Extensive Sprouting of Sensory Afferents and Hyperalgesia Induced by Conditional Expression of Nerve Growth Factor in the Adult Spinal Cord

Romero, Mario I.; Rangappa, Nagarathnamma; Li, Li; Lightfoot, Ellis; Garry, Mary G.; Smith, George M.

doi:10.1523/jneurosci.20-12-04435.2000

Cited by 166 publications

(164 citation statements)

References 78 publications

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“…The most obvious example here is NGF, which while promoting the robust regeneration of small-diameter peptidergic afferents into the spinal cord following rhizotomy also produces severe hyperalgesia. 163 One of the apparent issues is that NGF-treated axons far overshoot their targets 164,165 to terminate deep in the dorsal horn. Tang et al 166 have taken advantage of a developmental mechanism of axon repulsion in the spinal grey matter by transfecting ventral cells with semaphorin 3A.…”

Section: Myelin and Myelin Signaling: An Inhibitory Chorus Linementioning

confidence: 99%

“…While NGF has been shown to promote intraspinal sprouting of nociceptive primary afferents, 164,165 the usefulness of NGF in SCI is severely limited by its painful side effects (discussed above). 163 Exogenous NT-3 promotes sprouting of intact CST axons developmentally 197 and following rubrospinal tract ablation in adults. 184 Like neurotrophic factors, neutralizing inhibitory myelin and ECM molecules can promote sprouting of some intact systems: blocking Nogo-A promotes sprouting of adult CST axons, 198 and digestion of glial scarassociated CSPGs promotes behavioral recovery following dorsal column injury in the absence of robust regeneration of injured axons.…”

Section: Myelin and Myelin Signaling: An Inhibitory Chorus Linementioning

confidence: 99%

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Setting the stage for functional repair of spinal cord injuries: a cast of thousands

2005

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Here we review mechanisms and molecules that necessitate protection and oppose axonal growth in the injured spinal cord, representing not only a cast of villains but also a company of therapeutic targets, many of which have yet to be fully exploited. We next discuss recent progress in the fields of bridging, overcoming conduction block and rehabilitation after spinal cord injury (SCI), where several treatments in each category have entered the spotlight, and some are being tested clinically. Finally, studies that combine treatments targeting different aspects of SCI are reviewed. Although experiments applying some treatments in combination have been completed, auditions for each part in the much-sought combination therapy are ongoing, and performers must demonstrate robust anatomical regeneration and/or significant return of function in animal models before being considered for a lead role.Spinal Cord (2005) 43, 134-161.

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Section: Myelin and Myelin Signaling: An Inhibitory Chorus Linementioning

confidence: 99%

Section: Myelin and Myelin Signaling: An Inhibitory Chorus Linementioning

confidence: 99%

Setting the stage for functional repair of spinal cord injuries: a cast of thousands

2005

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“…A concern has always been that small pain ®bres may regenerate better than larger sensory axons, bringing with it the danger of worsening the pain that many people with spinal injuries su er: however, this has not been seen in experiments except where nerve growth factor, which acts on pain ®bres, has been increased in the cord. 5 In addition to the speci®c innervation from sensory and motor axons there is evidence that di use innvervation from serotonergic axons may be bene®cial. In rats with complete spinal transections a transplant of embryonic serotonergic neurones below the injury led to extensive innvervation by small serotonergic ®bres, and a considerable return of stepping and weightbearing function.…”

Section: How Many Axons Are Needed?mentioning

confidence: 99%

“…30 Nerve growth factor also promotes regeneration, but receptors for it are prominent on small pain axons, so hyperalgesia can be caused by its presence in excess. 5 An alternative to the application of neurotrophins is to apply treatments that have direct e ects on axonal signalling pathways. There is evidence that the positive e ects of neurotrophins are mediated via cyclic nucleotides, and that inhibitory molecules in the environment act via the small GTPase Rho.…”

Section: Why Do Axons Fail To Regenerate In the Spinal Cord?mentioning

confidence: 99%

“…Treatment of the cord with neurotrophins produces local sprouting of axons with functional e ects. 5,52,53 One of these e ects is not helpful, which is NGF-induced sprouting of pain ®bres, leading to hyperalgesia. Overall, despite the fact that there are now treatments that can in¯uence plasticity in the cord, there remains a need to establish whether these treatments could be helpful in animal models of partial cord damage, and therefore to patients with partial lesions of the cord.…”

Section: Why Do Axons Fail To Regenerate In the Spinal Cord?mentioning

confidence: 99%

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Repair of spinal cord injuries: where are we, where are we going?

Fawcett

2002

Spinal Cord

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Repairing the spinal cord has for a long time been a`holy grail' for neuroscientists. No achievement in neuroscience is more di cult to achieve, and none would have the same impact amongst the medical profession and the public. Yet no patient has yet bene®ted from a regeneration therapy. At last su cient progress has been made in the basic science of axon regeneration that treatments that would partially repair a spinal injury are imminent. A full repair of spinal injury still remains elusive. This review summarises progress to date, and suggests ways in which progress towards treatment of spinal injury patients might be made.

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