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Prevention of Recurrent Ischemic Priapism with Ketoconazole: Evolution of a Treatment Protocol and Patient Outcomes

机译:酮康唑预防复发性缺血性普利普斯病:治疗方案和患者结果的演变

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Introduction: The management of recurrent ischemic priapism (RIP) is not clearly defined. Ketoconazole (KTZ) is used to treat RIP and produces a temporary hypogonadal state to suppress sleep-related erections (SREs), which often evolve into episodes of ischemic priapism in this population. Aim: We review our experience to prevent RIP using KTZ and present our outcomes using a decreased dose regimen. Methods: A retrospective chart review and phone survey of 17 patients with RIP was performed. KTZ inhibits adrenal and gonadal testosterone production with a half-life of 8 hours. By suppressing testosterone levels, SREs are interrupted. We compared our previous protocol of three times daily (TID) KTZ dosing with prednisone for 6 months with our current regimen of initiating KTZ 200mg TID with prednisone 5mg daily for 2 weeks and then tapering to KTZ 200mg nightly for 6 months. Main Outcome Measures: The primary outcome was the prevention of RIP using KTZ. Secondary outcomes included side effects secondary to KTZ use and patient satisfaction. Results: All men experienced daily or almost daily episodes of prolonged, painful erections prior to starting KTZ. The mean number of emergency room (ER) visits per patient prior to starting KTZ was 6.5. No patient required an ER visit for RIP while on KTZ. Sixteen of 17 patients (94%) had complete resolution of priapism while on KTZ with effects noted immediately after starting therapy and no reported sexual side effects attributed to KTZ. One man stopped therapy after 4 days because of nausea/vomiting. Fourteen of 16 men eventually discontinued KTZ after a median duration of 7 months. Twenty-nine percent reported no recurrent priapic episodes after discontinuing. A total of 78.6% had partial or complete resolution of symptoms persisting after KTZ was discontinued with a mean post-treatment follow-up of 36.7 months. Conclusion: No reliable effective preventative therapy has been identified for RIP. In our relatively sizable single-center experience, KTZ appears to be a reasonably effective, safe, and inexpensive treatment to prevent RIP while preserving sexual function. We now recommend our tapered dose regimen listed above. After 6 months, we recommend stopping the medication as we have found a majority of patients will not need to resume nightly KTZ.
机译:简介:复发性缺血性癫痫(RIP)的治疗方法尚不明确。酮康唑(KTZ)用于治疗RIP并产生暂时性性腺功能减退状态,以抑制睡眠相关的勃起(SRE),而勃起通常在该人群中发展为缺血性阴茎异常发作。目的:我们回顾我们使用KTZ预防RIP的经验,并使用减少剂量的治疗方案来介绍我们的结果。方法:对17例RIP患者进行回顾性图表回顾和电话调查。 KTZ抑制肾上腺和性腺睾丸激素的产生,半衰期为8小时。通过抑制睾丸激素水平,SRE被中断。我们比较了之前使用泼尼松每日3次(TID)KTZ给药6个月的方案,以及我们目前使用每天泼尼松5mg每日200mg TID进行2周,然后每晚逐渐减少200mg KTZ的方案。主要结果指标:主要结果是使用KTZ预防RIP。次要结果包括使用KTZ和患者满意度带来的副作用。结果:所有男性在开始KTZ之前每天或几乎每天经历长时间的痛苦勃起。开始KTZ之前,每位患者的急诊室平均回访次数为6.5。在KTZ上,没有患者需要对RIP进行急诊就诊。 17例患者中有16例(94%)在接受KTZ治疗时已完全消退,并在开始治疗后即刻注意到疗效,但未报告归因于KTZ的性副作用。一名男子在4天后因恶心/呕吐而停止治疗。在中位时间7个月后,十六名男子中有十四名最终终止了KTZ的治疗。有29%的人在停药后没有复发的发作性发作。停用KTZ后,共有78.6%的患者症状部分或完全缓解,而平均治疗后随访时间为36.7个月。结论:尚未确定可靠的有效的RIP预防疗法。根据我们相对丰富的单中心治疗经验,KTZ似乎是一种合理有效,安全且廉价的治疗方法,可在保持性功能的同时预防RIP。现在,我们建议上面列出的逐渐剂量方案。 6个月后,我们建议停止用药,因为我们发现大多数患者不需要每晚恢复KTZ。

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