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首页> 美国卫生研究院文献>The Journal of Neuroscience >ZPK/DLK and MKK4 Form the Critical Gateway to Axotomy-Induced Motoneuron Death in Neonates
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ZPK/DLK and MKK4 Form the Critical Gateway to Axotomy-Induced Motoneuron Death in Neonates

机译:ZPK / DLK和MKK4形成了轴突切开术引起的新生儿动尿素死亡的关键途径

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Motoneuron death after transection of the axons (axotomy) in neonates is believed to share the same mechanistic bases as naturally occurring programmed cell death during development. The c-Jun N-terminal kinase pathway is activated in both forms of motoneuron death, but it remains unknown to what extent these two forms of motoneuron death depend on this pathway and which upstream kinases are involved. We found that numbers of facial motoneurons are doubled in neonatal mice deficient in either ZPK/DLK (zipper protein kinase, also known as dual leucine zipper kinase), a mitogen-activated protein kinase kinase kinase, or in MKK4/MAP2K4, a mitogen-activated protein kinase kinase directly downstream of ZPK/DLK, and that the facial motoneurons in those mutant mice are completely resistant to axotomy-induced death. Conditional deletion of MKK4/MAP2K4 in neurons further suggested that ZPK/DLK and MKK4/MAP2K4-dependent mechanisms underlying axotomy-induced death are motoneuron autonomous. Nevertheless, quantitative analysis of facial motoneurons during embryogenesis revealed that both ZPK/DLK and MKK4/MAP2K4-dependent and -independent mechanisms contribute to developmental elimination of excess motoneurons. In contrast to MKK4/MAP2K4, mice lacking MKK7/MAP2K7, another mitogen-activated protein kinase kinase directly downstream of ZPK/DLK, conditionally in neurons did not have excess facial motoneurons. However, some MKK7/MAP2K7-deficient facial motoneurons were resistant to axotomy-induced death, indicating a synergistic effect of MKK7/MAP2K7 on axotomy-induced death of these facial motoneurons. Together, our study provides compelling evidence for the pivotal roles of the ZPK/DLK and MKK4/MAP2K4-dependent mechanism in axotomy-induced motoneuron death in neonates and also demonstrates that axotomy-induced motoneuron death is not identical to developmental motoneuron death with respect to the involvement of ZPK/DLK, MKK4/MAP2K4 and MKK7/MAP2K7.
机译:新生儿的轴突横断后(轴切术),Mourouron死亡被认为与发育过程中自然发生的程序性细胞死亡具有相同的机制基础。 c-Jun N末端激酶途径在两种形式的运动神经元死亡中均被激活,但尚不清楚这两种形式的运动神经元死亡在多大程度上取决于该途径以及涉及哪些上游激酶。我们发现,在缺乏ZPK / DLK(拉链蛋白激酶,也称为双重亮氨酸拉链激酶),促分裂原活化蛋白激酶激酶或MKK4 / MAP2K4(促细胞分裂剂)的新生小鼠中,面部运动神经元的数量增加了一倍。激活的蛋白激酶激酶直接位于ZPK / DLK的下游,并且这些突变小鼠中的面部运动神经元完全抗轴突切伤所致的死亡。神经元中MKK4 / MAP2K4的条件缺失进一步表明,轴突切伤所致死亡的ZPK / DLK和MKK4 / MAP2K4依赖性机制是运动神经元自主的。尽管如此,在胚胎发生过程中对面部运动神经元的定量分析显示,ZPK / DLK和MKK4 / MAP2K4依赖性和非依赖性机制均有助于过量运动神经元的发育消除。与MKK4 / MAP2K4相反,缺少MKK7 / MAP2K7(正好在ZPK / DLK下游的另一个有丝分裂原激活的蛋白激酶激酶)的小鼠有条件地在神经元中没有多余的面部运动神经元。然而,一些缺乏MKK7 / MAP2K7的面部运动神经元对轴突切开引起的死亡具有抗性,表明MKK7 / MAP2K7对这些面部运动神经元的轴突切开引起的死亡具有协同作用。总之,我们的研究为ZPK / DLK和MKK4 / MAP2K4依赖性机制在新生儿轴突切开运动神经元死亡中的关键作用提供了令人信服的证据,并且还证明了轴突切开引起的运动神经元死亡与发育性运动神经元死亡并不相同。 ZPK / DLK,MKK4 / MAP2K4和MKK7 / MAP2K7的参与。

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