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内溶酶体的有效轴突运输依赖于微管酪氨酸化和去酪氨酸化的平衡比例。

Efficient axonal transport of endolysosomes relies on the balanced ratio of microtubule tyrosination and detyrosination.

机构信息

RG Optobiology, Institute of Biology, Humboldt Universität zu Berlin, Berlin 10115, Germany.

Guest Group 'Neuronal Protein Transport', Center for Molecular Neurobiology, ZMNH, University Medical Center Hamburg-Eppendorf, Hamburg 20251, Germany.

出版信息

J Cell Sci. 2024 Apr 15;137(8). doi: 10.1242/jcs.261737. Epub 2024 Apr 30.

Abstract

In neurons, the microtubule (MT) cytoskeleton forms the basis for long-distance protein transport from the cell body into and out of dendrites and axons. To maintain neuronal polarity, the axon initial segment (AIS) serves as a physical barrier, separating the axon from the somatodendritic compartment and acting as a filter for axonal cargo. Selective trafficking is further instructed by axonal enrichment of MT post-translational modifications, which affect MT dynamics and the activity of motor proteins. Here, we compared two knockout mouse lines lacking the respective enzymes for MT tyrosination and detyrosination, and found that both knockouts led to a shortening of the AIS. Neurons from both lines also showed an increased immobile fraction of endolysosomes present in the axon, whereas mobile organelles displayed shortened run distances in the retrograde direction. Overall, our results highlight the importance of maintaining the balance of tyrosinated and detyrosinated MTs for proper AIS length and axonal transport processes.

摘要

在神经元中,微管(MT)细胞骨架为从细胞体到树突和轴突的远距离蛋白质运输提供了基础。为了维持神经元极性,轴突起始段(AIS)充当物理屏障,将轴突与体树突隔室分开,并作为轴突货物的过滤器。通过轴突中 MT 翻译后修饰的富集,进一步进行有选择性的运输,这影响 MT 动力学和运动蛋白的活性。在这里,我们比较了两种缺失 MT 酪氨酸化和去酪氨酸化各自酶的敲除小鼠系,发现这两种敲除都导致 AIS 缩短。来自这两种系的神经元还显示出存在于轴突中的内溶酶体的不可动分数增加,而可动细胞器在逆行方向上的运行距离缩短。总的来说,我们的结果强调了维持酪氨酸化和去酪氨酸化 MT 之间平衡对于适当的 AIS 长度和轴突运输过程的重要性。

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