1991
DOI: 10.1007/bf01186989
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Focal axonal injury: the early axonal response to stretch

Abstract: The development of a model for axonal injury in the optic nerve of the guinea pig has allowed analysis of early morphological changes within damaged axons. We provide evidence that the initial site of damage after stretch is the nodes of Ranvier, some of which develop 'nodal blebs'. The development of nodel blebs is correlated with the loss of subaxolemmal density, disruption of the neurofilament cytoskeleton and aggregation of membranous profiles of smooth endoplasmic reticulum. Nodal blebs are numerous 15 mi… Show more

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Cited by 87 publications
(57 citation statements)
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“…In response to excitotoxic perikaryal injury, this study found nodal changes in the form of bleb formation and abnormal accumulation of organelles in the paranodal region with no obvious myelin terminal loop retraction as early changes. These changes resembled the response observed after non-disruptive stretch injury, where accumulation of membranous organelles in the paranodal and internodal regions preceeded the nodal bleb formation related with loss of axolemmal undercoating [60]. …”
Section: Discussionmentioning
confidence: 58%
“…In response to excitotoxic perikaryal injury, this study found nodal changes in the form of bleb formation and abnormal accumulation of organelles in the paranodal region with no obvious myelin terminal loop retraction as early changes. These changes resembled the response observed after non-disruptive stretch injury, where accumulation of membranous organelles in the paranodal and internodal regions preceeded the nodal bleb formation related with loss of axolemmal undercoating [60]. …”
Section: Discussionmentioning
confidence: 58%
“…Equally compelling support for an axo-glial integration of function is provided by the disruption of the myelin structure or maintenance of the glial cell in Charcot-Marie-Tooth disease, a set of human hereditary neuropathies (Bergoffen et al, 1993;Martini, 2001), causing changes in axonal morphology and nerve impulse conduction. Pathological conditions in peripheral neuropathies are also found when constituent proteins of the node of Ranvier malfunction (Bergoffen et al, 1993;Griffin et al, 1996;Rasband et al, 2003;Sima, 1993), are deficiently expressed (Bhat et al, 2001;Boyle et al, 2001;Sherman et al, 2005;Weber et al, 1999) or after axonal ischemic injury (Waxman et al, 1992) and trauma (Maxwell et al, 1991).…”
Section: Discussionmentioning
confidence: 99%
“…39,78,79 Owing, in part, to the isolated nature of the white matter injury, these models have proven very useful in evaluating ultrastructural changes in axons after trauma as well as identifying pathological chemical cascades that may represent important therapeutic targets. 34,39,47,[78][79][80][81][82][83][84][85][86][87][88][89][90][91][92][93] These models, however, are not widely used or practical for high-throughput therapy evaluation. Nonetheless, they represent a potential stepwise bridge between in vitro and in vivo therapy development.…”
Section: Lissencephalic Animal Models Of Taimentioning
confidence: 99%