营养补充剂Alzer®和Diamel预防严重糖尿病黄斑水肿的疗效

Juana Elvira Maciques Rodríguez, M. Muñoz, Eduardo Cabrera Rode, L. Piñó, R. Sáinz, T. G. Calero, M. Puig, J. L. Anta, R. Santiesteban, Yordanka Marrero Álvarez, Eduardo Sanz Navares
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引用次数: 0

摘要

黄斑水肿是糖尿病患者低视力的主要原因。激光光凝仍然是治疗的选择,同时使用类固醇和抗血管生成,但这些治疗包括可能的眼部并发症。营养补充剂Alzer(其主要活性成分是银杏叶,一种强大的抗氧化剂,对血管因子和氧化损伤起作用,这是糖尿病性黄斑水肿发病机制的两种机制),已用于其他非糖尿病性黄斑疾病,与Diamel营养补充剂一起已被证明对血糖控制有效,并且可以通过减少黄斑视网膜的厚度和防止其他更难以治疗的晚期临床表现的进展,成为轻度至中度黄斑水肿的治疗选择。目的:探讨Alzer联合Diamel对轻度至中度糖尿病性黄斑水肿患者黄斑视网膜厚度的减薄效果。材料与方法:对2016年1月至2016年12月在哈瓦那内分泌研究所眼科就诊的64例非重度糖尿病黄斑水肿非增殖性糖尿病视网膜病变患者进行II期双盲临床试验。治疗随机分为两组:一组接受Alzer + Diamel治疗(n = 32),另一组接受Alzer安慰剂+ Diamel安慰剂治疗(n = 32)。所有患者在治疗开始时和随访1年后进行初步临床评估、血液检查和眼科评估。结果:研究结束后,Alzer和Diamel治疗组黄斑厚度均有明显改善。这种厚度的减少在左眼有统计学意义。治疗一年后视力未见下降。不良事件轻微且罕见。结论:Alzer和Diamel组未发生严重黄斑水肿。在试验组中获得的临床但不具有统计学意义的成功证明了关于所研究产品功效的协议假设。这个小样本的阳性结果导致了进行更大规模研究(III期)的建议。临床试验已在clinical Trials.gov注册,识别码:NCT03533478。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Efficacy of Alzer® and Diamel, Nutritional Supplements, in the Prevention of Severe Diabetic Macular Edema
Introduction: Macular edema is the main cause of low vision in diabetic patients. Laser photocoagulation continues to be the treatment of choice in conjunction with the use of steroids and anti-angiogenics, but these treatments include possible ocular complications. The nutritional supplement Alzer (whose primary active ingredient is Ginkgo biloba, a powerful antioxidant that acts on vascular factors and oxidative damage, which are two of the mechanisms implicated in the pathogenesis of diabetic macular edema), which has been used on other non-diabetic macular conditions, along with the Diamel nutritional supplement has been shown to be effective on glycemic control and could represent a treatment alternative for mild to moderate macular edema by reducing the thickness of the macular retina and preventing the progression of other more advanced clinical presentations that are harder to treat. Objective: Identify the effect of Alzer along with Diamel in reduction of the thickness of the macular retina among patients with mild to moderate diabetic macular edema. Materials and Methods: A phase II double-blind clinical trial was conducted in 64 patients with non-severe diabetic macular edema over the course of non-proliferative diabetic retinopathy, who attended the ophthalmology service of the Institute of Endocrinology of Havana from January 2016 to December 2016. The treatment was randomly assigned to two groups: one received Alzer plus Diamel (n = 32) and the other group received Alzer placebo + Diamel placebo (n = 32). All patients were given an initial clinical evaluation, blood testing and ophthalmological evaluation at the start of treatment and after one year of follow-up. Results: There was a clinical improvement in the macular thickness upon the conclusion of the study in the patients treated with Alzer and Diamel. This decrease in thickness was statistically significant in the left eye. There was no decrease in visual acuity one year after treatment. Adverse events were mild and uncommon. Conclusions: Severe macular edema did not evolve in the Alzer and Diamel group. The clinical, but not statistically significant, success obtained in the experimental group proves the protocol hypothesis regarding the efficacy of the product being researched. The positive results in this small sample lead to the suggestion of performing larger-scale studies (Phase III). The clinical trial was registered in Clinical Trials.gov Identifier: NCT03533478.
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