta1 receptor II expression, suggesting a role of TGF-beta1 and its receptor II in cavernosal fibrosis in vasculogenic ED patients.…”

Section: Changes In Tgf-beta Expressionmentioning

confidence: 82%

“…35 Furthermore, this study has shown that the abundance of collagen fibers closely correlates with both TGF-beta1 and TGF-beta1 receptor II expression, suggesting a role of TGF-beta1 and its receptor II in cavernosal fibrosis in vasculogenic ED patients. 35 Exogenous treatment with TGF-beta has been shown to induce a 2.5-to 4.5-fold increase in the synthesis of types I and III collagen. 36 This effect was reduced by adding the eicosanoid PGE1.…”

Section: Changes In Tgf-beta Expressionmentioning

confidence: 94%

“…35 Patients with vascular risk factors such as hyperlipidemia and atherosclerosis were found to have significantly greater degrees of cavernosal fibrosis than those without these conditions. 35 Furthermore, this study has shown that the abundance of collagen fibers closely correlates with both TGF-beta1 and TGF-beta1 receptor II expression, suggesting a role of TGF-beta1 and its receptor II in cavernosal fibrosis in vasculogenic ED patients. 35 Exogenous treatment with TGF-beta has been shown to induce a 2.5-to 4.5-fold increase in the synthesis of types I and III collagen.…”

Section: Changes In Tgf-beta Expressionmentioning

confidence: 99%

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Oxidative Stress and Molecular Reactions in Arteriogenic Erectile Dysfunction

Azadzoi

Siroky

2009

Chonnam Med J

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Vascular disorders are the leading causes of organic erectile dysfunction (ED). Most cases of arteriogenic ED are associated with vascular risk factors such as hypercholesterolemia, atherosclerosis, diabetes mellitus, hypertension, and smoking. These conditions impair vascular structure directly or indirectly by facilitating oxidative damage due to accumulation of reactive oxygen and nitrogen species such as superoxide (O 2 − ), hydrogen peroxide (H 2 O 2 ), hydroxyl radicals and peroxynitrite (O=NOO − ). Clinical studies have shown that the degree of arteriogenic ED cannot be predicted exclusively by the arterial integrity, suggesting that it involves local changes within penile smooth muscle cells, endothelium, nerves, and microvasculature. It is thought that arterial occlusion and subsequent lack of erectile tissue perfusion, nutrient deficiency, hypoxia, and accumulation of waste products constitute an environment hospitable to free radical formation and detrimental to nitric oxide (NO) bioavailability. Studies of animal and cell culture models have revealed that exposure to ischemia and hypoxia triggers a cascade of cellular and molecular changes in the erectile tissue with devastating impact on its structure and function. These alterations involve cytotoxic radicals, nitric oxide synthase (NOS), eicosanoids, neurotoxic elements, and growth factors and lead to impairment of NO/cGMP pathway, smooth muscle dysfunction, microvascular damage, and neurodegeneration. Ultimately, these events lead to erectile tissue fibrosis and the failure of penile veno-occlusive mechanism. These local changes in the hypoxic erectile tissue may explain the failure of revascularization surgery to completely cure arteriogenic ED and imply the need for newer therapeutic strategies to remove cytotoxic and neurotoxic elements from the chronically ischemic penis.

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Sonic hedgehog delivery from self-assembled nanofiber hydrogels reduces the fibrotic response in models of erectile dysfunction

et al. 2016

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Erectile dysfunction (ED) is a serious medical condition in which current treatments are ineffective in prostatectomy and diabetic patients, due to injury to the cavernous nerve (CN), which causes irreversible remodeling of the penis (decreased smooth muscle and increased collagen), through a largely undefined mechanism. We propose that sonic hedgehog (SHH) and neural innervation, are indispensable regulators of collagen in the penis, with decreased SHH protein being an integral component of the fibrotic response to loss of innervation. We examined collagen abundance and morphology in control (Peyronie’s), prostatectomy and diabetic patients, and in rat models of penile development, CN injury, SHH inhibition and under regenerative conditions, utilizing self-assembling peptide amphiphile (PA) nanofiber hydrogels for SHH delivery. Collagen abundance increased in penis of ED patients. In rats, collagen increased with CN injury in a defined time frame independent of injury severity. An inverse relationship between SHH and collagen abundance was identified; SHH inhibition increased and SHH treatment decreased penile collagen. SHH signaling in the pelvic ganglia (PG)/CN is important to maintain CN integrity and when inhibited, down stream collagen induction occurs. Collagen increased throughout penile development and with age, which is important when considering how to treat fibrosis clinically. These studies show that SHH PA treatment reduces collagen under regenerative post-prostatectomy conditions, indicating broad application for ED prevention in prostatectomy, diabetic and aging patients and in other peripheral nerve injuries. The PA nanofiber protein vehicle may be widely applicable as an in vivo delivery tool.

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Expression of cavernous transforming growth factor‐β₁ and its Type II Receptor in patients with erectile dysfunction

Cited by 41 publications

References 31 publications

Erectile tissue molecular alterations with aging—differential activation of the p42/44 MAP Kinase pathway

Erectile tissue molecular alterations with aging—differential activation of the p42/44 MAP Kinase pathway

Oxidative Stress and Molecular Reactions in Arteriogenic Erectile Dysfunction

Sonic hedgehog delivery from self-assembled nanofiber hydrogels reduces the fibrotic response in models of erectile dysfunction

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Expression of cavernous transforming growth factor‐β1 and its Type II Receptor in patients with erectile dysfunction

Cited by 41 publications

References 31 publications

Erectile tissue molecular alterations with aging—differential activation of the p42/44 MAP Kinase pathway

Erectile tissue molecular alterations with aging—differential activation of the p42/44 MAP Kinase pathway

Oxidative Stress and Molecular Reactions in Arteriogenic Erectile Dysfunction

Sonic hedgehog delivery from self-assembled nanofiber hydrogels reduces the fibrotic response in models of erectile dysfunction

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Expression of cavernous transforming growth factor‐β₁ and its Type II Receptor in patients with erectile dysfunction