The first‐generation phosphodiesterase 5 inhibitors and their pharmacokinetic issue

Zucchi, Alessandro; Costantini, Elisabetta; Scroppo, Fabrizio Ildefonso; Silvani, Mauro; Kopa, Zsolt; Illiano, Ester; Petrillo, Maria Grazia; Cari, Luigi; Nocentini, Giuseppe

doi:10.1111/andr.12683

Cited by 20 publications

(15 citation statements)

References 77 publications

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“…This suggests that PDE5 may serve as a potentially promising target for the treatment of BPH/LUTS ( 13 , 14 ). However, since PDE5 is ubiquitously expressed in the human body and participates in a number of physiological and pathological processes in numerous tissues or organs, inhibition of PDE5 using traditional inhibitors may induce various adverse side effects ( 15 , 16 ). Therefore, an effective inhibitor targeting PDE5 that causes fewer adverse side effects is required.…”

Section: Introductionmentioning

confidence: 99%

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca²⁺ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia

Jiang

et al. 2021

Exp Ther Med

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Section: Introductionmentioning

confidence: 99%

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca²⁺ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia

Jiang

et al. 2021

Exp Ther Med

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“…Pharmacological intervention into intracellular pathways regulating smooth muscle tone has become a common strategy in urology for relief of symptoms caused by dysfunctions of the urogenital tract. Based on the physiological mechanisms regulating the male genital tract, vasoactive drugs (such as selective PDE5 inhibitors or prostaglandin E1) modulating signal transduction cascades represent a straightforward logical approach for effectively treating ED of various origins (vasculogenic/neurogenic/psychogenic) in a significant number of patients [62]. While some strategies of treatment target the cyclic GMP system, other approaches take into account the cyclic AMP system.…”

Section: Resultsmentioning

confidence: 99%

The Use of Vasoactive Drugs in the Treatment of Male Erectile Dysfunction: Current Concepts

Kedia

Ückert

Tsikas

et al. 2020

JCM

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It is widely accepted that disorders of the male (uro)genital tract, such as erectile dysfunction (ED) and benign diseases of the prostate (lower urinary tract symptomatology or benign prostatic hyperplasia), can be approached therapeutically by influencing the function of both the vascular and non-vascular smooth muscle of the penile erectile tissue or the transition zone/periurethral region of the prostate, respectively. As a result of the discovery of nitric oxide (NO) and cyclic guanosine monophosphate (GMP) as central mediators of penile smooth muscle relaxation, the use of drugs known to increase the local production of NO and/or elevate the intracellular level of the second messenger cyclic GMP have attracted broad attention in the treatment of ED of various etiologies. Specifically, the introduction of vasoactive drugs, including orally active inhibitors of the cyclic GMP-specific phosphodiesterase (PDE) 5, has offered great advantage in the pharmacotherapy of ED and other diseases of the genitourinary tract. These drugs have been proven efficacious with a fast on-set of action and an improved profile of side-effects. This review summarizes current strategies for the treatment of ED utilizing the application of vasoactive drugs via the oral, transurethral, topical, or self-injection route.

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“…Nonetheless, despite this high selectivity, each of these drugs inhibits other PDE isoenzymes to some extent. Sildenafil and vardenafil, for example, have shown only 10 and 15 times lower specificity for PDE6 than for PDE5, respectively (reviewed in [ 14 ]), which could be explained by the fact that the kinetic and catalytic properties of PDE6 are very similar to those of PDE5 [ 15 , 16 , 17 ].…”

Section: Introductionmentioning

confidence: 99%

“…In addition to the three drugs mentioned above, the second-generation inhibitor avanafil (Stendra ® ) became internationally available in 2013. Avanafil exhibited 100 times lower specificity for PDE6 than for PDE5, presumably reducing the potential side effects derived from the nonselective inhibition of PDE6 by sildenafil and vardenafil (reviewed in [ 14 ]). Other second-generation (udenafil and mirodenafil) or third-generation (lodenafil, SLX-2101, JNJ-10280205, and JNJ-10287069) PDE5 inhibitors have been either approved and introduced into the market in some parts of the world or are at the final stages of their clinical development.…”

Section: Introductionmentioning

confidence: 99%

Visual Side Effects Linked to Sildenafil Consumption: An Update

2021

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Phosphodiesterase type 5 (PDE5) inhibitors such as Viagra® (sildenafil citrate) have demonstrated efficacy in the treatment of erectile dysfunction (ED) by inducing cyclic guanosine monophosphate (cGMP) elevation followed by vasodilation and increased blood flow. It also exerts minor inhibitory action against PDE6, which is present exclusively in rod and cone photoreceptors. The effects of sildenafil on the visual system have been investigated in a wide variety of clinical and preclinical studies due to the fact that a high dose of sildenafil may cause mild and transient visual symptoms in some patients. A literature review was performed using PubMed, Cochrane Library and Clinical Trials databases from 1990 up to 2020, focusing on the pathophysiology of visual disorders induced by sildenafil. The aim of this review was not only to gather and summarize the information available on sildenafil clinical trials (CTs), but also to spot subpopulations with increased risk of developing undesirable visual side effects. This PDE inhibitor has been associated with transient and reversible ocular side effects, including changes in color vision and light perception, blurred vision, photophobia, conjunctival hyperemia and keratitis, and alterations in the electroretinogram (ERG). Sildenafil may induce a reversible increase in intraocular pressure (IOP) and a few case reports suggest it is involved in the development of nonarteritic ischemic optic neuropathy (NAION). Reversible idiopathic serous macular detachment, central serous retinopathy and ERG disturbances have been related to the significant impact of sildenafil on retinal perfusion. So far, sildenafil does not seem to cause permanent toxic effects on chorioretinal tissue and photoreceptors as long as the therapeutic dose is not exceeded and is taken under a physician’s direction to treat a medical condition. However, the recreational use of sildenafil can lead to harmful side effects, including vision changes.

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The first‐generation phosphodiesterase 5 inhibitors and their pharmacokinetic issue

Cited by 20 publications

References 77 publications

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca²⁺ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca²⁺ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia

The Use of Vasoactive Drugs in the Treatment of Male Erectile Dysfunction: Current Concepts

Visual Side Effects Linked to Sildenafil Consumption: An Update

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The first‐generation phosphodiesterase 5 inhibitors and their pharmacokinetic issue

Cited by 20 publications

References 77 publications

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca2+ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca2+ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia

The Use of Vasoactive Drugs in the Treatment of Male Erectile Dysfunction: Current Concepts

Visual Side Effects Linked to Sildenafil Consumption: An Update

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Product

Resources

About

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca²⁺ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia

Effects of shRNA‑mediated silencing of PDE5A3 on intracellular cGMP and free Ca²⁺ levels and human prostate smooth muscle cell proliferation from benign prostatic hyperplasia