Literature DB >> 11514988

Chronic intrathecal infusions after spinal cord injury cause scarring and compression.

L L Jones1, M H Tuszynski.   

Abstract

Intrathecal infusions are used in a number of rodent studies to deliver substances to the injured spinal cord. Whereas this method has been successful in certain paradigms, two potential limitations of this model have not been extensively reported: (1) scar formation at the catheter tip, which can lead to infusion failure, and (2) damage to the spinal cord caused by the catheter itself. Thus, the purpose of the present study was threefold: (1) to determine intrathecal infusion efficiency over 14 days following spinal cord injury; (2) to examine possible secondary damage caused by intrathecal tubing; and (3) to explore whether alternative protocols that avoid such damage are effective. Adult Fischer 344 rats were subjected to spinal cord lesions at T7, followed by placement of an intrathecal catheter attached to an Alzet minipump. Seven or 14 days following injury and catheter placement, tube patency was evaluated by diffusion of Evans Blue dye from the minipump. Results indicate that infusion was efficient 7 days following injury but was markedly reduced after 14 days. Further, histology and immunocytochemistry 14 days after injury demonstrated compression damage to the cord where the tubing rested. Alternative protocols, including intrathecal infusions through metal cannulae, or "drip" infusions directly over the lesion, did not improve delivery. These data suggest that results from rodent studies using infusion from catheters placed adjacent to lesion sites may be attributable to acute or subacute effects of the delivered substance. Future rodent studies using intrathecal infusions should include rigorous evaluation of infusion efficiency and possible secondary tissue damage. Copyright 2001 Wiley-Liss, Inc.

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Mesh:

Year:  2001        PMID: 11514988     DOI: 10.1002/jemt.1144

Source DB:  PubMed          Journal:  Microsc Res Tech        ISSN: 1059-910X            Impact factor:   2.769


  28 in total

1.  Sponge-mediated lentivirus delivery to acute and chronic spinal cord injuries.

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2.  Intraspinal microinjection of chondroitinase ABC following injury promotes axonal regeneration out of a peripheral nerve graft bridge.

Authors:  Veronica J Tom; John D Houlé
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3.  Feasible stabilization of chondroitinase abc enables reduced astrogliosis in a chronic model of spinal cord injury.

Authors:  Andrea Raspa; Edoardo Bolla; Claudia Cuscona; Fabrizio Gelain
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4.  Gene delivery to overcome astrocyte inhibition of axonal growth: an in vitro model of the glial scar.

Authors:  Hannah M Tuinstra; Melissa M Ducommun; William E Briley; Lonnie D Shea
Journal:  Biotechnol Bioeng       Date:  2012-11-01       Impact factor: 4.530

Review 5.  Tissue Engineering Approaches to Modulate the Inflammatory Milieu following Spinal Cord Injury.

Authors:  Courtney M Dumont; Daniel J Margul; Lonnie D Shea
Journal:  Cells Tissues Organs       Date:  2016-10-05       Impact factor: 2.481

6.  Chondroitinase activity can be transduced by a lentiviral vector in vitro and in vivo.

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Journal:  J Neurosci Methods       Date:  2011-05-11       Impact factor: 2.390

7.  Sustained dual drug delivery of anti-inhibitory molecules for treatment of spinal cord injury.

Authors:  Thomas S Wilems; Shelly E Sakiyama-Elbert
Journal:  J Control Release       Date:  2015-06-27       Impact factor: 9.776

8.  Promoting directional axon growth from neural progenitors grafted into the injured spinal cord.

Authors:  Joseph F Bonner; Armin Blesch; Birgit Neuhuber; Itzhak Fischer
Journal:  J Neurosci Res       Date:  2010-05-01       Impact factor: 4.164

9.  Diffusion tensor imaging of cocaine-treated rodents.

Authors:  Ponnada A Narayana; Pallavi Ahobila-Vajjula; Jaivijay Ramu; Juan Herrera; Joel L Steinberg; F Gerard Moeller
Journal:  Psychiatry Res       Date:  2009-02-12       Impact factor: 3.222

10.  [Neurological complications and loss of efficacy with intrathecal pain therapy].

Authors:  D Kindler; C Maier; T Kagel; S Schulz; T Weiss; M Zenz
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