dorsal funiculus
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2021 ◽  
Vol 22 (18) ◽  
pp. 10123
Author(s):  
Ken Muramatsu ◽  
Satoshi Shimo ◽  
Toru Tamaki ◽  
Masako Ikutomo ◽  
Masatoshi Niwa

This study aimed to reveal functional and morphological changes in the corticospinal tract, a pathway shown to be susceptible to diabetes. Type 1 diabetes was induced in 13-week-old male Wistar rats administered streptozotocin. Twenty-three weeks after streptozotocin injection, diabetic animals and age-matched control animals were used to demonstrate the conduction velocity of the corticospinal tract. Other animals were used for morphometric analyses of the base of the dorsal funiculus of the corticospinal tract in the spinal cord using both optical and electron microscopy. The conduction velocity of the corticospinal tract decreased in the lumbar spinal cord in the diabetic animal, although it did not decrease in the cervical spinal cord. Furthermore, atrophy of the fibers of the base of the dorsal funiculus was observed along their entire length, with an increase in the g-ratio in the lumbar spinal cord in the diabetic animal. This study indicates that the corticospinal tract fibers projecting to the lumbar spinal cord experience a decrease in conduction velocity at the lumbar spinal cord of these axons in diabetic animals, likely caused by a combination of axonal atrophy and an increased g-ratio due to thinning of the myelin sheath.


2017 ◽  
Vol 2 (1) ◽  
pp. 9-13
Author(s):  
Christine Radtke ◽  
Jeffery D. Kocsis ◽  
Wolfgang Baumgärtner ◽  
Peter M. Vogt

AbstractAxon visualization techniques are important in assessing the efficacy of interventional approaches to stimulate neural regeneration. Whereas the labeling of descending tracts in the spinal cord has been well established using the intracortical injection of biotin dextran amine (BDA), the labeling of ascending sensory fibers of the dorsal funiculus is more problematic. Fluoro-Ruby (FR; dextran tetramethylrhodamine; MW 10,000) is a bidirectional permanent tracer, but the retrograde tracing of fibers is particularly prominent, and FR is a highly sensitive tracer that can be applied in discrete injection sites. In the present report, we used FR to efficiently label ascending fibers in the dorsal columns of the rat spinal cord. After transplantation of olfactory ensheathing cells into the transected dorsal funiculus, the application of FR was able to detect regenerating ascending fibers in the spinal cord. Regenerated fibers crossing the injury site were labeled and easily identified. It is likely that the tracer was taken up by damaged fibers. As additional advantages, the labeling is resistant to photobleaching and no additional tissue processing is necessary for visualization. It can be used for in vivo as well as in vitro injections. The findings indicate that FR can be used as a reliable fluorescent marker to study ascending regenerated fibers in the spinal cord axonal regeneration.


Author(s):  
Esther Herberich ◽  
Christine Hassler ◽  
Torsten Hothorn

AbstractMuch biological experimental data are represented as curves, including measurements of growth, hormone, or enzyme levels, and physical structures. Here we consider the multiple testing problem of comparing two or more nonlinear curves. We model smooth curves of unknown form nonparametrically using penalized splines. We use random effects to model subject-specific deviations from the group-level curve. We present an approach that allows examination of overall differences between the curves of multiple groups and detection of sections in which the curves differ. Adjusted


2013 ◽  
Vol 2013 ◽  
pp. 1-14 ◽  
Author(s):  
Frank Cloutier ◽  
Ilse Sears-Kraxberger ◽  
Krista Keachie ◽  
Hans S. Keirstead

The glial scar formed by reactive astrocytes and axon growth inhibitors associated with myelin play important roles in the failure of axonal regeneration following central nervous system (CNS) injury. Our laboratory has previously demonstrated that immunological demyelination of the CNS facilitates regeneration of severed axons following spinal cord injury. In the present study, we evaluate whether immunological demyelination is accompanied with astrogliosis. We compared the astrogliosis and macrophage/microglial cell responses 7 days after either immunological demyelination or a stab injury to the dorsal funiculus. Both lesions induced a strong activated macrophage/microglial cells response which was significantly higher within regions of immunological demyelination. However, immunological demyelination regions were not accompanied by astrogliosis compared to stab injury that induced astrogliosis which extended several millimeters above and below the lesions, evidenced by astroglial hypertrophy, formation of a glial scar, and upregulation of intermediate filaments glial fibrillary acidic protein (GFAP). Moreover, a stab or a hemisection lesion directly within immunological demyelination regions did not induced astrogliosis within the immunological demyelination region. These results suggest that immunological demyelination creates a unique environment in which astrocytes do not form a glial scar and provides a unique model to understand the putative interaction between astrocytes and activated macrophage/microglial cells.


2010 ◽  
Vol 104 (3) ◽  
pp. 1707-1716 ◽  
Author(s):  
Tatsuya Umeda ◽  
Masahito Takahashi ◽  
Kaoru Isa ◽  
Tadashi Isa

Neonatally hemidecorticated rats show fairly normal reaching and grasping behaviors of the forelimb contralateral to the lesion at the adult stage. Previous experiments using an anterograde tracer showed that the corticospinal fibers originating from the sensorimotor cortex of the intact side projected aberrant collaterals to the spinal gray matter on the ipsilateral side. The present study used electrophysiological methods to investigate whether the aberrant projections of the corticospinal tract mediated the pyramidal excitation to the ipsilateral forelimb motoneurons and, if so, which pathways mediate the effect in the hemidecorticated rats. Electrical stimulation to the intact medullary pyramid elicited bilateral negative field potentials in the dorsal horn of the spinal cord. In intracellular recordings of forelimb motoneurons, oligosynaptic pyramidal excitation was detected on both sides of the spinal cord in the hemidecorticated rats, whereas pyramidal excitation of motoneurons on the side ipsilateral to the stimulation was much smaller in normal rats. By lesioning the dorsal funiculus at the upper cervical level, we clarified that the excitation was transmitted to the ipsilateral motoneurons by at least two pathways: one via the corticospinal tract and spinal interneurons and the other via the cortico-reticulo-spinal pathways. These results suggested that in the neonatally hemidecorticated rats, the forelimb movements on the side contralateral to the lesion were modulated by motor commands through the indirect ipsilateral descending pathways from the sensorimotor cortex of the intact side either via the spinal interneurons or reticulospinal neurons.


2010 ◽  
Vol 1 (1) ◽  
Author(s):  
Sarah Galley ◽  
Gavin Clowry

AbstractA CST-YFP transgenic mouse has been developed for the study of the corticospinal tract in which yellow fluorescent protein is expressed under the control of thy1 and emx1 promoters in order to restrict expression to forebrain neurones. We explored plasticity of the developing corticospinal tract of these mice following a unilateral lesion to the sensorimotor cortex at postnatal day 7. The extent of innervation of the cervical spinal cord at time points post-lesion was assessed by measuring density of immunoperoxidase reactivity for yellow fluorescent protein in the dorsal funiculi and a defined region of each dorsal horn, and by counting immunoreactive axonal varicosities in the ventral horns. Two/three days post-lesion, the density of immunoreactivity in the dorsal horn contralateral to the lesion was reduced proportional to the decrease in positive fibres in the dorsal funiculus, however density of immunoreactive varicosities in the ventral horn was more resistant to loss. Over a three week period, immunoreactive axonal processes in the grey matter increased on the contralateral side, particularly in the ventral horn, but without an increase in immunopositive fibres in the contralateral dorsal funiculus, demonstrating sprouting of surviving immunoreactive fibres to replace lesioned corticospinal axons. However, the origin of sprouting fibres could not be identified with confidence as parallel observations revealed strongly immunoreactive neuronal cell bodies in the spinal cord, medulla and red nucleus. We have demonstrated plasticity in response to a developmental lesion but discovered a drawback to using these mice if visualisation of individual axons is enhanced by immunohistochemistry.


Author(s):  
William D. Willis ◽  
Richard E. Coggeshall

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