GS-101反义寡核苷酸滴眼液可抑制角膜新生血管形成:一项随机II期试验的中期结果
GS-101 antisense oligonucleotide eye drops inhibit corneal neovascularization: interim results of a randomized phase II trial.
作者信息
Cursiefen Claus, Bock Felix, Horn Folkert K, Kruse Friedrich E, Seitz Berthold, Borderie Vincent, Früh Beatrice, Thiel Michael A, Wilhelm Frank, Geudelin Bernard, Descohand Isabelle, Steuhl Klaus-Peter, Hahn Angela, Meller Daniel
机构信息
Department of Ophthalmology, University of Erlangen-Nürnberg, Schwabachanlage 6, Erlangen, Germany.
出版信息
Ophthalmology. 2009 Sep;116(9):1630-7. doi: 10.1016/j.ophtha.2009.04.016. Epub 2009 Jul 29.
PURPOSE
Pathologic corneal neovascularization not only reduces corneal transparency and visual acuity, but also is one of the most significant preoperative and postoperative risk factors for graft rejection after corneal transplantation. The aim of this study was to test tolerability and efficacy of gene signal (GS)-101 eye drops, an antisense oligonucleotide against insulin receptor substrate-1, versus placebo on inhibition of progressive corneal neovascularization.
DESIGN
Randomized, double-blind, multicenter, phase II clinical study.
PARTICIPANTS AND CONTROLS
Interim analysis on 40 patients with progressive corneal neovascularization resulting from various underlying diseases being nonresponsive to conventional therapy.
INTERVENTIONS
Four groups of 10 patients were treated for 3 months in this dose-finding study comparing 3 doses of GS-101 (eye drops twice daily; 43, 86, and 172 microg/day total) with placebo (10 patients per group).
MAIN OUTCOME MEASURES
The primary end point was the area covered by pathologic corneal blood vessels, which was measured morphometrically on digitized slit-lamp pictures using image analysis techniques.
RESULTS
GS-101 eye drops were well tolerated. All serious and 95% of all other adverse events were categorized by the investigators as unrelated. In 3 patients, there was a potentially related side effect of ocular surface discomfort. At a dose of 86 microg/day (43 microg/drop), GS-101 eye drops produced a significant inhibition and regression of corneal neovascularization (-2.04+/-1.57% of total corneal area; P = 0.0047), whereas the low dose tended to stabilize it (0.07+/-2.94%; P = 0.2088) compared with placebo (0.89+/-2.15%), where corneal neovascularization progressed in all patients. There was no apparent benefit to the higher dose (1.60+/-7.63%).
CONCLUSIONS
The interim results of this phase II study suggest that GS-101 eye drops at an optimal dose of 86 microg/day are an effective and noninvasive approach specifically to inhibit and regress active corneal angiogenesis, a major risk factor for corneal graft transplantation and graft rejection. Safety concerns were not detected.
FINANCIAL DISCLOSURE(S): Proprietary or commercial disclosure may be found after the references.
目的
病理性角膜新生血管不仅会降低角膜透明度和视力,还是角膜移植术前和术后移植排斥反应最重要的危险因素之一。本研究的目的是测试基因信号(GS)-101滴眼液(一种针对胰岛素受体底物-1的反义寡核苷酸)与安慰剂相比,在抑制进行性角膜新生血管方面的耐受性和疗效。
设计
随机、双盲、多中心II期临床研究。
参与者和对照组
对40例因各种基础疾病导致进行性角膜新生血管且对传统治疗无反应的患者进行中期分析。
干预措施
在这项剂量探索研究中,将四组每组10例患者治疗3个月,比较3种剂量的GS-101(滴眼液,每日两次;每日总量分别为43、86和172微克)与安慰剂(每组10例患者)。
主要观察指标
主要终点是病理性角膜血管覆盖的面积,使用图像分析技术在数字化裂隙灯图片上进行形态学测量。
结果
GS-101滴眼液耐受性良好。所有严重不良事件和95%的其他不良事件被研究者归类为无关事件。3例患者出现了可能相关的眼表不适副作用。在每日剂量为86微克(每滴43微克)时,GS-101滴眼液对角膜新生血管产生了显著的抑制和消退作用(占角膜总面积的-2.04±1.57%;P = 0.0047),而与安慰剂(0.89±2.15%,所有患者角膜新生血管均进展)相比,低剂量组倾向于使其稳定(0.07±2.94%;P = 0.2088)。高剂量组(1.60±7.63%)没有明显益处。
结论
这项II期研究的中期结果表明,每日最佳剂量为86微克的GS-101滴眼液是一种有效且无创的方法,可特异性抑制和消退活跃的角膜血管生成,这是角膜移植和移植排斥的主要危险因素。未发现安全问题。
财务披露
专有或商业披露信息可在参考文献之后找到。
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