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L2/HNK-1碳水化合物优先由重新支配的周围神经中先前与运动轴突相关的施万细胞表达。

The L2/HNK-1 carbohydrate is preferentially expressed by previously motor axon-associated Schwann cells in reinnervated peripheral nerves.

作者信息

Martini R, Schachner M, Brushart T M

机构信息

Department of Neurobiology, Swiss Federal Institute of Technology, Hönggerberg, Zürich.

出版信息

J Neurosci. 1994 Nov;14(11 Pt 2):7180-91. doi: 10.1523/JNEUROSCI.14-11-07180.1994.

Abstract

The carbohydrate epitope L2/HNK-1 (hereafter designated L2) is expressed in the adult mouse by myelinating Schwann cells of ventral roots and muscle nerves, but rarely by those of dorsal roots or cutaneous nerves. Since substrate-coated L2 glycolipids promote outgrowth of cultured motor but not sensory neurons, L2 may thus influence the preferential reinnervation of muscle nerves by regenerating motor axons in vivo. In the present study, we have analyzed the influence of regenerating axons on L2 expression by reinnervated Schwann cells by directing motor or sensory axons into the muscle and cutaneous branches of femoral nerves of 8-week-old mice. We observed that regenerating axons from cutaneous branches did not lead to immunocytochemically detectable L2 expression in muscle or cutaneous nerve branches. Axons regenerating from muscle branches led to a weak L2 expression by few Schwann cells of the cutaneous branch, but provoked a strong L2 expression by many Schwann cells of the muscle branch. Myelinating Schwann cells previously associated with motor axons thus differed from previously sensory axon-associated myelinating Schwann cells in their ability to express L2 when contacted by motor axons. This upregulation of L2 expression during critical stages of reinnervation may provide motor axons regenerating into the appropriate, muscle pathways with an advantage over those regenerating into the inappropriate, sensory pathways.

摘要

碳水化合物表位L2/HNK-1(以下简称L2)在成年小鼠中由腹根和肌肉神经的髓鞘形成雪旺细胞表达,但背根或皮神经的髓鞘形成雪旺细胞很少表达。由于包被底物的L2糖脂促进培养的运动神经元而非感觉神经元的生长,因此L2可能在体内通过再生运动轴突影响肌肉神经的优先再支配。在本研究中,我们通过将运动或感觉轴突导入8周龄小鼠股神经的肌肉和皮支,分析了再生轴突对再支配雪旺细胞L2表达的影响。我们观察到,来自皮支的再生轴突在肌肉或皮神经支中未导致免疫细胞化学可检测到的L2表达。从肌肉支再生的轴突导致皮支中少数雪旺细胞弱表达L2,但引发肌肉支中许多雪旺细胞强烈表达L2。因此,先前与运动轴突相关的髓鞘形成雪旺细胞在与运动轴突接触时表达L2的能力与先前与感觉轴突相关的髓鞘形成雪旺细胞不同。在再支配关键阶段L2表达的这种上调可能为再生到合适的肌肉通路中的运动轴突提供优于再生到不合适的感觉通路中的运动轴突的优势。

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