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使用磷酸二酯酶 5 抑制剂与眼部不良事件无关。

Use of phosphodiesterase 5 inhibitors is not associated with ocular adverse events.

机构信息

Division of Experimental Oncology/Unit of Urology, URI, IRCCS Ospedale San Raffaele, Milan 20132, Italy.

University Vita-Salute San Raffaele, Milan 20132, Italy.

出版信息

J Sex Med. 2023 Nov 30;20(12):1399-1406. doi: 10.1093/jsxmed/qdad137.

Abstract

BACKGROUND

Phosphodiesterase 5 inhibitor (PDE5i) use has been linked to a number of ocular side effects, such as serous retinal detachment (SRD), retinal vascular occlusion (RVO), and ischemic optic neuropathy (ION).

AIM

We investigated the risk for SRD, RVO, and ION in patients using PDE5is.

METHODS

We utilized the IBM MarketScan (2007-2021) Commercial and Medicare Supplemental Databases (version 2.0) for this analysis. To estimate overall events risk, Cox proportional hazard models were applied to calculate the hazard ratios (HRs) for erectile dysfunction (ED) diagnosis and the different treatments, adjusting for region, median age, obesity, diabetes mellitus, hyperlipidemia, smoking, hypertension, coronary artery disease, and sleep apnea. Additionally, the same analyses were performed to calculate the HRs for benign prostatic hyperplasia (BPH) diagnosis and the different treatments.

OUTCOMES

HRs for SRD, RVO, and ION.

RESULTS

In total, 1 938 262 men with an ED diagnosis were observed during the study period. Among them, 615 838 (31.8%) were treated with PDE5is. In total, 2 175 439 men with a BPH diagnosis were observed during the study period. Among them, 175 725 (8.1%) were treated with PDE5is. On adjusted Cox regression analysis, PDE5i use was not associated with SRD, RVO, ION, and any ocular event when compared with ED diagnosis and other ED treatments. Importantly, as the intensity of ED treatment increased, so did the risk of ocular events. In addition, PDE5i use was not associated with SRD and ION when compared with BPH diagnosis and other BPH treatments. In contrast, in patients with BPH, PDE5i use was associated with RVO (HR, 1.14; 95% CI, 1.06-1.23). Importantly, patients with BPH receiving other medical treatment (ie, 5a reductase/alpha blocker; HR, 1.11; 95% CI, 1.06-1.16) or surgical treatment (HR, 1.10; 95% CI, 1.02-1.19) had a higher risk of RVO.

CLINICAL IMPLICATIONS

We did not observe any consistent association between PDE5i use and any ocular adverse events (SRD, RVO, and ION).

STRENGTHS AND LIMITATIONS

Because we did not have access to the patients' medical records, we recorded outcome definitions using ICD-9 and ICD-10 coding.

CONCLUSIONS

Patients using PDE5is for ED or BPH indications did not have an increased risk of ocular events, even when compared with other treatments for ED or BPH.

摘要

背景

磷酸二酯酶 5 抑制剂(PDE5i)的使用与许多眼部副作用有关,例如浆液性视网膜脱离(SRD)、视网膜血管闭塞(RVO)和缺血性视神经病变(ION)。

目的

我们研究了使用 PDE5i 的患者发生 SRD、RVO 和 ION 的风险。

方法

我们利用 IBM MarketScan(2007-2021)商业和医疗保险补充数据库(版本 2.0)进行了这项分析。为了估计总体事件风险,我们应用 Cox 比例风险模型来计算勃起功能障碍(ED)诊断和不同治疗的风险比(HRs),并调整了区域、中位年龄、肥胖、糖尿病、高脂血症、吸烟、高血压、冠心病和睡眠呼吸暂停。此外,还进行了相同的分析,以计算良性前列腺增生(BPH)诊断和不同治疗的 HRs。

结果

共观察到 1938262 名患有 ED 诊断的男性在研究期间发生了 SRD、RVO 和 ION。其中,615838 名(31.8%)接受了 PDE5i 治疗。共观察到 2175439 名患有 BPH 诊断的男性在研究期间发生了 SRD、RVO 和 ION。其中,175725 名(8.1%)接受了 PDE5i 治疗。经调整后的 Cox 回归分析显示,与 ED 诊断和其他 ED 治疗相比,PDE5i 治疗与 SRD、RVO、ION 和任何眼部事件无关。重要的是,随着 ED 治疗强度的增加,眼部事件的风险也随之增加。此外,与 BPH 诊断和其他 BPH 治疗相比,PDE5i 治疗与 SRD 和 ION 无关。相比之下,在患有 BPH 的患者中,PDE5i 治疗与 RVO 相关(HR,1.14;95%CI,1.06-1.23)。重要的是,接受其他药物治疗(即 5a 还原酶/α 阻滞剂;HR,1.11;95%CI,1.06-1.16)或手术治疗(HR,1.10;95%CI,1.02-1.19)的 BPH 患者发生 RVO 的风险更高。

临床意义

我们没有观察到 PDE5i 使用与任何眼部不良事件(SRD、RVO 和 ION)之间存在一致的关联。

优势和局限性

由于我们无法获取患者的病历,因此我们使用 ICD-9 和 ICD-10 编码记录了结局定义。

结论

对于 ED 或 BPH 指征的患者,即使与 ED 或 BPH 的其他治疗相比,使用 PDE5i 也不会增加眼部事件的风险。

相似文献

本文引用的文献

1
In Defense of Phosphodiesterase 5 Inhibitors.为磷酸二酯酶5抑制剂辩护。
JAMA Ophthalmol. 2022 Sep 1;140(9):908. doi: 10.1001/jamaophthalmol.2022.2612.
4
Marked Increase in Sales of Erectile Dysfunction Medication During COVID-19.新冠疫情期间勃起功能障碍药物销量显著增长。
J Gen Intern Med. 2021 Sep;36(9):2912-2914. doi: 10.1007/s11606-021-06968-2. Epub 2021 Jun 25.
8
Erectile dysfunction.勃起功能障碍。
Nat Rev Dis Primers. 2016 Feb 4;2:16003. doi: 10.1038/nrdp.2016.3.

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