Peripheral Demyelination and Neuropathic Pain Behavior in Periaxin-Deficient Mice

Gillespie, C S; Sherman, Diane L.; Fleetwood-Walker, Susan M.; Cottrell, David F.; Tait, Steven; Garry, Emer M.; Wallace, Victoria C.J.; Ure, Jan; Griffiths, I. R.; Smith, Austin; Brophy, Peter

doi:10.1016/s0896-6273(00)81184-8

Cited by 194 publications

(169 citation statements)

References 48 publications

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“…In particular, the myelin degradation of A␤ afferents promotes susceptibility of their axonal plasma membrane to pronociceptive stimuli, leading to ectopic depolarization and mechanical allodynia (Kobayashi et al, 2008). Accordingly, neuropathic pain behaviors occurred after experimental demyelination of peripheral or central neurons (Wallace et al, 2003;Inoue et al, 2004;Moalem-Taylor et al, 2007;Zhu et al, 2012) and in mutant mice with aberrant myelination or loss of myelin (Gillespie et al, 2000;Chen et al, 2006). Moreover, neuropathic pain accompanies many demyelinating human diseases, such as Guillain-Barré syndrome, CharcotMarie-Tooth type I disease, and multiple sclerosis (Ueda, 2008).…”

Section: Discussionmentioning

confidence: 99%

NADPH Oxidase-4 Maintains Neuropathic Pain after Peripheral Nerve Injury

Kallenborn-Gerhardt¹,

Schröder²,

Turco³

et al. 2012

Journal of Neuroscience

102

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Reactive oxygen species (ROS) contribute to sensitization of pain pathways during neuropathic pain, but little is known about the primary sources of ROS production and how ROS mediate pain sensitization. Here, we show that the NADPH oxidase isoform Nox4, a major ROS source in somatic cells, is expressed in a subset of nonpeptidergic nociceptors and myelinated dorsal root ganglia neurons. Mice lacking Nox4 demonstrated a substantially reduced late-phase neuropathic pain behavior after peripheral nerve injury. The loss of Nox4 markedly attenuated injury-induced ROS production and dysmyelination processes of peripheral nerves. Moreover, persisting neuropathic pain behavior was inhibited after tamoxifen-induced deletion of Nox4 in adult transgenic mice. Our results suggest that Nox4 essentially contributes to nociceptive processing in neuropathic pain states. Accordingly, inhibition of Nox4 may provide a novel therapeutic modality for the treatment of neuropathic pain.

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Section: Discussionmentioning

confidence: 99%

NADPH Oxidase-4 Maintains Neuropathic Pain after Peripheral Nerve Injury

Kallenborn-Gerhardt¹,

Schröder²,

Turco³

et al. 2012

Journal of Neuroscience

102

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“…L-periaxin is expressed on the abaxonal surface of myelinated Schwann cells and forms a complex with dystrophin-related protein 2 linking the basal lamina outside the cell to the cytoskeleton within the cell (Scherer et al 1995;Sherman and Brophy 2000;Sherman et al 2001). From experiments with knockout mice, L-periaxin is known to play a significant role in the maintenance and repair of peripheral nerve myelin (Gillespie et al 2000;Williams and Brophy 2002). However, expression of L-periaxin in Schwann cells moves from the nucleus to the adaxonal or periaxonal cytoplasm, then to the abaxonal membrane of myelinating Schwann cells with the maturation of myelin.…”

Section: Discussionmentioning

confidence: 99%

Periaxin mutation causes early-onset but slow-progressive Charcot-Marie-Tooth disease

et al. 2004

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Periaxin (PRX) plays a significant role in the myelination of the peripheral nerve. To date, seven nonsense or frameshift PRX mutations have been reported in six pedigrees with Dejerine-Sottas neuropathy or severe Charcot-Marie-Tooth neuropathy (CMT). We detected a PRX mutation in three patients in the screening of 66 Japanese demyelinating CMT patients who were negative for the gene mutation causing dominant or X-linked demyelinating CMT. Three unrelated patients were homozygous for a novel R1070X mutation and presented early-onset but slowly progressive distal motor and sensory neuropathies. Mutations lacking the carboxyl-terminal acidic domain may show loss-offunction effects and cause severe demyelinating CMT.

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“…During PNS development, L-periaxin-deficient mice show focal thickenings, infoldings of internodal myelin, and late-onset demyelination, which is similar to DGnull mice (Gillespie et al, 2000). L-periaxin is required for the formation of the DG-dystrophin-related protein-2 (DG-DRP2) complex and is involved in the link between the ECM and the Schwann cell cytoskeleton (Sherman et al, 2001).…”

Section: Laminin Signaling In Schwann Cell Morphogenesismentioning

confidence: 97%

Regulation of Schwann cell function by the extracellular matrix

Chernousov

Chen

et al. 2008

Glia

172

138

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Laminins and collagens are extracellular matrix proteins that play essential roles in peripheral nervous system development. Laminin signals regulate Schwann cell proliferation and survival as well as actin cytoskeleton dynamics, which are essential steps for radial sorting and myelination of peripheral axons by Schwann cells. Collagen and their receptors promote Schwann cell adhesion, spreading, and myelination as well as neurite outgrowth. In this article, we will review the recent advances in the studies of laminin and collagen function in Schwann cell development. V V C

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Peripheral Demyelination and Neuropathic Pain Behavior in Periaxin-Deficient Mice

Cited by 194 publications

References 48 publications

NADPH Oxidase-4 Maintains Neuropathic Pain after Peripheral Nerve Injury

NADPH Oxidase-4 Maintains Neuropathic Pain after Peripheral Nerve Injury

Periaxin mutation causes early-onset but slow-progressive Charcot-Marie-Tooth disease

Regulation of Schwann cell function by the extracellular matrix

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