Azab Mohammad, Benchaboune Mustapha, Blinder Kevin J, Bressler Neil M, Bressler Susan B, Gragoudas Evangelos S, Fish Gary Edd, Hao Yong, Haynes Laurie, Lim Jennifer I, Menchini Ugo, Miller Joan W, Mones Jordi, Potter Michael J, Reaves Al, Rosenfeld Philip J, Strong Andrew, Su Xiang Yao, Slakter Jason S, Schmidt-Erfurth Ursula, Sorenson John A
Retina. 2004 Feb;24(1):1-12. doi: 10.1097/00006982-200402000-00001.
We sought to evaluate the detailed safety profile of photodynamic therapy with verteporfin in patients with subfoveal choroidal neovascularization (CNV) caused by age-related macular degeneration (ARMD) from the combined analysis of three multicenter, double-masked, placebo-controlled, randomized 24-month clinical trials of similar design (TAP Investigation Studies A and B and the VIP ARMD Trial), and to clarify the adverse reaction information in the current verteporfin product prescription information approved in the United States.
Nine hundred forty-eight patients were randomly assigned to verteporfin or placebo. Treatment was administered as described in previous reports. All general entry criteria were similar, so systemic safety results were combined for this analysis. Entry criteria for CNV lesion composition and visual acuity in the two TAP Investigation trials was different from those used in the VIP ARMD trial, so ocular safety results for the treated eye were not combined.
The percentage of patients who experienced at least one ocular or nonocular adverse event, regardless of relationship to therapy, was similar between the verteporfin and placebo groups (92.3 and 89.1%, respectively, P = 0.114). The overall incidence of study eye adverse events was not significantly different between verteporfin and placebo. The only clinically relevant ocular adverse events reported with higher incidence after verteporfin compared with placebo were visual disturbances (22.1 versus 15.5% in TAP [P = 0.054] and 41.7 and 22.8% in VIP [P < 0.001]). Acute severe visual acuity decrease (defined as a visual acuity letter score decrease of at least 20, equivalent to at least four-line decrease, within 7 days of therapy) occurred in 3 patients treated with verteporfin in the TAP Investigation (0.7%) and 11 in the VIP ARMD trial (4.9%). Systemic adverse events with increased incidence after verteporfin compared with placebo, most of which were transient and mild or moderate, were injection site reactions (13.1 versus 5.6%; P < 0.001), photosensitivity reactions (2.4 versus 0.3%; P = 0.016), and infusion-related back pain (2.4 versus 0%; P = 0.004). No clinically relevant difference was observed between the verteporfin and placebo groups in any other adverse event.
In 948 ARMD patients, verteporfin therapy had an overall safety profile similar to that for placebo, with a few exceptions. Visual disturbances, including acute severe visual acuity decrease, did not affect the net vision outcome benefits associated with treatment that has been reported previously. This detailed safety profile of verteporfin therapy clarifies the adverse reaction information in the current verteporfin product prescription information.
我们试图通过对三项设计相似的多中心、双盲、安慰剂对照、随机化24个月临床试验(TAP研究A和B以及VIP年龄相关性黄斑变性试验)的联合分析,评估维替泊芬光动力疗法治疗年龄相关性黄斑变性(ARMD)所致中心凹下脉络膜新生血管(CNV)患者的详细安全性概况,并阐明美国目前批准的维替泊芬产品处方信息中的不良反应信息。
948例患者被随机分配至维替泊芬组或安慰剂组。治疗按既往报道所述进行。所有一般入选标准相似,因此将全身安全性结果合并进行该分析。TAP研究两项试验中CNV病变组成和视力的入选标准与VIP年龄相关性黄斑变性试验所用标准不同,因此未合并治疗眼的眼部安全性结果。
无论与治疗有无关联,维替泊芬组和安慰剂组中至少发生1次眼部或非眼部不良事件的患者百分比相似(分别为92.3%和89.1%,P = 0.114)。维替泊芬组和安慰剂组研究眼不良事件的总体发生率无显著差异。与安慰剂相比,维替泊芬治疗后报告发生率较高的唯一具有临床相关性的眼部不良事件是视觉障碍(TAP研究中分别为22.1%和15.5%[P = 0.054],VIP试验中为41.7%和22.8%[P < 0.001])。TAP研究中有3例接受维替泊芬治疗的患者(0.7%)以及VIP年龄相关性黄斑变性试验中有11例患者(4.9%)发生急性严重视力下降(定义为治疗7天内视力字母评分至少下降20,相当于至少下降4行)。与安慰剂相比,维替泊芬治疗后发生率增加的全身不良事件,其中大多数为短暂性且轻度或中度,包括注射部位反应(13.1%对5.6%;P < 0.001)、光敏反应(2.4%对0.3%;P = 0.016)以及输液相关背痛(2.4%对0%;P = 0.004)。在任何其他不良事件方面,维替泊芬组和安慰剂组之间未观察到具有临床相关性的差异。
在948例ARMD患者中,维替泊芬治疗的总体安全性概况与安慰剂相似,有少数例外情况。视觉障碍,包括急性严重视力下降,并未影响先前报道的与治疗相关的净视力获益。维替泊芬治疗的这一详细安全性概况阐明了当前维替泊芬产品处方信息中的不良反应信息。
