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人胰岛素和结肠活性素:用于治疗阿尔茨海默病和肌萎缩侧索硬化症的神经细胞死亡抑制肽。

Humanin and colivelin: neuronal-death-suppressing peptides for Alzheimer's disease and amyotrophic lateral sclerosis.

作者信息

Matsuoka Masaaki, Hashimoto Yuichi, Aiso Sadakazu, Nishimoto Ikuo

机构信息

Department of Pharmacology, KEIO University School of Medicine, Shnanomachi, Tokyo, Japan.

出版信息

CNS Drug Rev. 2006 Summer;12(2):113-22. doi: 10.1111/j.1527-3458.2006.00113.x.

Abstract

Humanin (HN), a 24-amino-acid neuroprotective peptide, was originally found in the occipital lobe of an autopsied Alzheimer's disease (AD) patient. HN inhibits neuronal death by binding to its specific receptor on the cell membrane and triggering a Jak2/STAT3 prosurvival pathway. The activation of this pathway may represent a therapeutic approach to AD. HN also exhibits neuroprotective activity against toxicity by familial amyotrophic lateral sclerosis (ALS)-related mutant superoxide dismutase (SOD1). Recent investigations established that AGA-(C8R)-HNG17, a 17-amno-acid derivative of HN, is 10(5) times more potent as a neuroprotective than HN; at 10-picomolar and higher concentrations in vitro it completely suppresses neuronal death. Moreover, a 26-amino-acid peptide colivelin (CL), composed of activity-dependent neurotrophic factor (ADNF) C-terminally fused to AGA-(C8R)-HNG17, provides complete neuroprotection at 100-femtomolar or higher concentrations in vitro. A series of experiments using mouse AD and ALS models further established the efficacy of HN derivatives, including CL, against these diseases in vivo. HN and CL can be viewed as drug candidates for neuronal death suppression therapy in AD or ALS.

摘要

人胰岛素(HN)是一种由24个氨基酸组成的神经保护肽,最初在一名阿尔茨海默病(AD)尸检患者的枕叶中发现。HN通过与细胞膜上的特定受体结合并触发Jak2/STAT3促生存途径来抑制神经元死亡。该途径的激活可能代表了一种治疗AD的方法。HN还对家族性肌萎缩侧索硬化症(ALS)相关突变超氧化物歧化酶(SOD1)的毒性表现出神经保护活性。最近的研究表明,AGA-(C8R)-HNG17是HN的一种17个氨基酸的衍生物,其神经保护作用比HN强10^5倍;在体外10皮摩尔及更高浓度下,它能完全抑制神经元死亡。此外,一种由活性依赖性神经营养因子(ADNF)C末端与AGA-(C8R)-HNG17融合而成的26个氨基酸的肽colivelin(CL),在体外100飞摩尔及更高浓度下能提供完全的神经保护。一系列使用小鼠AD和ALS模型的实验进一步证实了包括CL在内的HN衍生物在体内对这些疾病的疗效。HN和CL可被视为AD或ALS中抑制神经元死亡治疗的候选药物。

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