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前列腺炎的多学科治疗方法。

Multidisciplinary approach to prostatitis.

作者信息

Magri Vittorio, Boltri Matteo, Cai Tommaso, Colombo Roberto, Cuzzocrea Salvatore, De Visschere Pieter, Giuberti Rosanna, Granatieri Clara Maria, Latino Maria Agnese, Larganà Gaetano, Leli Christian, Maierna Giorgio, Marchese Valentina, Massa Elisabetta, Matteelli Alberto, Montanari Emanuele, Morgia Giuseppe, Naber Kurt G, Papadouli Vaia, Perletti Gianpaolo, Rekleiti Nektaria, Russo Giorgio I, Sensini Alessandra, Stamatiou Konstantinos, Trinchieri Alberto, Wagenlehner Florian M E

机构信息

ASST Nord Milano.

出版信息

Arch Ital Urol Androl. 2019 Jan 18;90(4):227-248. doi: 10.4081/aiua.2018.4.227.

DOI:10.4081/aiua.2018.4.227
PMID:30655633
Abstract

The modern clinical research on prostatitis started with the work of Stamey and coworkers who developed the basic principles we are still using. They established the segmented culture technique for localizing the infections in the males to the urethra, the bladder, or the prostate and to differentiate the main categories of prostatitis. Such categories with slight modifications are still used according to the NIH classification: acute bacterial prostatitis, chronic bacterial prostatitis, Chronic Pelvic Pain Syndrome (CPPS) and asymptomatic prostatitis. Prostatic inflammation is considered an important factor in influencing both prostatic growth and progression of symptoms of benign prostatic hyperplasia and prostatitis. Chronic inflammation/neuroinflammation is a result of a deregulated acute phase response of the innate immune system affecting surrounding neural tissue at molecular, structural and functional levels. Clinical observations suggest that chronic inflammation correlates with chronic prostatitis/chronic pelvic pain syndrome (CP/CPPS) and benign prostatic hyperplasia (BPH) and an history of clinical chronic prostatitis significantly increases the odds for prostate cancer. The NIHNIDDK classification based on the use of the microbiological 4- glasses localization test or simplified 2-glasses test, is currently accepted worldwide. The UPOINT system identifies groups of clinicians with homogeneous clinical presentation and is used to recognize phenotypes to be submitted to specific treatments. The UPOINTS algorithm implemented the original UPOINT adding to the urinary domains (U), psycho-social (P), organspecific (O), infection (I), neurological (N), muscle tension and tenderness (T) a further domain related to sexuality (S). In fact sexual dysfunction (erectile, ejaculatory, libido loss) has been described in 46-92% of cases with a high impact on the quality of life of patients with CP/CPPS. Prostatic ultrasound represents the most popular imaging test in the work-up of either acute and chronic prostatitis although no specific hypo-hyperechoic pattern has been clearly associated with chronic bacterial prostatitis and CPPS. Use of a digital-processing software to calculate the extension of prostatic calcification area at ultrasound demonstrated a higher percentage of prostatic calcification in patients with chronic bacterial prostatitis. Multiparametric Magnetic Resonance Imaging (mpMRI) is the current state-of-the art imaging modality in the assessment of patients with prostate cancer although a variety of benign conditions, including inflammation, may mimic prostate cancer and act as confounding factors in the discrimination between neoplastic and non-neoplastic lesions. Bacteria can infect prostate gland by: ascending the urethra, reflux of urine into the prostatic ducts, direct inoculation of bacteria through inserted biopsy needles or hematogenous seeding. Enterobacteriaceae are the predominant pathogens in acute and chronic bacterial prostatitis, but an increasing role of Enterococci has been reported. Many strains of these uropathogens exhibit the ability to form biofilm and multidrug- resistance. Sexually Transmitted Infections (STI) agents, in particular Chlamydia trachomatis and Mycoplasma genitalium, have been also considered as causative pathogens of chronic bacterial prostatitis. On the contrary the effective role in genital diseases of other "genital mycoplasmas" is still a much debated issue. Sexually Transmitted Infections agents should be investigated by molecular methods in both patient and sexual partner. "Next generation" investigations, such as cytokine analysis, cytological typing of immune cells could help stratifying the immune response. Epigenetic dysregulation of inflammatory factors should be investigated according to systemic and compartment-specific signals. The search for biomarkers should also include evaluation of hormonal pathways, as measurement of estrogen levels in semen. Antimicrobials are the first line agents for the treatment of bacterial prostatitis. The success of antimicrobial treatment depends on the antibacterial activity and the pharmacokinetic characteristics of the drug which must reach high concentrations in prostate secretion and prostate tissue. Acute bacterial prostatitis can be a serious infection with a potential risk for urosepsis For iInitial treatment of severely ill patients, intravenous administration of high doses of bactericidal antimicrobials, such as broad-spectrum penicillins, third-generation cephalosporins or fluoroquinolones, is recommended in combination with an aminoglycoside. Use of piperacillin-tazobactam and meropenem is justified in presence of multiresistant gramnegative pathogens. The antibiotic treatment of chronic prostatitis is currently based on the use of fluoroquinolones that, given for 2 to 4 weeks, cured about 70% of men with chronic bacterial prostatitis. For the treatment of Chlamydial prostatitis macrolides were shown to be more effective than fluoroquinolones, whereas no differences were observed in microbiological and clinical efficacy between macrolides and tetracyclines for the treatment of infections caused by intracellular pathogens. Aminoglycosides and fosfomycin could be considered as a therapeutic alternative for the treatment of quinolone resistant prostatitis. Use of alpha-blockers in CP/CPPS patients with urinary symptoms and analgesics +/- non steroidal anti-inflammatory drugs (NSAID), in presence of pain demonstrated a reduction of symptoms reduction and an improvement of quality of life, although long term use of NSAID is limited by side effect profile. However, the multimodal therapeutic regimen by contemporary use of alphablockers, antibiotics and anti-inflammatory showed a better control of prostatitis symptoms than single drug treatment. Novel therapeutic substances for the treatment of pain, such as the cannabinoid anandamide would be highly interesting to test. An alternative for the treatment of chronic prostatitis/chronic pelvic pain syndrome is phytotherapy, as primary therapy or in association with other drugs. Quercetin, pollen extract, extract of Serenoa repens and other mixtures of herbal extracts showed a positive effect on symptoms and quality of life without side effects. The association of CP/CPPS with alterations of intestinal function has been described. Diet has its effects on inflammation by regulation of the composition of intestinal flora and direct action on the intestinal cells (sterile inflammation). Intestinal bacteria (microbiota) interacts with food influencing the metabolic, immune and inflammatory response of the organism. The intestinal microbiota has protective function against pathogenic bacteria, metabolic function by synthesis of vitamins, decomposition of bile acids and production of trophic factors (butyrate), and modulation of the intestinal immune system. The alteration of the microbiota is called "dysbiosis" causing invasive intestinal diseases pathologies (leaky gut syndrome and food intolerances, irritable bowel syndrome or chronic inflammatory bowel diseases) and correlating with numerous systemic diseases including acute and chronic prostatitis. Administration of live probiotics bacteria can be used to regulate the balance if intestinal flora. Sessions of hydrocolontherapy can represent an integration to this therapeutic approach. Finally, microbiological examination of sexual partners can offer supplementary information for treatment.

摘要

现代前列腺炎临床研究始于斯塔米及其同事的工作,他们确立了我们仍在使用的基本原则。他们开发了分段培养技术,用于将男性感染定位到尿道、膀胱或前列腺,并区分前列腺炎的主要类别。根据美国国立卫生研究院(NIH)的分类,这些类别虽有细微修改但仍在使用:急性细菌性前列腺炎、慢性细菌性前列腺炎、慢性盆腔疼痛综合征(CPPS)和无症状性前列腺炎。前列腺炎症被认为是影响前列腺生长以及良性前列腺增生和前列腺炎症状进展的重要因素。慢性炎症/神经炎症是先天免疫系统急性期反应失调的结果,在分子、结构和功能水平上影响周围神经组织。临床观察表明,慢性炎症与慢性前列腺炎/慢性盆腔疼痛综合征(CP/CPPS)和良性前列腺增生(BPH)相关,临床慢性前列腺炎病史会显著增加患前列腺癌的几率。基于微生物学4杯定位试验或简化2杯试验的NIHNIDDK分类目前在全球被广泛接受。UPOINT系统可识别临床表现相似的临床医生群体,并用于识别适合特定治疗的表型。UPOINTS算法在原始UPOINT基础上增加了一个与性功能(S)相关的领域,即除了泌尿领域(U)、心理社会领域(P)、器官特异性领域(O)、感染领域(I)、神经领域(N)、肌肉紧张和压痛领域(T)之外。事实上,46 - 92%的CP/CPPS患者存在性功能障碍(勃起、射精、性欲丧失),这对患者的生活质量有很大影响。前列腺超声是急性和慢性前列腺炎检查中最常用的影像学检查,尽管没有特定的低回声/高回声模式与慢性细菌性前列腺炎和CPPS明确相关。使用数字处理软件计算超声下前列腺钙化面积的范围,结果显示慢性细菌性前列腺炎患者的前列腺钙化百分比更高。多参数磁共振成像(mpMRI)是目前评估前列腺癌患者的先进影像学检查方法,尽管包括炎症在内的多种良性疾病可能会模拟前列腺癌,并在区分肿瘤性和非肿瘤性病变时成为混淆因素。细菌可通过以下途径感染前列腺:沿尿道上行、尿液反流至前列腺导管、通过插入的活检针直接接种细菌或血行播散。肠杆菌科是急性和慢性细菌性前列腺炎的主要病原体,但据报道肠球菌的作用日益增加。这些尿路病原体的许多菌株具有形成生物膜和多重耐药的能力。性传播感染(STI)病原体,特别是沙眼衣原体和解脲脲原体,也被认为是慢性细菌性前列腺炎的致病病原体。相反,其他“生殖支原体”在生殖系统疾病中的实际作用仍是一个备受争议的问题。应通过分子方法对患者及其性伴侣进行性传播感染病原体的检测。“下一代”研究,如细胞因子分析、免疫细胞的细胞学分型,有助于对免疫反应进行分层。应根据全身和局部特异性信号研究炎症因子的表观遗传失调。寻找生物标志物还应包括评估激素途径,如测量精液中的雌激素水平。抗菌药物是治疗细菌性前列腺炎的一线药物。抗菌治疗的成功取决于药物的抗菌活性和药代动力学特性,药物必须在前列腺分泌物和前列腺组织中达到高浓度。急性细菌性前列腺炎可能是一种严重感染,有发生尿脓毒症的潜在风险。对于重症患者的初始治疗,建议静脉注射高剂量的杀菌抗菌药物,如广谱青霉素、第三代头孢菌素或氟喹诺酮类药物,并联合使用氨基糖苷类药物。在存在多重耐药革兰阴性病原体的情况下,使用哌拉西林 - 他唑巴坦和美罗培南是合理的。慢性前列腺炎的抗生素治疗目前基于使用氟喹诺酮类药物,连续使用2至4周,可治愈约70%的慢性细菌性前列腺炎男性患者。对于衣原体性前列腺炎,大环内酯类药物比氟喹诺酮类药物更有效,而对于细胞内病原体引起的感染,大环内酯类药物和四环素类药物在微生物学和临床疗效上没有差异。氨基糖苷类药物和磷霉素可被视为治疗喹诺酮耐药性前列腺炎的替代治疗药物。对于有排尿症状的CP/CPPS患者使用α受体阻滞剂,以及在有疼痛时使用镇痛药和/或非甾体抗炎药(NSAID),可减轻症状并改善生活质量,尽管长期使用NSAID会受到副作用的限制。然而,同时使用α受体阻滞剂、抗生素和抗炎药的多模式治疗方案比单一药物治疗能更好地控制前列腺炎症状。新型治疗疼痛的物质,如大麻素类的花生四烯乙醇胺,将是非常值得测试的。治疗慢性前列腺炎/慢性盆腔疼痛综合征的另一种方法是植物疗法,可作为主要治疗方法或与其他药物联合使用。槲皮素、花粉提取物、锯叶棕提取物和其他草药提取物混合物对症状和生活质量有积极影响且无副作用。已有研究描述了CP/CPPS与肠道功能改变之间的关联。饮食通过调节肠道菌群组成和对肠道细胞的直接作用(无菌性炎症)对炎症产生影响。肠道细菌(微生物群)与食物相互作用,影响机体的代谢、免疫和炎症反应。肠道微生物群具有抵御病原菌的保护功能、通过合成维生素、分解胆汁酸和产生营养因子(丁酸盐)的代谢功能以及调节肠道免疫系统的功能。微生物群的改变被称为“生态失调”,可导致侵袭性肠道疾病(肠漏综合征和食物不耐受、肠易激综合征或慢性炎症性肠病),并与包括急性和慢性前列腺炎在内的多种全身性疾病相关。服用活的益生菌可用于调节肠道菌群平衡。结肠水疗可作为这种治疗方法的补充。最后,对性伴侣进行微生物学检查可为治疗提供补充信息。

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