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抗Syndecan 2抗体治疗可减轻小鼠激光诱导性脉络膜新生血管的水肿形成和炎症反应。

Anti-Syndecan 2 Antibody Treatment Reduces Edema Formation and Inflammation of Murine Laser-Induced CNV.

作者信息

Corti Federico, Locri Filippo, Plastino Flavia, Perrotta Paola, Zsebo Krisztina, Ristori Emma, Yin Xiangyun, Song Eric, André Helder, Simons Michael

机构信息

Yale Cardiovascular Research Center, Department of Internal Medicine, Yale University School of Medicine, New Haven, CT, USA.

Department of Clinical Neuroscience, St. Erik Eye Hospital, Karolinska Institutet, Stockholm, Sweden.

出版信息

Transl Vis Sci Technol. 2025 Jan 2;14(1):10. doi: 10.1167/tvst.14.1.10.

Abstract

PURPOSE

Alteration of visual acuity in wet age-related macular degeneration (AMD) is mostly driven by vascular endothelial growth factor A (VEGF-A)-induced edema from leaky newly forming blood vessels below the retina layers. To date, all therapies aimed at alleviation of this process have relied on inhibition of VEGF-A activity. Although effective in preventing vascular leak and edema, this approach also leads to the loss of normal vasculature and multiple related side effects.

METHODS

We have developed an alternative strategy that uses anti-syndecan-2 polyclonal antibody (anti-Sdc2 pAb) to block VEGF-A-induced permeability without interfering with other VEGF-A activities. The effect of anti-Sdc2 pAb therapy was assessed in vitro using a transendothelial electrical resistance (TEER) assay, as well as staining of the endothelial cell junction, and in vivo in the laser-induced choroidal neovascularization (CNV) model.

RESULTS

Anti-Sdc2 pAb blocked VEGF-A-induced permeability in vitro, and both local intravitreal injections and systemic intravenous treatments with anti-Sdc2 pAb were as effective as intravitreal anti-VEGF therapy in reducing edema, size of retinal lesions, and local inflammation in this model. Post-injury neovascularization was not affected by treatment with anti-Sdc2 pAb.

CONCLUSIONS

These findings indicate that anti-Sdc2 pAb therapy can be an effective alternative to anti-VEGF-A approaches for suppression of edema and to prevent retinal lesions in wet neovascular AMD (nAMD).

TRANSLATIONAL RELEVANCE

Intravitreal anti-Sdc2 treatment may avoid side effects observed with the long-term anti-VEGF therapy, and systemic treatment with an anti-Sdc2 pAb antibody can address the issues associated with repeated intravitreal injections.

摘要

目的

湿性年龄相关性黄斑变性(AMD)患者视力下降主要是由视网膜层下新生血管渗漏导致的血管内皮生长因子A(VEGF-A)诱导的水肿引起的。迄今为止,所有旨在缓解这一过程的治疗方法都依赖于抑制VEGF-A的活性。尽管这种方法在预防血管渗漏和水肿方面有效,但也会导致正常血管系统丧失以及多种相关副作用。

方法

我们开发了一种替代策略,使用抗syndecan-2多克隆抗体(抗Sdc2 pAb)来阻断VEGF-A诱导的通透性,而不干扰其他VEGF-A活性。使用跨内皮电阻(TEER)测定法以及内皮细胞连接染色在体外评估抗Sdc2 pAb治疗的效果,并在激光诱导的脉络膜新生血管(CNV)模型中进行体内评估。

结果

抗Sdc2 pAb在体外阻断了VEGF-A诱导的通透性,在该模型中,玻璃体内局部注射和抗Sdc2 pAb全身静脉治疗在减轻水肿、视网膜病变大小和局部炎症方面与玻璃体内抗VEGF治疗同样有效。抗Sdc2 pAb治疗对损伤后新生血管形成没有影响。

结论

这些发现表明,抗Sdc2 pAb治疗可以作为抗VEGF-A方法的有效替代方案,用于抑制湿性新生血管性AMD(nAMD)中的水肿和预防视网膜病变。

转化相关性

玻璃体内抗Sdc2治疗可能避免长期抗VEGF治疗中观察到的副作用,并且用抗Sdc2 pAb抗体进行全身治疗可以解决与反复玻璃体内注射相关的问题。

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