人 NGF "无痛 "眼部给药治疗视网膜色素变性:一项体内研究。

IF 2.7 3区 医学 Q3 NEUROSCIENCES eNeuro Pub Date : 2024-09-18 Print Date: 2024-09-01 DOI:10.1523/ENEURO.0096-24.2024
Debora Napoli, Noemi Orsini, Giulia Salamone, Maria Antonietta Calvello, Simona Capsoni, Antonino Cattaneo, Enrica Strettoi
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引用次数: 0

摘要

视网膜色素变性(RP)是一种基因异质性疾病,至今仍无药可治。尽管致病基因突变通常不在视锥光感受器中表达,但这些细胞在视杆细胞死亡后不可避免地发生退化,从而导致失明。锥体 "旁观者 "退化的原因目前尚不清楚,但生存因子的减少、氧化应激和炎症都在其中发挥了作用。以这些普遍的生物过程为靶点是开发突变诊断疗法的一种策略,可以挽救大量 RP 患者的视力。支持神经元存活的经典方法是使用神经营养因子,如 NGF。本研究使用了无痛人 NGF(hNGFp),它是一种偏向 TrkA 受体的原生分子变体,对痛觉感受器的亲和力较低,作为疼痛诱导剂的活性有限;该分子具有与原生分子相同的神经营养能力,但对 p75NTR 受体的亲和力较低,而 p75NTR 受体已知会引发细胞凋亡。hNGFp 对大脑小胶质细胞具有公认的活性,可诱导小胶质细胞从高度活化的表型转换为更稳定的表型。然而,这种疗法抵消锥状体旁观变性的能力仍然有限。
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Human NGF "Painless" Ocular Delivery for Retinitis Pigmentosa: An In Vivo Study.

Retinitis pigmentosa (RP) is a family of genetically heterogeneous diseases still without a cure. Despite the causative genetic mutation typically not expressed in cone photoreceptors, these cells inevitably degenerate following the primary death of rods, causing blindness. The reasons for the "bystander" degeneration of cones are presently unknown but decrement of survival factors, oxidative stress, and inflammation all play a role. Targeting these generalized biological processes represents a strategy to develop mutation-agnostic therapies for saving vision in large populations of RP individuals. A classical method to support neuronal survival is by employing neurotrophic factors, such as NGF. This study uses painless human NGF (hNGFp), a TrkA receptor-biased variant of the native molecule with lower affinity for nociceptors and limited activity as a pain inducer; the molecule has identical neurotrophic power of the native form but a reduced affinity for the p75NTR receptors, known to trigger apoptosis. hNGFp has a recognized activity on brain microglial cells, which are induced to a phenotype switch from a highly activated to a more homeostatic configuration. hNGFp was administered to RP-like mice in vivo with the aim of decreasing retinal inflammation and also providing retinal neuroprotection. However, the ability of this treatment to counteract the bystander degeneration of cones remained limited.

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来源期刊
eNeuro
eNeuro Neuroscience-General Neuroscience
CiteScore
5.00
自引率
2.90%
发文量
486
审稿时长
16 weeks
期刊介绍: An open-access journal from the Society for Neuroscience, eNeuro publishes high-quality, broad-based, peer-reviewed research focused solely on the field of neuroscience. eNeuro embodies an emerging scientific vision that offers a new experience for authors and readers, all in support of the Society’s mission to advance understanding of the brain and nervous system.
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