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基于通路的治疗方法治疗年龄相关性黄斑变性:新兴治疗选择的综合调查。

Pathway-based therapies for age-related macular degeneration: an integrated survey of emerging treatment alternatives.

机构信息

Institute of Ophthalmology and Visual Science, University of Medicine and Dentistry of New Jersey, New Jersey Medical School, Newark, New Jersey 07103, USA.

出版信息

Retina. 2010 Oct;30(9):1350-67. doi: 10.1097/IAE.0b013e3181f57e30.

Abstract

PURPOSE

To review treatments under development for age-related macular degeneration (AMD) in the context of current knowledge of AMD pathogenesis.

METHODS

Review of the scientific literature published in English.

RESULTS

Steps in AMD pathogenesis that appear to be good targets for drug development include 1) oxidative damage; 2) lipofuscin accumulation; 3) chronic inflammation; 4) mutations in the complement pathway; and 5) noncomplement mutations that influence chronic inflammation and/or oxidative damage (e.g., mitochondria and extracellular matrix structure). Steps in neovascularization that can be targeted for drug development and combination therapy include 1) angiogenic factor production; 2) factor release; 3) binding of factors to extracellular receptors (and activation of intracellular signaling after receptor binding); 4) endothelial cell activation (and basement membrane degradation); 5) endothelial cell proliferation; 6) directed endothelial cell migration; 7) extracellular matrix remodeling; 8) tube formation; and 9) vascular stabilization.

CONCLUSION

The era of pathway-based therapy for the early and late stages of AMD has begun. At each step in the pathway, a new treatment could be developed, but complete inhibition of disease progression will likely require a combination of the various treatments. Combination therapy will likely supplant monotherapy as the treatment of choice because the clinical benefits (visual acuity and frequency of treatment) will likely be superior to monotherapy in preventing the late-stage complications of AMD.

摘要

目的

根据 AMD 发病机制的现有知识,综述与年龄相关性黄斑变性(AMD)相关的治疗方法。

方法

对英文发表的科学文献进行综述。

结果

AMD 发病机制中似乎是药物开发的良好靶点的步骤包括 1)氧化损伤;2)脂褐素积累;3)慢性炎症;4)补体途径突变;以及 5)影响慢性炎症和/或氧化损伤的非补体突变(例如,线粒体和细胞外基质结构)。可针对药物开发和联合疗法靶向的新生血管形成步骤包括 1)血管生成因子的产生;2)因子释放;3)因子与细胞外受体的结合(以及受体结合后细胞内信号的激活);4)内皮细胞的激活(以及基底膜的降解);5)内皮细胞的增殖;6)定向内皮细胞迁移;7)细胞外基质重塑;8)管形成;以及 9)血管稳定。

结论

基于途径的 AMD 早期和晚期治疗的时代已经开始。在该途径的每个步骤中,都可以开发出新的治疗方法,但要完全抑制疾病进展,可能需要将各种治疗方法结合起来。联合治疗可能会取代单一疗法成为首选治疗方法,因为在预防 AMD 的晚期并发症方面,联合治疗在提高视力和减少治疗频率方面的临床获益可能优于单一疗法。

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