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胰岛素样生长因子信号系统与肌萎缩侧索硬化症的神经营养因子治疗策略。

The insulin-like growth factor signaling system and ALS neurotrophic factor treatment strategies.

作者信息

Festoff B W, Yang S X, Vaught J, Bryan C, Ma J Y

机构信息

Neurobiology Research Laboratory (151), VA Medical Center, Kansas City, MO 64128, USA.

出版信息

J Neurol Sci. 1995 May;129 Suppl:114-21. doi: 10.1016/0022-510x(95)00080-l.

DOI:10.1016/0022-510x(95)00080-l
PMID:7595601
Abstract

Because of its multi-faceted potential as a neurotrophic factor, insulin-like growth factor I (IGF-I) has been given to hundreds of ALS patients world-wide. Unlike some patients with post-polio syndrome and fragile elderly males, it is unclear whether any of these patients possess disturbances in IGF signaling. We found that about 25% of ALS patients in a controlled trial of human growth hormone (hGH) had lower or higher than normal IGF-I serum levels. Many ALS patients do have some of the characteristics of type II diabetes mellitus, where IGF-I therapy is also under way. In addition, in type I diabetes significant increase in a circulating molecule that binds IGF-I, IGF-I binding protein 1 (IGFBP-1), occurs along with reduced IGF-I, when neuropathic complications are prominent. We have studied the response of IGFBPs in ALS patients to subcutaneous rhIGF-I and found transient induction of IGFBP-1. Studies related to the IGFBPs have not been done in familial ALS (FALS) patients. However, the gene for another IGFBP, BP-2, co-localizes with the gene for juvenile ALS (ALSJ) on chromosome 2. IGF-I has been given to several models of motor neuron degeneration in the mouse, including motor neuron disease and wobbler, with beneficial effects. However, it is also not known whether any accepted genetic mouse model of motor neuron degeneration possesses any disturbance in the IGF signaling system.

摘要

由于胰岛素样生长因子I(IGF-I)作为一种神经营养因子具有多方面的潜力,全球已有数百名肌萎缩侧索硬化症(ALS)患者接受了IGF-I治疗。与一些患有小儿麻痹后遗症的患者和体弱的老年男性不同,目前尚不清楚这些患者中是否有任何IGF信号传导紊乱的情况。我们发现在一项人类生长激素(hGH)对照试验中,约25%的ALS患者的IGF-I血清水平低于或高于正常水平。许多ALS患者确实具有II型糖尿病的一些特征,针对II型糖尿病的IGF-I治疗也正在进行。此外,在I型糖尿病中,当神经病变并发症突出时,与IGF-I结合的循环分子IGF-I结合蛋白1(IGFBP-1)会显著增加,同时IGF-I水平降低。我们研究了ALS患者的IGF结合蛋白(IGFBPs)对皮下注射重组人IGF-I(rhIGF-I)的反应,发现IGFBP-1有短暂诱导现象。尚未对家族性ALS(FALS)患者进行与IGFBPs相关的研究。然而,另一种IGFBP即BP-2的基因与2号染色体上的青少年ALS(ALSJ)基因共定位。IGF-I已应用于小鼠运动神经元变性的多种模型中,包括运动神经元疾病和震颤小鼠模型,并产生了有益效果。然而,目前也不清楚任何公认的运动神经元变性基因小鼠模型是否存在IGF信号系统紊乱的情况。

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