Abstract

BackgroundThe relationship between chronic prostatitis/chronic pelvic pain syndrome (CP/CPPS) and erectile dysfunction (ED) has been shown in many studies. However, the specific mechanism remains unclear. This study was to investigate the corpus cavernosum smooth muscle cell function and phenotype transformation in Experimental autoimmune prostatitis (EAP) rats.MethodsEAP was induced in rats by using prostate protein supplemented with immuneadjuvant extraction, and the max-ICP and MAP were measured. IHC and Masson staining were done to assess inflammatory infiltration and collagen deposition in the corpus cavernosum, respectively. Subsequently, normal rat and EAP rat CCSMCs were purified by tissue block implantation and differential adherence method. The oxidative stress, smooth muscle phenotype transformation, cell cycle and intracellular calcium ion transport were also evaluated.ResultsThe ratio of max ICP/MAP in EAP rats significantly reduced, and the TNF-α content and collagen deposition in the corpus cavernosum markedly increased as compared to healthy rats. High-purity rat CCSMCs were obtained. Oxidative stress was evident and the cGMP content decreased in the EAP rat CCSMCs. The expression of Cav1.2, IP3R1 and RyR2 increased, but the SERCA2 expression decreased in EAP rat CCSMCs, which was accompanied by increased intracellular calcium. Increased expression of OPN, collagen and KCa3.1, decreased Calponin expression and increased proportion of cells in the S phase were also observed in the EAP rat CCSMCs.ConclusionCP causes oxidative stress and imbalance of intracellular calcium in CCSMCs and promotes CCSMCs transformation from contractile to synthetic state, which may be involved in the pathogenesis of ED.

Highlights

  • Prostatitis is one of common urological diseases in men younger than 50 years and may significantly affect the quality of life in these patients [1]

  • This study investigated the intracellular calcium and phenotype transformation of Corpus cavernosum smooth muscle cells (CCSMCs) in Experimental autoimmune prostatitis (EAP) rats, which may provide evidence on the pathogenesis of erectile dysfunction (ED) in EAP rats

  • Effect of Chronic prostatitis/ chronic pelvic pain syndrome (CP/CPPS) on erectile function in rats There were no significant differences in the body weight (517.12 ± 8.63 g vs 506.28 ± 7.98 g, A) and penis weight (374.71 ± 13.22 mg vs 368.05 ± 8.92 mg, B) between normal control rats and EAP rats

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Summary

Introduction

Prostatitis is one of common urological diseases in men younger than 50 years and may significantly affect the quality of life in these patients [1]. Chronic prostatitis/ chronic pelvic pain syndrome (CP/CPPS) is the most common type of prostatitis [2], and about 15% of men (2020) 17:2 proposed [5, 6]. The underlying mechanism underlying the relationship between prostatitis and ED remains unclear. Corpus cavernosum is composed of endothelial-lined sinusoids which are surrounded by fibrous tissues and smooth muscles. Corpus cavernosum smooth muscle cells (CCSMCs) account for 38.5–52.0% of total cells in the corpus cavernosum [10]. Little is known about whether prostatitis causes ED via damaging CCSMCs. The relationship between chronic prostatitis/chronic pelvic pain syndrome (CP/CPPS) and erectile dysfunction (ED) has been shown in many studies. This study was to investigate the corpus cavernosum smooth muscle cell function and phenotype transformation in Experimental autoimmune prostatitis (EAP) rats

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