前列腺炎的鉴别、药理学考虑和治疗

Daryl S. Schiller PharmD , Ashish Parikh MD
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Treatment responses to α-blockers appear to be greater with longer durations of therapy in α-blocker–naïve patients (National Institutes of Health-Chronic Prostatitis Symptom Index [NIH-CPSI] score reduction of at least 3.6 points after 6 weeks of tamsulosin therapy [<em>P =</em> 0.04] and up to 14.3 and 9.9 point NIH-CPSI score reductions with 14 weeks of terazosin and 24 weeks of alfuzosin therapy, respectively [<em>P =</em> 0.01 for both]). Combination therapy with an α-blocker, an anti-inflammatory, and a muscle relaxant does not appear to offer significant advantages over monotherapy (12.7 vs 12.4 point reduction in NIH-CPSI scores) and a stepwise approach to therapy involving antibiotics followed by bioflavonoids and then α-blockers appears to effectively reduce symptoms for up to 1 year in patients with chronic prostatitis (mean NIH-CPSI point reduction of 9.5 points compared with baseline, <em>P</em> &lt; 0.0001). 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引用次数: 15

摘要

背景:前列腺炎是由前列腺炎症或肿胀引起的一系列体征和症状。前列腺炎有许多不同的原因,包括感染;有时没有发现炎症的明确病因。有效的治疗往往取决于病因的确定,但微生物并不总是可检测的,特别是在慢性前列腺炎的情况下。目的综述前列腺炎的鉴别和治疗方法,包括药物和非药物干预。方法通过检索MEDLINE(1966 - 2010年6月)、International Pharmaceutical Abstracts(1970 - 2010年6月)和EMBASE(1947 - 2010年6月)对相关信息进行检索。检查前列腺癌、良性前列腺肥大或前列腺相关手术(即活组织检查)的随机对照试验被排除在外。结果1999年建立了前列腺炎工作分类系统,但对不同治疗方案进行区分的随机对照试验较少。细菌性前列腺炎可急性或慢性,但总是需要一定程度的抗菌治疗。氟喹诺酮类药物的药理特点使其成为大多数患者的首选药物。由于前列腺组织和血清之间的pH值差异,这些抗生素可能会被困在慢性炎症的前列腺中。许多氟喹诺酮类药物的渗透比(前列腺水平:血清水平)高达4:1。一项针对诊断为慢性细菌性前列腺炎而接受左氧氟沙星500 mg/d治疗的欧洲男性(N = 117)的研究显示,在治疗后5-12天、1个月、3个月和6个月,临床成功率分别为92% (95% CI 84.8%-96.5%)、77.4% (95% CI 68.2-84.9%)、66.0% (95% CI 56.2%-75.0%)和61.9% (95% CI 51.9%-71.2%)。此外,在慢性前列腺炎患者中进行了大量随机、安慰剂对照试验,研究了α-受体阻滞剂、类固醇抑制剂、抗炎剂和生物类黄酮。在α-blocker-naïve患者中,α-阻滞剂的治疗效果似乎随着治疗时间的延长而增加(美国国立卫生研究院慢性前列腺炎症状指数[NIH-CPSI]评分在坦舒罗新治疗6周后降低至少3.6分[P = 0.04],而在特拉唑嗪治疗14周和阿夫唑嗪治疗24周时,NIH-CPSI评分分别降低14.3和9.9分[P = 0.01])。α-受体阻滞剂、抗炎剂和肌肉松弛剂联合治疗似乎没有比单药治疗提供显著优势(NIH-CPSI评分降低12.7分vs 12.4分),而采用循序渐进的治疗方法,包括抗生素、生物类黄酮和α-受体阻滞剂,似乎可以有效减轻慢性前列腺炎患者长达1年的症状(与基线相比,NIH-CPSI平均降低9.5分,P <0.0001)。有多种治疗方案不成功的患者可以通过电磁或电针疗法直接刺激骨盆肌肉。结论前列腺炎可能与其他疾病相似,但正确的分类、了解其药理特征和治疗药物的期望有助于确定有效的治疗策略。氟喹诺酮类药物是治疗细菌性前列腺炎的首选药物,并已证明在某些尚未确定有机体的慢性前列腺炎病例中有效。然而,使用具有抗炎或抗肾上腺素能特性的药物可能需要与抗菌剂联合使用或在尝试抗菌剂后使用。
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Identification, Pharmacologic Considerations, and Management of Prostatitis

Background

Prostatitis is a collection of signs and symptoms that occur as a result of inflammation or swelling of the prostate gland. There are many different causes for prostatitis, including infection; occasionally no clear etiology for the inflammation is found. Effective treatment often depends on identification of the cause, but a microbiologic organism is not always detectable, especially in cases of chronic prostatitis.

Objective

The aim of this article was to review identification and treatment options for prostatitis, including pharmacologic and nonpharmacologic interventions.

Methods

Relevant information was identified through a search of MEDLINE (1966–June 2010), International Pharmaceutical Abstracts (1970–June 2010), and EMBASE (1947–June 2010). Randomized, controlled trials that examined prostate cancer, benign prostatic hypertrophy, or procedures related to the prostate (ie, biopsies) were excluded.

Results

A working classification system for prostatitis was developed in 1999, but there are few randomized controlled trials that distinguish between the various treatment options. Bacterial prostatitis can be acute or chronic but always requires some degree of antimicrobial therapy. Pharmacologic features of fluoroquinolones make them the preferred agents for most patients. These antibiotics can become trapped in a chronically inflamed prostate due to pH differences between prostatic tissue and serum. Many fluoroquinolones have penetration ratios (prostate level:serum level) of up to 4:1. A study in European men (N = 117) who received levofloxacin 500 mg/d with a diagnosis of chronic bacterial prostatitis demonstrated clinical success rates of 92% (95% CI 84.8%–96.5%), 77.4% (95% CI, 68.2–84.9%), 66.0% (95% CI, 56.2%–75.0%), and 61.9% (95% CI, 51.9%–71.2%) at 5–12 days, 1 month, 3 months, and 6 months after treatment. Additionally, there have been numerous randomized, placebo-controlled trials in patients with chronic prostatitis that have studied α-blockers, steroid inhibitors, anti-inflammatory agents, and bioflavonoids. Treatment responses to α-blockers appear to be greater with longer durations of therapy in α-blocker–naïve patients (National Institutes of Health-Chronic Prostatitis Symptom Index [NIH-CPSI] score reduction of at least 3.6 points after 6 weeks of tamsulosin therapy [P = 0.04] and up to 14.3 and 9.9 point NIH-CPSI score reductions with 14 weeks of terazosin and 24 weeks of alfuzosin therapy, respectively [P = 0.01 for both]). Combination therapy with an α-blocker, an anti-inflammatory, and a muscle relaxant does not appear to offer significant advantages over monotherapy (12.7 vs 12.4 point reduction in NIH-CPSI scores) and a stepwise approach to therapy involving antibiotics followed by bioflavonoids and then α-blockers appears to effectively reduce symptoms for up to 1 year in patients with chronic prostatitis (mean NIH-CPSI point reduction of 9.5 points compared with baseline, P < 0.0001). Patients who have had multiple unsuccessful treatment regimens may benefit from direct stimulation of the pelvic muscles through electromagnetic or electroacupuncture therapy.

Conclusions

Prostatitis can resemble various other medical conditions but proper classification and an understanding of the pharmacologic features and expectations of the medications used to treat it can help identify effective treatment strategies. Fluoroquinolones are the preferred agents for treating bacterial causes of prostatitis and have demonstrated efficacy in some cases of chronic prostatitis when an organism has not been identified. However, the use of agents with anti-inflammatory or antiadrenergic properties may be necessary in combination with or after trying antimicrobial agents.

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来源期刊
American Journal Geriatric Pharmacotherapy
American Journal Geriatric Pharmacotherapy GERIATRICS & GERONTOLOGY-PHARMACOLOGY & PHARMACY
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