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The effect of Jun dimerization on neurite outgrowth and motif binding

机译:Jun二聚化对神经突幼虫和基序结合的影响

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Axon regeneration is a necessary step toward functional recovery after spinal cord injury. The AP-1 transcription factor c-Jun has long been known to play an important role in directing the transcriptional response of Dorsal Root Ganglion (DRG) neurons to peripheral axotomy that results in successful axon regeneration. Here we performed ChlPseq for Jun in mouse DRG neurons after a sciatic nerve crush or sham surgery in order to measure the changes in Jun's DNA binding in response to peripheral axotomy. We found that the majority of Jun's injury responsive changes in DNA binding occur at putative enhancer elements, rather than proximal to transcription start sites. We also used a series of single polypeptide chain tandem transcription factors to test the effects of different Jun-containing dimers on neurite outgrowth in DRG, cortical and hippocampal neurons. These experiments demonstrated that dimers composed of Jun and Atf3 promoted neurite outgrowth in rat CNS neurons as well as mouse DRG neurons. Our work provides new insight into the mechanisms underlying Jun's role in axon regeneration.
机译:轴突再生是脊髓损伤后功能恢复的必要步骤。已知AP-1转录因子C-6月份在将背根神经节(DRG)神经元(DRG)神经元对外周轴突的转录响应中发挥重要作用,这导致成功的轴突再生。在这里,我们在坐骨神经粉碎或假手术后在小鼠DRG神经元中进行了CHLPSEQ,以便测量Jun的DNA结合的变化,以应对外周轴突。我们发现,大多数jun的伤病在推定的增强子元素中发生了DNA结合的反应变化,而不是转录起始位点。我们还使用一系列单一多肽链串联转录因子来测试DRG,皮质和海马神经元在神经沸肌产物上的不同jun-and的影响。这些实验表明,由Jun和ATF3组成的二聚体在大鼠CNS神经元以及小鼠DRG神经元中促进了神经突的产物。我们的工作提供了新的洞察Jun轴突再生在君兵中的作用机制。

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