New therapeutic targets to prevent benign prostatic enlargement and symptomatic progression to benign prostatic obstruction—ICI‐RS 2023

Author:

Kanai Anthony12ORCID,Chakrabarty Basu3ORCID,Winder Michael4,Hashim Hashim5ORCID,Wein Alan6,Abrams Paul5ORCID,Fry Christopher3ORCID

Affiliation:

1. Department of Medicine University of Pittsburgh Pittsburgh Pennsylvania US

2. Department of Pharmacology & Chemical Biology University of Pittsburgh Pittsburgh Pennsylvania US

3. School of Physiology, Pharmacology & Neuroscience University of Bristol Bristol UK

4. Department of Pharmacology University of Gothenburg Gothenburg SE

5. Bristol Urological Institute North Bristol NHS Trust Bristol UK

6. Desai Sethi Institute of Urology University of Miami Miller School of Medicine Miami Florida US

Abstract

AbstractAimsBenign prostatic enlargement (BPE) can impact lower urinary tract function due to its potential progression to benign prostatic obstruction (BPO). Treatment options include removal of the obstruction by surgery or through use of therapeutics designed to slow growth or reduce tissue stress imposed by muscular stromal components. Inflammation and development of fibrosis can also raise intrinsic tissue stress within the gland, further impacting obstruction. Outflow tract obstruction can also impact emission and ejaculation if the obstruction persists.MethodsThis review summarizes an ICI‐RS think tank considering novel drug treatments that might address BPO caused by progressive development of BPE, as well as manage decompensation changes to bladder function.ResultsTopics included recent advances in our understanding of pathological changes occurring to the prostate and other lower urinary tract tissues during progressive development of BPE, and how prevention or reversal might benefit from the identification of novel drug targets. These included contractile properties of prostatic tissues, the impact of BPE and its effects on bladder function, the deposition of intramural fibrotic tissue with protracted BPO, the role of inflammation in the development of BPE and its progression to BPO. In particular, we discussed current therapeutic options for treating BPE/BPO, and new therapeutic targets, what they treat and their advantage over current medications.ConclusionSeveral new drug targets were identified, including soluble guanylate cyclase (sGC), the receptor for nitric oxide (NO•), and sGC activators that promotes sGC‐mediated cGMP production when sGC is inactivated and unresponsive to NO•.

Funder

National Institutes of Health

Publisher

Wiley

Subject

Urology,Neurology (clinical)

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