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迈向阿尔茨海默病的非侵入性神经生长因子疗法。

Towards non invasive nerve growth factor therapies for Alzheimer's disease.

作者信息

Cattaneo Antonino, Capsoni Simona, Paoletti Francesca

机构信息

European Brain Research Institute (EBRI) - Rita Levi Montalcini Foundation, Rome, Italy.

出版信息

J Alzheimers Dis. 2008 Oct;15(2):255-83. doi: 10.3233/jad-2008-15210.

Abstract

In the past thirty years, nerve growth factor (NGF) has received much attention for its potential role as a therapeutic agent for Alzheimer's disease (AD) due to its neurotrophic activities on basal forebrain cholinergic neurons. This attention has been renewed by recent findings that provide new causal links between defects in NGF signaling, transport or processing to the activation of the amyloidogenic route and, more generally, to AD neurodegeneration. Thus, the concept of therapeutic administration of human recombinant NGF in AD patients has a strong rationale, being further validated by recent and ongoing clinical trials with a gene-therapy approach. However, the widespread clinical application of gene or cell-therapy strategies for the delivery of NGF to AD patients seems unpractical, and it would be more advantageous to have non-invasive methods, that should also limit the adverse effects of NGF in activating nociceptive responses. This review will describe: 1) the data from preclinical and clinical studies underlying the rationale of NGF as a potential therapeutic agent for AD; and 2) the alternative strategies to reach adequate concentrations of NGF in relevant brain areas while preventing the onset of adverse effects.

摘要

在过去三十年中,神经生长因子(NGF)因其对基底前脑胆碱能神经元的神经营养活性,作为治疗阿尔茨海默病(AD)的潜在药物而备受关注。最近的研究结果为NGF信号传导、运输或加工缺陷与淀粉样蛋白生成途径的激活以及更普遍的AD神经退行性变之间提供了新的因果联系,这再次引发了人们的关注。因此,在AD患者中治疗性给予人重组NGF的概念具有充分的理论依据,最近正在进行的基因治疗方法临床试验进一步证实了这一点。然而,将基因或细胞治疗策略广泛应用于向AD患者递送NGF似乎不切实际,采用非侵入性方法会更具优势,这种方法还应限制NGF激活伤害性反应的不良反应。本综述将描述:1)NGF作为AD潜在治疗药物的理论依据的临床前和临床研究数据;2)在相关脑区达到足够浓度的NGF同时防止不良反应发生的替代策略。

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