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神经元活动在体内对轴突选择髓鞘形成具有偏向性。

Neuronal activity biases axon selection for myelination in vivo.

作者信息

Hines Jacob H, Ravanelli Andrew M, Schwindt Rani, Scott Ethan K, Appel Bruce

机构信息

Department of Pediatrics, University of Colorado School of Medicine, Aurora, Colorado, USA.

School of Biomedical Sciences, The University of Queensland, St. Lucia, Queensland, Australia.

出版信息

Nat Neurosci. 2015 May;18(5):683-9. doi: 10.1038/nn.3992. Epub 2015 Apr 6.

Abstract

An essential feature of vertebrate neural development is ensheathment of axons with myelin, an insulating membrane formed by oligodendrocytes. Not all axons are myelinated, but mechanisms directing myelination of specific axons are unknown. Using zebrafish, we found that activity-dependent secretion stabilized myelin sheath formation on select axons. When VAMP2-dependent exocytosis was silenced in single axons, oligodendrocytes preferentially ensheathed neighboring axons. Nascent sheaths formed on silenced axons were shorter in length, but when activity of neighboring axons was also suppressed, inhibition of sheath growth was relieved. Using in vivo time-lapse microscopy, we found that only 25% of oligodendrocyte processes that initiated axon wrapping were stabilized during normal development and that initiation did not require activity. Instead, oligodendrocyte processes wrapping silenced axons retracted more frequently. We propose that axon selection for myelination results from excessive and indiscriminate initiation of wrapping followed by refinement that is biased by activity-dependent secretion from axons.

摘要

脊椎动物神经发育的一个基本特征是轴突被髓鞘包裹,髓鞘是一种由少突胶质细胞形成的绝缘膜。并非所有轴突都有髓鞘,但指导特定轴突髓鞘形成的机制尚不清楚。利用斑马鱼,我们发现活动依赖性分泌稳定了特定轴突上的髓鞘形成。当单个轴突中依赖VAMP2的胞吐作用沉默时,少突胶质细胞优先包裹相邻的轴突。在沉默轴突上形成的新生髓鞘长度较短,但当相邻轴突的活动也受到抑制时,髓鞘生长的抑制就会解除。利用体内延时显微镜,我们发现在正常发育过程中,只有25%开始包裹轴突的少突胶质细胞突起会稳定下来,而且起始过程并不需要活动。相反,包裹沉默轴突的少突胶质细胞突起更频繁地回缩。我们提出,髓鞘形成的轴突选择源于过度且无差别地起始包裹,随后通过轴突活动依赖性分泌产生的偏向性进行优化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7955/4414883/905baf8fa825/nihms671661f1.jpg

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