WldS, Nmnats and axon degeneration-progress in the past two decades

Yan, Feng; Yan, Tingting; He, Zhigang; Zhai, Qiwei

doi:10.1007/s13238-010-0021-2

Cited by 22 publications

(24 citation statements)

References 73 publications

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“…The in vivo protective effect of the Wld S protein has also been demonstrated in different species, such as rat and Drosophila (Feng et al, 2010). Additionally, the cation of the percentage of remaining distal axons before (0 hr) and after lesion (32 or 52 hr).…”

Section: Discussionmentioning

confidence: 90%

Overexpression of Wld^s or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish

Yan

Zheng

et al. 2010

J of Neuroscience Research

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Axon degeneration is supposed to be a therapeutic target for treating neurodegenerative diseases. Mauthner cells (M-cells) are ideal for studying axons in vivo because of their limited numbers, large size, and long axons. In this study, we labeled M-cells by single-cell electroporation with plasmids expressing DsRed2 or EGFP. Injury-induced axon degeneration in labeled M-cell was imaged under a confocal microscope, and we found that the Mauthner axons started to degenerate about 24 hr after lesion. The Wld(S) protein containing full-length Nmnat1 is well-known for its axon-protective function in many systems. Overexpression of Wld(S) in M-cells also greatly delayed axon degeneration in live zebrafish. Nmnat2 is the only Nmnat highly expressed in brain. Here we demonstrated that overexpression of Nmnat2 in M-cells significantly delayed axon degeneration in vivo, and disruption of the NAD synthesis activity of Nmnat2 markedly attenuated its axon-protective function. All these data show that injury-induced axon degeneration of M-cell has a mechanism similar to that in mammalians and would be a valuable model for studying axon degeneration in vivo.

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Section: Discussionmentioning

confidence: 90%

Overexpression of Wld^s or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish

Yan

Zheng

et al. 2010

J of Neuroscience Research

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“…This mutation arose spontaneously in C57Bl/6 mice, and it was demonstrated to cause delayed Wallerian degeneration in peripheral nerve after axotomy (Lunn et al, 1989). Wld S can delay axonal degeneration about ten-fold from a wide variety of genetic and toxin-inducing stimuli both in vivo and in vitro (Coleman and Freeman, 2010, Feng et al, 2010). Wld S is a chimeric protein composed of the N-terminal 70 amino acids of the ubiquitination factor Ube4b followed by a 18 amino acid linker region and the entire sequence of Nmnat1, a key enzyme in the biosynthesis of NAD + (Mack et al, 2001).…”

Section: Mechanisms Of Axon Degeneration Wldsmentioning

confidence: 99%

Axon degeneration in Parkinson's disease

Burke

O’Malley

2013

Experimental Neurology

380

291

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Parkinson's disease (PD) is the most common neurodegenerative disease of the basal ganglia. Like other adult-onset neurodegenerative disorders, it is without a treatment that forestalls its chronic progression. Efforts to develop disease-modifying therapies to date have largely focused on the prevention of degeneration of the neuron soma, with the tacit assumption that such approaches will forestall axon degeneration as well. We herein propose that future efforts to develop neuroprotection for PD may benefit from a shift in focus to the distinct mechanisms that underlie axon degeneration. We review evidence from human post-mortem studies, functional neuroimaging, genetic causes of the disease and neurotoxin models that axon degeneration may be the earliest feature of the disease, and it may therefore be the most appropriate target for early intervention. In addition, we present evidence that the molecular mechanisms of degeneration of axons are separate and distinct from those of neuron soma. Progress is being made in understanding these mechanisms, and they provide possible new targets for therapeutic intervention. We also suggest that the potential for axon re-growth in the adult central nervous system has perhaps been underestimated, and it offers new avenues for neurorestoration. In conclusion, we propose that a new focus on the neurobiology of axons, their molecular pathways of degeneration and growth, will offer novel opportunities for neuroprotection and restoration in the treatment of PD and other neurodegenerative diseases.

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“…Upon injury, the axon begins a degeneration process at the injury site and progresses distally. Morphologically, this process is characterized by a beading appearance followed by granular disintegration of the axons at, and distal to, the site of exposure [14]. Concurrently, the myelin sheath undergoes a degeneration phase, and the macrophages and Schwann cells function to clear the cellular debris.…”

Section: Cryoneurolysis Wallerian Degeneration and Nerve Regenerationmentioning

confidence: 99%

Novel cryoneurolysis device for the treatment of sensory and motor peripheral nerves

Ilfeld

Preciado

Trescot

2016

Expert Review of Medical Devices

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Introduction: Cryoneurolysis is the direct application of low temperatures to reversibly ablate peripheral nerves to provide pain relief. Recent development of a handheld cryoneurolysis device with small gauge probes and an integrated skin warmer broadens the clinical applications to include treatment of superficial nerves, further enabling treatments for pre-operative pain, post-surgical pain, chronic pain, and muscle movement disorders. Areas covered: Cryoneurolysis is the direct application of cold temperatures to a peripheral nerve, resulting in reversible ablation due to Wallerian degeneration and nerve regeneration. Use over the last 50 years attests to a very low incidence of complications and adverse effects. Cryoprobes have traditionally been applied through a surgical incision; but, recent technical advances allow percutaneous administration. A new hand-held device is now approved for use within the United States. Cryoneurolysis has been used to treat postoperative and chronic pain states as well as spasticity. Expert commentary: Changes in the US healthcare system such as a push for the reduction of opioid use and the incorporation of Diagnostic Related Group codes, as well as recent technological advances including a handheld unit that allows for treatment of superficial nerves while protecting the skin from damage, may contribute to the resurgence of cryoneurolysis for the treatment of peripheral nerves. ARTICLE HISTORY

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WldS, Nmnats and axon degeneration-progress in the past two decades

Cited by 22 publications

References 73 publications

Overexpression of Wld^s or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish

Overexpression of Wld^s or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish

Axon degeneration in Parkinson's disease

Novel cryoneurolysis device for the treatment of sensory and motor peripheral nerves

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WldS, Nmnats and axon degeneration-progress in the past two decades

Cited by 22 publications

References 73 publications

Overexpression of Wlds or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish

Overexpression of Wlds or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish

Axon degeneration in Parkinson's disease

Novel cryoneurolysis device for the treatment of sensory and motor peripheral nerves

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Product

Resources

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Overexpression of Wld^s or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish

Overexpression of Wld^s or Nmnat2 in mauthner cells by single‐cell electroporation delays axon degeneration in live zebrafish