Pathologic and Phenotypic Alterations in a Mouse Expressing a Connexin47 Missense Mutation That Causes Pelizaeus-Merzbacher–Like Disease in Humans

Tress, Oliver; Maglione, Marta; Zlomuzica, Armin; May, Dennis; Dicke, Nikolai; Degen, Joachim; Dere, Ekrem; Kettenmann, Helmut; Hartmann, Dieter; Willecke, Klaus

doi:10.1371/journal.pgen.1002146

Cited by 65 publications

(59 citation statements)

References 67 publications

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“…Two batches of experimentally naïve mice at ages of P23 (n = 9 Cx47 +/+ ; n = 12 Cx47 +/M282T ; n = 9 Cx47 M282T/M282T ) and 3 months (n = 14 Cx47 +/+ ; n = 18 Cx47 +/M282T ; n = 12 Cx47 M282T/M282T ) were used. The generation and genotyping of Cx47M282T mutant mice has been described previously [32]. Mutant mice were backcrossed with C57BL/6 mice to provide a >96% C57BL/6 genetic background.…”

Section: Methodsmentioning

confidence: 99%

“…We have generated a transgenic mouse model of PMLD that carries the Cx47M282T point mutation, the mouse ortholog of the corresponding human Cx47M283T mutation [32]. Homozygous Cx47M282T mice exhibited hypomyelination during the first weeks after birth accompanied by vacuolation of white matter tracts, astrogliosis and microglia activation.…”

Section: Introductionmentioning

confidence: 99%

“…Three-week-old mice homozygous for the Cx47M282T mutation showed impaired rotarod performance. No significant changes in myelin formation or rotarod performance were observed in 3-month-old Cx47M282T mice [32]. Here, we examined the effects of Cx47M282T expression in the juvenile and adult mouse on anxiety-like behaviour, neuromotor performance and on learning and memory.…”

Section: Introductionmentioning

confidence: 99%

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Changes in Object Recognition and Anxiety-Like Behaviour in Mice Expressing a Cx47 Mutation That Causes Pelizaeus-Merzbacher-Like Disease

Zlomuzica¹,

Tress²,

Binder³

et al. 2012

Dev Neurosci

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Pelizaeus-Merzbacher-like disease is characterized by impaired psychomotor development, ataxia, progressive spasticity and mental retardation. It is induced by mutations in the gap junction gene GJC2 that encodes for the gap junction protein connexin 47. Mice bearing a human Cx47M283T missense mutation have been generated as a transgenic mouse model of Pelizaeus-Merzbacher-like disease. Homozygous expression of the mutant connexin 47 gene in oligodendrocytes resulted in a complex and variable neuropathologic phenotype, which was associated with impairments in motor coordination in juvenile, but not adult mice. In the present study, we have investigated anxiety-like behaviour and spatial working memory in juvenile (P23) and adult (3-month-old) Cx47M282T mutant mice. Adult Cx47M282T mice were also evaluated in terms of neuromotor functions and in the novel object recognition test. Juvenile Cx47M282T mutant mice exhibited an increase in anxiety-like behaviour in the open field test, but no changes in spatial working memory performance. No significant changes in anxiety-like behaviour, spatial working memory or neuromotor functions were observed in the adult Cx47M282T mutant mice. However, novel object recognition was significantly impaired in adult Cx47M282T mice. Our results suggest that the expression of the human Cx47M282T mutation in the mouse causes changes in anxiety-like behaviour in juvenile and novel object recognition impairments in adult mice. It appears that the distortion of panglial gap junction coupling in white and grey matter tissue in the Cx47M282T mice is associated with a complex age-dependent behavioural phenotype including changes in psychomotor, emotional and memory functions.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Changes in Object Recognition and Anxiety-Like Behaviour in Mice Expressing a Cx47 Mutation That Causes Pelizaeus-Merzbacher-Like Disease

Zlomuzica¹,

Tress²,

Binder³

et al. 2012

Dev Neurosci

Self Cite

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“…In the brain of patients suffering from neurodegenerative diseases [138][139][140] and in animal models of these disorders [141][142][143][144], signs of massive neuroinflammation are detected. Importantly, the phenotype of both astrocytes and microglia changes in ageing.…”

Section: Processes Contributing To Brain Ageingmentioning

confidence: 99%

The endocannabinoid system in normal and pathological brain ageing

Bilkei-Gorzó

2012

Phil. Trans. R. Soc. B

116

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The role of endocannabinoids as inhibitory retrograde transmitters is now widely known and intensively studied. However, endocannabinoids also influence neuronal activity by exerting neuroprotective effects and regulating glial responses. This review centres around this less-studied area, focusing on the cellular and molecular mechanisms underlying the protective effect of the cannabinoid system in brain ageing. The progression of ageing is largely determined by the balance between detrimental, proageing, largely stochastic processes, and the activity of the homeostatic defence system. Experimental evidence suggests that the cannabinoid system is part of the latter system. Cannabinoids as regulators of mitochondrial activity, as anti-oxidants and as modulators of clearance processes protect neurons on the molecular level. On the cellular level, the cannabinoid system regulates the expression of brainderived neurotrophic factor and neurogenesis. Neuroinflammatory processes contributing to the progression of normal brain ageing and to the pathogenesis of neurodegenerative diseases are suppressed by cannabinoids, suggesting that they may also influence the ageing process on the system level. In good agreement with the hypothesized beneficial role of cannabinoid system activity against brain ageing, it was shown that animals lacking CB1 receptors show early onset of learning deficits associated with age-related histological and molecular changes. In preclinical models of neurodegenerative disorders, cannabinoids show beneficial effects, but the clinical evidence regarding their efficacy as therapeutic tools is either inconclusive or still missing.

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“…Oligodendrocytes, for example, coexpress Cx47, and at least in rodents, the loss of both Cx32 and Cx47 is far more deleterious than the loss of either one alone (Menichella et al, 2003;Odermatt et al, 2003). However, loss-of-function mutations in GJC2 encoding Cx47 in humans cause PelizeausMerzbacher-like disease (Uhlenberg et al, 2004;Tress et al, 2011). Thus, in humans and not in mice the loss of Cx47 alone produces a severe leukodystrophy.…”

Section: Clinical and Pathological Features Of Cmt1xmentioning

confidence: 99%

The Role of Gap Junctions in Charcot-Marie-Tooth Disease

Kleopa¹

2011

J. Neurosci.

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Pathologic and Phenotypic Alterations in a Mouse Expressing a Connexin47 Missense Mutation That Causes Pelizaeus-Merzbacher–Like Disease in Humans

Cited by 65 publications

References 67 publications

Changes in Object Recognition and Anxiety-Like Behaviour in Mice Expressing a Cx47 Mutation That Causes Pelizaeus-Merzbacher-Like Disease

Changes in Object Recognition and Anxiety-Like Behaviour in Mice Expressing a Cx47 Mutation That Causes Pelizaeus-Merzbacher-Like Disease

The endocannabinoid system in normal and pathological brain ageing

The Role of Gap Junctions in Charcot-Marie-Tooth Disease

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