Evidence that Very Slow Wallerian Degeneration in C57BL/Ola Mice is an Intrinsic Property of the Peripheral Nerve

Perry, V.H.; Brown, Michael C.; Lunn, E. R.; Tree, Peter; Gordon, Siamon

doi:10.1111/j.1460-9568.1990.tb00472.x

Cited by 159 publications

(86 citation statements)

References 18 publications

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“…On returning the nerves to 37°C after 3-4 d at 25°C, the CAP also returned to values not significantly different from those nerves incubated for the same length of time at 37°C (data not shown), similar to the effect seen in wild-type nerves. At 37°C in vitro the nerve survival was prolonged to 9 d, further extending previous data (Perry et al, 1990b;Tsao et al, 1994).…”

Section: The Effect Of Temperature Changes On the Rate Of Axonal Degesupporting

confidence: 75%

“…Using previously described methods (Perry et al, 1990b(Perry et al, , 1992, we analyzed the maximal peak height and peak area of both A and C waves with the Sigavg Program (C ambridge Electronic Design, C ambridge, UK) after digitization (CED 1401) at 80 kHz and found them to be equivalent (Tsao et al, 1994). Selected nerves were fixed in 2% paraformaldehyde, osmicated for 2 hr, infiltrated with glycerol, and then teased apart and examined by light microscopy.…”

Section: Methodsmentioning

confidence: 99%

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Temperature Modulation Reveals Three Distinct Stages of Wallerian Degeneration

1999

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After peripheral nerve transection, axons distal to the cut site rapidly degenerate, a process termed Wallerian degeneration. In wild-type mice the compound action potential (CAP) disappears by 3 d. Previous studies have demonstrated that cold temperatures and lower extracellular calcium ion (Ca 2ϩ ) concentrations can slow the rate of Wallerian degeneration. We have incubated isolated sciatic nerve segments from wild-type and C57BL/Wld mice (which carry a gene slowing Wallerian degeneration) in vitro at 25 and 37°C. At 25°C we found that the degeneration rate of wild-type axons was slowed dramatically, with the CAP preserved up to 7 d post-transection. In contrast, at 37°C the CAPs were minimal at 2 d. When the temperature of wild-type nerves was raised to 37°C after 24-72 hr at 25°C, degeneration occurred within the subsequent 24 hr. Wld nerves, too, were preserved longer at 25°C but, on return to 37°C, degenerated promptly. Cooling the nerve within 12 hr after axotomy enhanced axonal preservation. Neither wild-type nor Wld nerves showed different degeneration rates when they were incubated with 250 M or 5 or 10 mM extracellular Ca 2ϩ for 1-2 d, suggesting that an abrupt increase in intracellular Ca 2ϩ occurs at the time of axonal destruction. Wallerian degeneration, thus, appears to progress through three distinct stages. Initiation occurs at the time of injury with subsequent temperature-dependent and -independent phases. Nerves appear to remain intact and are able to exclude Ca 2ϩ from entering until an as yet unknown process finally increases axolemmal permeability.

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Section: The Effect Of Temperature Changes On the Rate Of Axonal Degesupporting

confidence: 75%

Section: Methodsmentioning

confidence: 99%

Temperature Modulation Reveals Three Distinct Stages of Wallerian Degeneration

1999

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“…The Wld S mouse strain displays a phenotype of slow Wallerian degeneration due to spontaneous mutation on chromosome 4 (Lyon et al, 1993) that is intrinsic to axons (Lunn et al, 1989;Perry et al, 1990) and is identified as an 85-kb tandem triplication (Coleman et al, 1998) that translates into a neuroprotective chimeric fusion protein of ubiquitin assembly factor E4B (Ube4b) and mononucleotide adenylyltransferase (Nmnat) (Conforti et al, 2000). Using the model of Wld S degeneration, we found a positive correlation between TNFα and MMP-9 expression and the macrophage migration capacity of injured nerve.…”

Section: Discussionmentioning

confidence: 99%

TNFα-induced MMP-9 promotes macrophage recruitment into injured peripheral nerve

Shubayev

Angert

Dolkas

et al. 2006

Molecular and Cellular Neuroscience

146

152

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Matrix metalloproteinase-9 (MMP-9) is an extracellular protease that is induced hours after injury to peripheral nerve. This study shows that MMP-9 gene deletion and neutralization with MMP-9 antibody reduce macrophage content in injured wild-type nerves. In mice with delayed Wallerian degeneration (Wld S ), MMP-9 and tumor necrosis factor alpha (TNFα) decline in association with the reduced macrophage recruitment to injured nerve that characterizes this strain of mice. We further determined that TNFα acts as an MMP-9 inducer by establishing increased MMP-9 levels after TNFα injection in rat sciatic nerve in vivo and primary Schwann cells in vitro. We found reduced MMP-9 expression in crushed TNFα knockout nerves that was rescued with exogenous TNFα. Finally, local application of MMP-9 on TNFα−/− nerves increased macrophage recruitment to the lesion. These data suggest that TNFα lies upstream of MMP-9 in the pathway of macrophage recruitment to injured peripheral nerve.

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“…9 -13 Experiments using bone marrow chimaeras have proven that this is a property that affects "cell populations intrinsic to the Wld s nerve and is not attributable to an anomaly in circulating monocytes." 14 We have recently shown that compared with wild-type (WT) mice, Wld s mice, when immunized to induce chronic EAE, developed a delayed onset and an attenuated disease course, 15 which was associated with a reduction in both axonal loss and demyelination in spinal cord sections. Axonal protection in Wld s mice was associated with increased nicotinamide adenine dinucleotide (NAD) levels; however, the molecular mechanisms mediating axon protection in Wld s mice have not been elucidated.…”

mentioning

confidence: 99%

Elevated Neuronal Expression of CD200 Protects Wlds Mice from Inflammation-Mediated Neurodegeneration

Chitnis

Imitola

Wang

et al. 2007

The American Journal of Pathology

131

124

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Axonal damage secondary to inflammation is likely the substrate of chronic disability in multiple sclerosis and is found in the animal model of experimental autoimmune encephalomyelitis (EAE). Wld s mice have a triplication of the fusion gene Ube4b/Nmnat and a phenotype of axon protection. Wld s mice develop an attenuated disease course of EAE, with decreased demyelination, reduced axonal pathology, and decreased central nervous system (CNS) macrophage and microglial accumulation. We show that attenuated disease in Wld s mice was associated with robust constitutive expression of the nonsignaling CD200 molecule on neurons in the CNS compared with control mice. CD200 interacts with its signaling receptor CD200R, which we found to be expressed on microglia, astrocytes, and oligodendrocytes at similar levels in control and Wld s mice. Administration of blocking anti-CD200 antibody to Wld s mice abrogated disease attenuation and was associated with increased CNS inflammation and neurodegeneration. In vitro, Wld s neuronal cultures were protected from microglial-induced neurotoxicity compared with control cultures, but protection was abrogated by anti-CD200 antibody. The CD200-CD200R pathway plays a critical role in attenuating EAE and reducing inflammationmediated damage in the CNS. Strategies that up-regulate the expression of CD200 in the CNS or molecules that ligate the CD200R may be relevant as neuroprotective strategies in multiple sclerosis. (Am J Pathol

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Evidence that Very Slow Wallerian Degeneration in C57BL/Ola Mice is an Intrinsic Property of the Peripheral Nerve

Cited by 159 publications

References 18 publications

Temperature Modulation Reveals Three Distinct Stages of Wallerian Degeneration

Temperature Modulation Reveals Three Distinct Stages of Wallerian Degeneration

TNFα-induced MMP-9 promotes macrophage recruitment into injured peripheral nerve

Elevated Neuronal Expression of CD200 Protects Wlds Mice from Inflammation-Mediated Neurodegeneration

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