Prostatic ischemia induces ventral prostatic hyperplasia in the SHR; possible mechanism of development of BPH

Saito, Motoaki; Tsounapi, Panagiota; Oikawa, Ryo; Shimizu, Shogo; Honda, Masashi; Sejima, Takehiro; Kinoshita, Yukako; Tomita, Shuhei

doi:10.1038/srep03822

Cited by 58 publications

(81 citation statements)

References 41 publications

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“…Moreover, it has been reported that SHR exhibit a lower basal bladder perfusion than normotensive Wistar Kyoto rats, a frequently used control strain in SHR studies; treatment of SHR with doxazosin increased perfusion and expression of NO synthase (which chronically may facilitate perfusion), whereas treatment with nifedipine did not (Yono et al 2007). The study also showed reduced prostate perfusion in SHR, a finding confirmed in a separate study (Saito et al 2014). In the latter study, treatment with nicorandil restored prostate perfusion and concomitantly reduced the elevated expression of hypoxia-inducible factor 1α, transforming growth factor β1, and basic fibroblast growth factor.…”

Section: Clinical Associations Between Atherosclerosis Risk Factors Amentioning

confidence: 55%

“…The rho-kinase inhibitor Y 27,632 is a known vasodilator, at least in hypertensive animals, and along with a reduction of systemic blood pressure reduced detrusor overactivity in spontaneously hypertensive rats (Rajasekaran et al 2005); however, this may reflect direct effects of rho-kinase inhibition on detrusor smooth muscle function (Peters et al 2006). Possibly more interesting are findings with nicorandil, which reduced prostate weight and increased prostate perfusion in SHR in the absence of effects on systemic blood pressure (Saito et al 2014). Limited clinical data show that a combination of the α 1 -adrenoceptor antagonist terazosin and the Ca 2+ -entry blocker amlodipine yielded superior blood pressure and LUTS reduction than either monotherapy in a group of 355 men (Liu et al 2009).…”

Section: Effects Of Therapeutics On Bladder Perfusionmentioning

confidence: 94%

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Are blood vessels a target to treat lower urinary tract dysfunction?

Michel

Chess-Williams

Hegde

2015

Naunyn-Schmiedeberg's Arch Pharmacol

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Bladder dysfunction is common in the general population (Stewart et al. 2010) and even more so among patients seeing a physician for any reason (Goepel et al. 2002). It often manifests as lower urinary tract symptoms (LUTS), a term originally coined to describe voiding and storage symptoms in men with benign prostatic hyperplasia (BPH) but now more universally used to describe any type of voiding and storage symptoms in both sexes. Studies into possible causes of urinary bladder dysfunction have long focused on detrusor smooth muscle cells (Turner and Brading 1999). More recently, it became clear that several other types of cells and organs contribute to regulating detrusor smooth muscle function. These include the urothelium (Andersson and McCloskey 2014; Michel 2015), afferent nerves (Michel and Igawa 2015; Yoshimura et al. 2014b), and the central and autonomic nervous systems (Fowler and Griffiths 2010; Yoshimura et al. 2014a). Alterations in any of these may at least partly be responsible for detrusor dysfunction and, accordingly, be potential targets for the treatment of bladder dysfunction. As highlighted by an article in this issue of Naunyn-Schmiedeberg's Archives of Pharmacology (Bayrak et al. 2015), there is an additional suspect, the bladder vasculature. This article will discuss the currently available experimental and clinical evidence for a role of the vasculature in causing bladder dysfunction, and how existing and emerging treatments may modulate bladder function by acting on blood vessels. Due to a similarity in concept, data on prostate perfusion will also be discussed to some extent.

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Section: Clinical Associations Between Atherosclerosis Risk Factors Amentioning

confidence: 55%

Section: Effects Of Therapeutics On Bladder Perfusionmentioning

confidence: 94%

Are blood vessels a target to treat lower urinary tract dysfunction?

Michel

Chess-Williams

Hegde

2015

Naunyn-Schmiedeberg's Arch Pharmacol

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“…In the atherosclerosis-induced chronic bladder ischemia rat model, the resulting detrusor overactivity leads to an increase in the voiding frequency (18). Since atherosclerosis is thought to be a risk factor for benign prostatic hyperplasia (BPH), it has been suggested that there is a relationship between high vascular resistance and the development of BPH (12,23). Therefore, it is thought that the hypertension and/or arteriosclerosis that reduces arterial blood flow and subsequently causes ischemia will induce BPH or overactive bladder.…”

mentioning

confidence: 99%

“…Rats were anesthetized with urethane (0.6 g/kg subcutaneously) and placed in a restraining cage (NAIGAI-CFK-1P; NMS, Tokyo, Japan), after which a polyethylene catheter (PE50; Clay Adams, NJ, USA) was inserted transurethrally into the bladder. This catheter was then connected to an infua lower prostate blood flow and have an increased prostate size (23). In the atherosclerosis-induced chronic bladder ischemia rat model, the resulting detrusor overactivity leads to an increase in the voiding frequency (18).…”

mentioning

confidence: 99%

<b>Naftopidil improves locomotor activity and urinary frequency in rats with pelvic venous </b><b>congestion </b>

Sugaya¹,

Nishijima²,

Kadekawa³

et al. 2016

Biomed. Res.

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The α1D/A receptor antagonist, naftopidil, inhibits micturition reflex by acting on various different sites. We examined the effects of naftopidil on bladder activity and changes in the induced urinary frequency using female rats with pelvic venous congestion (PC). Twenty-four female rats were divided into sham, PC, and PC/naftopidil groups. After anesthetizing rats in the PC and PC/naftopidil groups, the bilateral common iliac veins and uterine veins were ligated. Rats in the sham and PC groups were fed a standard diet, while rats in the PC/naftopidil group were fed diets containing 0.04% naftopidil. After 4 weeks of treatment, locomotor activity, urinary nitric oxide metabolites (NOx), continuous cystometry, and plasma monoamine measurements were performed. PC rats exhibited a decrease of locomotor activity, a shorter interval between bladder contractions on continuous cystometry, and decreased urinary NOx and plasma serotonin levels than the sham rats. The PC/naftopidil rats exhibited an increase of locomotor activity, a longer interval between bladder contractions, and increased urinary NOx and plasma serotonin levels. Therefore, naftopidil might improve bladder dysfunction induced by pelvic venous congestion due to several actions in the central nervous system and bladder tissue, as well as acting as an α1 blocker to cause pelvic venous dilation.Unilateral or bilateral ovarian vein incompetence can cause pelvic congestion syndrome, which induces chronic pain, irritable bladder, dysfunction of the pelvic organs, or vulval varices and varicose veins in the lower limbs (1, 5, 7). Our previous study demonstrated that chronic prostatitis and stress urinary incontinence were related to the existence of vena cava reflux caused by tricuspid regurgitation (28). When we examined a female case with pelvic congestion syndrome using external iliac venography, we found that pelvic venous congestion occurred with tricuspid regurgitation and without pelvic venous valves (25). Our previous studies have also demonstrated that ligation of the bilateral common iliac veins in male rats or ligation of the bilateral common iliac veins and uterine veins in female rats induced changes in the urinary frequency and low locomotor activity (30). As compared to the intact rats, these surgically altered rats exhibited a bladder blood flow decrease that was about 80% of the flow in the intact bladder. Therefore, pelvic venous congestion may be one of the causes of pelvic ischemia, and might be related to several lower urinary tract symptoms/diseases. When examining hypertension, the relevance of lower urinary tract symptoms and their association with hypertension need to be taken into consideration. Spontaneously hypertensive rats have been shown to have a significantly lower bladder capacity and voiding volume (24), and these rats also exhibit

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“…In the last decade, the pathogenesis of BPH began to consider from the perspective of vascular dysfunction, for instance, age might activate systemic vascular risk factors, resulting in disturbed blood flow (7) , furthermore, development of prostatic hyperplasia may be associated with prostatic hypoxia (8) , and with a correlation between pelvic ischemia and lower urinary tract symptoms in elderly men (9) , and also increasing the pressure in the prostate (10) . Dr. Allen's research on the Origin of Diseases identifies the causal root of prostate enlargement, namely capillary expansion.…”

Section: Introductionmentioning

confidence: 99%

Efficacy and Safety of Thermobalancing Therapy in Men with Lower Urinary Tract Symptoms/Benign Prostatic Hyperplasia was Confirmed by Clinical Trial

2016

ARC Journal of Urology

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Prostatic ischemia induces ventral prostatic hyperplasia in the SHR; possible mechanism of development of BPH

Cited by 58 publications

References 41 publications

Are blood vessels a target to treat lower urinary tract dysfunction?

Are blood vessels a target to treat lower urinary tract dysfunction?

<b>Naftopidil improves locomotor activity and urinary frequency in rats with pelvic venous </b><b>congestion </b>

Efficacy and Safety of Thermobalancing Therapy in Men with Lower Urinary Tract Symptoms/Benign Prostatic Hyperplasia was Confirmed by Clinical Trial

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