慢性前列腺炎/慢性盆腔疼痛综合征会诱导前列腺分泌物和血浆中的代谢组发生变化。

Asian journal of andrology Pub Date : 2025-01-01 Epub Date: 2024-08-09 DOI:10.4103/aja202434
Fang-Xing Zhang, Xi Chen, De-Cao Niu, Lang Cheng, Cai-Sheng Huang, Ming Liao, Yu Xue, Xiao-Lei Shi, Zeng-Nan Mo
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引用次数: 0

摘要

慢性前列腺炎/慢性盆腔疼痛综合征(CP/CPPS)是一种复杂的疾病,通常伴有心理健康障碍。然而,CP/CPPS 异质性临床表现的潜在机制仍不确定。本研究分析了表达性前列腺分泌物(EPS)和血浆的广泛靶向代谢组学数据,以揭示 CP/CPPS 的潜在病理机制。本研究共纳入了南宁市第二人民医院(中国南宁)的 24 名 CP/CPPS 患者和广西医科大学第一附属医院(中国南宁)的 35 名无症状对照者。研究人员记录了与 CP/CPPS 和精神症状相关的指标。通过差异分析、共表达网络分析和相关分析,确定了患者体内发生特异性改变并与 CP/CPPS 不同表型相关的代谢物。研究还进一步探讨了 EPS 与血浆之间的重要联系。CP/CPPS 患者 EPS 的代谢组学数据与对照组有显著差异。通路分析显示,EPS 中氨基酸代谢、脂质代谢和柠檬酸循环失调。研究发现,色氨酸代谢途径是与 CP/CPPS 不同表型相关的改变最明显的途径。此外,研究还发现色氨酸和酪氨酸代谢失调以及血浆中氧化应激相关代谢物的升高有效地阐明了 CP/CPPS 抑郁症的发展过程。总体而言,患者 EPS 和血浆中的代谢组学改变主要与氧化损伤、能量代谢异常、神经损伤和免疫失调有关。这些改变可能与 CP/CPPS 患者的慢性疼痛、排尿症状、生育能力下降和抑郁有关。这项研究为了解 CP/CPPS 的病理机制提供了一个局部-全球视角,并提供了潜在的诊断和治疗目标。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Chronic prostatitis/chronic pelvic pain syndrome induces metabolomic changes in expressed prostatic secretions and plasma.

Abstract: Chronic prostatitis/chronic pelvic pain syndrome (CP/CPPS) is a complex disease that is often accompanied by mental health disorders. However, the potential mechanisms underlying the heterogeneous clinical presentation of CP/CPPS remain uncertain. This study analyzed widely targeted metabolomic data of expressed prostatic secretions (EPS) and plasma to reveal the underlying pathological mechanisms of CP/CPPS. A total of 24 CP/CPPS patients from The Second Nanning People's Hospital (Nanning, China), and 35 asymptomatic control individuals from First Affiliated Hospital of Guangxi Medical University (Nanning, China) were enrolled. The indicators related to CP/CPPS and psychiatric symptoms were recorded. Differential analysis, coexpression network analysis, and correlation analysis were performed to identify metabolites that were specifically altered in patients and associated with various phenotypes of CP/CPPS. The crucial links between EPS and plasma were further investigated. The metabolomic data of EPS from CP/CPPS patients were significantly different from those from control individuals. Pathway analysis revealed dysregulation of amino acid metabolism, lipid metabolism, and the citrate cycle in EPS. The tryptophan metabolic pathway was found to be the most significantly altered pathway associated with distinct CP/CPPS phenotypes. Moreover, the dysregulation of tryptophan and tyrosine metabolism and elevation of oxidative stress-related metabolites in plasma were found to effectively elucidate the development of depression in CP/CPPS. Overall, metabolomic alterations in the EPS and plasma of patients were primarily associated with oxidative damage, energy metabolism abnormalities, neurological impairment, and immune dysregulation. These alterations may be associated with chronic pain, voiding symptoms, reduced fertility, and depression in CP/CPPS. This study provides a local-global perspective for understanding the pathological mechanisms of CP/CPPS and offers potential diagnostic and therapeutic targets.

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