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新生大鼠轴浆运输减弱或眶下神经横断对脑干中单个三叉神经初级传入终末形态的影响。

Effects of neonatal attenuation of axoplasmic flow or transection of the rat's infraorbital nerve on the morphology of individual trigeminal primary afferent terminals in the brainstem.

作者信息

Goldstein F, Chiaia N L, Rhoades R W

机构信息

Department of Anatomy and Neurobiology, Medical College of Ohio, 3035 Arlington Avenue, Toledo, Ohio, 43614-5804, USA.

出版信息

Exp Neurol. 1999 Apr;156(2):283-93. doi: 10.1006/exnr.1999.7024.

Abstract

Attenuation of axoplasmic transport in the infraorbital nerve (ION), or transection of this trigeminal (V) branch at birth, results in degradation of the central cellular aggregates related to the mystacial vibrissae. However, blockade of axoplasmic transport does not result in the nearly 90% loss of ION ganglion cells that follows neonatal transection of this nerve. The present study was undertaken to further characterize the response of individual ION axons to attenuation of axoplasmic transport and to compare these effects to the changes observed following nerve transection. Neurobiotin injections were made into the V ganglion on postnatal day (P-) 6 in normal rats and animals that had vinblastine applied to the ION or received transection of the ION on P-0. Individual labeled fibers in the portions of V nucleus principalis (PrV) and subnucleus interpolaris (SpI) innervated by the ION were drawn from single sections with the aid of a computer. Morphological analysis of fibers drawn in SpI indicated no significant differences between axons from normal and vinblastine-treated animals. The fibers drawn from rats that sustained ION transection had significantly more branch points (P < 0.05) than those from either normal or vinblastine-treated animals. In PrV, fibers drawn from vinblastine-treated rats had a slightly, but significantly, larger total process length and cross-sectional area than those from the normal animals (P < 0.05). There were no other significant differences among the three groups of axons. These results support the conclusion that application of vinblastine to the developing ION does not dramatically alter the morphologic patterning of the central arbors of its axons.

摘要

眶下神经(ION)轴浆运输的减弱,或在出生时切断该三叉神经(V)分支,会导致与触须相关的中央细胞聚集体退化。然而,轴浆运输的阻断并不会导致该神经在新生期切断后ION神经节细胞近90%的损失。本研究旨在进一步描述单个ION轴突对轴浆运输减弱的反应,并将这些效应与神经切断后观察到的变化进行比较。在出生后第6天(P-6),对正常大鼠以及在P-0时将长春碱应用于ION或接受ION切断的动物的V神经节进行神经生物素注射。借助计算机从单张切片中绘制出ION支配的三叉神经主核(PrV)和极间亚核(SpI)部分中的单个标记纤维。对SpI中绘制的纤维进行形态学分析表明,正常动物和长春碱处理动物的轴突之间没有显著差异。与正常或长春碱处理动物的纤维相比,ION切断大鼠的纤维分支点明显更多(P < 0.05)。在PrV中,长春碱处理大鼠的纤维总长度和横截面积略大,但显著大于正常动物的纤维(P < 0.05)。三组轴突之间没有其他显著差异。这些结果支持以下结论:在发育中的ION上应用长春碱不会显著改变其轴突中央分支的形态模式。

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