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The p75 nerve growth factor receptor mediates survival or death depending on the stage of sensory neuron development.

机译:根据感觉神经元发育的阶段,p75神经生长因子受体介导生存或死亡。

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摘要

The function of the low-affinity nerve growth factor (NGF) receptor, p75NGFR, in regulating neuronal survival during development is unclear. The sensory deficit in mice with mutated p75NGFR suggests it is necessary for development of sensory neurons; however, whether it is required, in addition to trkA, for signal transduction or is more involved in localization of NGF is unresolved. In this study we demonstrate, in vitro, that lowering the levels of p75NGFR expression in sensory neurons with antisense oligonucleotides largely prevents the NGF-mediated survival of sensory neurons from embryonic day 12 and 15 mice but increases the survival of embryonic day 19 and postnatal day 2 sensory neurons in the absence of NGF. Thus, the p75NGFR is required for NGF-mediated survival in neurons at the stage of target innervation but can mediate an apoptotic signal at a later stage of cell development. Thus, p75NGFR undergoes a switch in function in the perinatal period: during embryogenesis it is required, probably with trkA, to mediate neuronal survival in the presence of NGF, but in the early postnatal period it acts as a constitutive death signal in the absence of NGF.
机译:低亲和力神经生长因子(NGF)受体p75NGFR在发育过程中调节神经元存活的功能尚不清楚。 p75NGFR突变的小鼠的感觉缺陷表明,感觉神经元的发育是必要的。然而,除了trkA以外,是否还需要信号转导或更多地参与NGF的定位尚未解决。在这项研究中,我们在体外证明,使用反义寡核苷酸降低感觉神经元中p75NGFR的表达水平,可以很大程度上阻止NGF介导的从胚胎12天和15天小鼠的感觉神经元存活,但可以增加胚胎19天和出生后一天的存活。 NGF缺失时2个感觉神经元。因此,在靶神经支配阶段神经元中NGF介导的存活需要p75NGFR,但在细胞发育的后期可介导凋亡信号。因此,p75NGFR在围产期会发生功能转换:在胚胎发生过程中,可能需要与trkA一起在NGF存在的情况下介导神经元的存活,但是在产后早期,p75NGFR会在不存在NGF的情况下作为组成性死亡信号。 NGF。

著录项

  • 作者

    Barrett, G L; Bartlett, P F;

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  • 年度 1994
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  • 原文格式 PDF
  • 正文语种 en
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