Molecular biology of neurotrophic factors.

Bailliere's clinical neurology Pub Date : 1995-11-01
M Sendtner
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引用次数: 0

Abstract

The survival and functional maintenance of spinal motoneurones and of peripheral neurones, such as sensory, sympathetic and parasympathetic neurones, has been shown to depend on neurotrophic factors, both during the period of developmental cell death and in adulthood. A variety of such factors has been identified over recent years, among them factors of the NGF gene family, for example BDNF, NT-3, NT-4/5 and NT-6, and factors such as CNTF and LIF acting on neuronal target cells via receptor components shared with cytokines such as IL-6. In addition, pluripotent mitogens, such as IGF-I and IGF-II can support the survival of a variety of neuronal cell types, including spinal motoneurones both in cell culture and in vivo. The establishment of mice in which the genes for these factors and their receptors have been inactivated by homologous recombination has been a major step in the understanding of their physiological function. It is not clear so far whether or not similar gene defects in human are associated with any neurological disease. However, some of these factors have been demonstrated to be effective in animal models of neuropathy and motoneurone disorders, so that first clinical trials using these factors for symptomatic treatment of amyotrophic lateral sclerosis (ALS) and peripheral neuropathies have already been initiated.

神经营养因子的分子生物学。
脊髓运动神经元和周围神经元(如感觉、交感和副交感神经元)的存活和功能维持已被证明依赖于神经营养因子,无论是在发育细胞死亡期间还是在成年期。近年来已经发现了多种这样的因子,其中包括NGF基因家族的因子,如BDNF、NT-3、NT-4/5和NT-6,以及CNTF和LIF等因子通过与IL-6等细胞因子共享的受体组分作用于神经元靶细胞。此外,多能分裂原,如IGF-I和IGF-II,可以在细胞培养和体内支持多种神经细胞类型的存活,包括脊髓运动神经元。通过同源重组使这些因子及其受体基因失活的小鼠的建立是了解其生理功能的重要一步。目前尚不清楚人类类似的基因缺陷是否与任何神经系统疾病有关。然而,其中一些因子已被证明在神经病变和运动神经元疾病的动物模型中有效,因此,使用这些因子对症治疗肌萎缩侧索硬化症(ALS)和周围神经病变的首次临床试验已经开始。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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