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神经营养因子在神经元细胞和非神经元细胞中与Trk受体相互作用方式的异同。

Similarities and differences in the way neurotrophins interact with the Trk receptors in neuronal and nonneuronal cells.

作者信息

Ip Nancy Y, Stitt Trevor N, Tapley Peter, Klein Rudiger, Glass David J, Fandl James, Greene Lloyd A, Barbacid Mariano, Yancopoulos George D

机构信息

Regeneron Pharmaceuticals, Inc., Tarrytown, New York 10591.

出版信息

Neuron. 1993 Feb;10(2):137-49. doi: 10.1016/0896-6273(93)90306-c.

Abstract

We have exploited a battery of approaches to address several controversies that have accompanied the expansion of the nerve growth factor (NGF) family of neurotrophic factors and the identification of the Trk tyrosine kinases as receptors for these factors. For example, we find that a recently cloned mammalian neurotrophin, known as either neurotrophin-4 or neurotrophin-5 and assigned widely differing receptor specificities, represents the functional counterpart of Xenopus neurotrophin-4 and is a "preferred" ligand for TrkB. However, its interactions with TrkB can be distinguished from those of brain-derived neurotrophic factor (BDNF) with TrkB. We also find that all of the Trks display similar dose responses to their "preferred" ligands in neuronal as compared with nonneuronal cells (i.e., NGF for TrkA, BDNF and NT-4/5 for TrkB, and NT-3 for TrkC), providing evidence against a role for accessory molecules expressed in neurons in generating receptors that would allow for responses to lower concentrations of the neurotrophins. However, we find that a neuronal environment does restrict the Trks in their ability to respond to their "nonpreferred" neurotrophin ligands.

摘要

我们运用了一系列方法来解决伴随神经营养因子神经生长因子(NGF)家族的扩展以及将Trk酪氨酸激酶鉴定为这些因子的受体而出现的几个争议。例如,我们发现最近克隆的一种哺乳动物神经营养因子,称为神经营养因子-4或神经营养因子-5,且具有广泛不同的受体特异性,它是非洲爪蟾神经营养因子-4的功能对应物,并且是TrkB的“首选”配体。然而,它与TrkB的相互作用可与脑源性神经营养因子(BDNF)与TrkB的相互作用区分开来。我们还发现,与非神经元细胞相比,所有Trk在神经元中对其“首选”配体均表现出相似的剂量反应(即,TrkA对应NGF,TrkB对应BDNF和NT-4/5,TrkC对应NT-3),这为反对神经元中表达的辅助分子在产生能够对较低浓度神经营养因子作出反应的受体方面发挥作用提供了证据。然而,我们发现神经元环境确实会限制Trk对其“非首选”神经营养因子配体作出反应的能力。

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