光周围全视网膜光凝治疗新生血管性年龄相关性黄斑变性的假想效果。

Ahmad M Mansour, Koushik Tripathy, Maurizio Battaglia Parodi
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引用次数: 0

摘要

背景:血管内皮生长因子(VEGF)是眼部血管生成的重要调节剂,包括新生血管性年龄相关性黄斑变性(nAMD)。玻璃体内注射抗vegf是大多数视网膜血管疾病的基准治疗方法,包括nAMD、糖尿病黄斑病变和继发于视网膜静脉闭塞的黄斑水肿。抗vegf治疗是一种高频、耗时、不划算的治疗方法,特别是在资源有限的国家和地区。这种治疗很容易受到限制,而且在实践中,维持长期的周期性护理对患者来说是具有挑战性的。假设:光周围全视网膜光凝(PPRP)在赤道前以轻度形式应用(几乎不可见轻度浅灰色标记),以免危及视野。PPRP可减轻引起新生血管形成的缺血,并降低视网膜周围的代谢需求。PPRP降低2型糖尿病合并增殖性糖尿病视网膜病变患者血清血管生成素-2和VEGF水平。我们建议使用轻型PPRP抑制VEGF的分泌,旨在减弱VEGF的驱动,阻止nAMD眼脉络膜新生血管的生长。我们的治疗方案基于两个概念:首先,nAMD是一种影响后段的弥漫性或广泛性疾病;第二,PPRP对糖尿病视网膜病变的消退非常有效。据报道,PPRP在黄斑水肿(糖尿病或静脉闭塞)抵抗VEGF拮抗剂的情况下是成功的。当玻璃体内注射VEGF拮抗剂不可行时,轻度PPRP可作为nAMD的预防、辅助治疗或单药治疗。结论:已建立的轻度PPRP治疗可能是一种有希望的一次性,具有成本效益的治疗或预防nAMD患者或高风险。这种建议的方式可能适合有注射恐惧症的患者,或者更喜欢一次性负担得起的治疗,而不是长期每月去看视网膜医生。未来的试验需要验证这种建议的治疗方式在选定的nAMD患者中的安全性和有效性。
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A hypothetical therapeutic effect of light peripheral panretinal photocoagulation in neovascular age-related macular degeneration.

Background: Vascular endothelial growth factor (VEGF) is a significant modulator of ocular angiogenesis, including that of neovascular age-related macular degeneration (nAMD). Intravitreal injection of anti-VEGF is the benchmark treatment for most retinal vascular diseases, including nAMD, diabetic maculopathy, and macular edema secondary to retinal venous occlusion. Anti-VEGF treatment is a high-frequency, time-consuming, non-cost-effective therapy, especially in countries and regions with limited resources. This treatment is easily restricted, and in practice, maintaining long-term periodic care is challenging for patients.

Hypothesis: Light peripheral panretinal photocoagulation (PPRP) is applied in a mild form (barely visible mild light gray mark) anterior to the equator so as not to jeopardize the visual field. PPRP lessens the ischemia that causes neovascularization and decreases the metabolic demand in the peripheral retina. PPRP reduces serum angiopoietin-2 and VEGF levels in patients with type 2 diabetes mellitus with proliferative diabetic retinopathy. We propose using light PPRP to suppress VEGF secretion, aiming to attenuate the VEGF drive and halt choroidal neovascular growth in eyes with nAMD. Our regimen is based on two concepts: first, nAMD is a diffuse or generalized disease that affects the posterior segment; and second, PPRP is very effective in regressing diabetic retinopathy. PPRP has reportedly been successful in cases of macular edema (diabetic or following venous occlusion) resistant to VEGF antagonists. Light PPRP may be used as prophylaxis, adjunctive treatment, or monotherapy in nAMD when intravitreal injections of VEGF antagonists are not feasible.

Conclusions: The established light PPRP therapy could be promising as a one-time, cost-effective therapy or prophylaxis in patients with nAMD or at high risk. This proposed modality could be suitable for patients who have injection phobia or prefer a one-time affordable therapy to the long-term monthly visits to retinologists. Future trials are necessary to verify the safety and efficacy of this proposed treatment modality in selected patients with nAMD.

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CiteScore
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19
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