Department of Urology, Qilu Hospital, Cheeloo College of Medicine, Shandong University, Jinan, 250012, Shandong, China.
Key Laboratory of Urinary Precision Diagnosis and Treatment in Universities of Shandong, Jinan, 250012, Shandong, China.
World J Urol. 2023 Nov;41(11):3019-3026. doi: 10.1007/s00345-023-04587-6. Epub 2023 Sep 9.
To investigate the difference in gut microbiome composition between patients with chronic prostatitis/chronic pelvic pain syndrome (CP/CPPS) and healthy controls, and to assess the potential of gut microbiota as predictive markers for CP/CPPS risk.
The present study included 41 CP/CPPS patients and 43 healthy controls in China. Fecal specimen data were obtained and analysed using 16S rRNA gene sequencing. Alpha and beta-diversity indices, relative microbiome abundances, cluster analysis, and linear discriminant analysis effect size (LEfSe) were employed. Microbial biomarkers were selected for the development of a diagnostic classification model, and the functional prediction was conducted using PICRUSt2.
Alpha-diversity measures revealed no statistically significant difference in bacterial community structure between CP/CPPS patients and controls. However, significant differences were observed in the relative abundances of several bacterial genera. Beta-diversity analysis revealed a distinct separation between the two groups. Significant inter-group differences were noted at various taxonomic levels, with specific bacterial genera being significantly different in abundance. The LEfSe analysis indicated that three bacterial species were highly representative and seven bacterial species were low in CP/CPPS patients as compared to the control group. A diagnostic model for CP/CPPS based on microbial biomarkers exhibited good performance. PICRUSt2 functional profiling indicated significant differences in the development and regeneration pathway.
Significant differences in the gut microbiome composition were found between groups. The study provided a novel diagnostic model for CP/CPPS based on microbiota, presenting promising potential for future therapeutic targets and non-invasive diagnostic biomarkers for CP/CPPS patients.
研究慢性前列腺炎/慢性骨盆疼痛综合征(CP/CPPS)患者与健康对照者肠道微生物组组成的差异,并评估肠道微生物群作为 CP/CPPS 风险预测标志物的潜力。
本研究纳入了中国的 41 例 CP/CPPS 患者和 43 例健康对照者。采集粪便标本,采用 16S rRNA 基因测序进行分析。采用α和β多样性指数、相对微生物丰度、聚类分析和线性判别分析效应量(LEfSe)进行分析。选择微生物标志物建立诊断分类模型,并使用 PICRUSt2 进行功能预测。
α多样性测量结果显示 CP/CPPS 患者和对照组之间细菌群落结构无统计学显著差异。然而,在几个细菌属的相对丰度方面观察到显著差异。β多样性分析显示两组之间存在明显分离。在不同分类水平上均观察到显著的组间差异,特定细菌属的丰度存在显著差异。LEfSe 分析表明,与对照组相比,CP/CPPS 患者中有 3 种细菌高度代表,7 种细菌丰度较低。基于微生物标志物的 CP/CPPS 诊断模型表现出良好的性能。PICRUSt2 功能分析表明,在发展和再生途径方面存在显著差异。
CP/CPPS 患者和对照组之间肠道微生物组组成存在显著差异。该研究为基于微生物组的 CP/CPPS 提供了一种新的诊断模型,为 CP/CPPS 患者的未来治疗靶点和非侵入性诊断生物标志物提供了有前景的潜力。
