Galactocerebrosidase-deficient oligodendrocytes maintain stable central myelin by exogenous replacement of the missing enzyme in mice

Kondo, Yoichi; Wenger, David A.; Gallo, Vittorio; Duncan, Ian D.

doi:10.1073/pnas.0506473102

Cited by 56 publications

(54 citation statements)

References 38 publications

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“…The generalized absence of myelin makes the analysis of transplant-induced myelination straightforward. First there is significantly more myelin than in controls, and the myelin is MBP positive [6,54,55]. Further confirmation that this myelin is not endogenous can be seen on electron microscope (EM), in which the myelin has a major dense line and a thicker sheath than compared to the thin myelin sheaths of the host [55].…”

Section: The Plp Mutantsmentioning

confidence: 81%

“…In the second study, we transplanted OPCs into the brain at P0 to P1 and into the dorsal column of the thoracolumbar spinal cord of the same shi mice In (f), GFP-positive cells are seen at high density in the white matter and also in appropriate numbers in grey matter. These cells have completely myelinated the cord (g) compared to a segment from the cervical cord of the same mouse, which is MBP negative (h) 3 weeks later [6]. At 120 days, the mice were examined and GFP-positive OPCs were found to have extensively migrated throughout the brain, associated with MBPpositive myelin patches, and across the entire spinal cord at the site of injection (Fig.…”

Section: Myelinationmentioning

confidence: 99%

“…Although a number of methods have been used to label cells prior to transplantation, the 2 methods most frequently used are to transduce the cells to express a reporter gene, usually β-galactosidase (lacZ) or GFP [6,55,83]. In the case of lacZ, the spinal cord or brain at the site of transplantation is incubated overnight in X-gal solution [23].…”

Section: Tracking Cells and Their Fate After Transplantationmentioning

confidence: 99%

“…Because of the complexity of the pathophysiology of the disease, it appears likely that a combined therapeutic approach, perhaps including exogenous cell-based remyelination will be necessary. In most lysosomal disorders, the affected cells can function when the missing enzyme is replaced, even exogenously [6,[91][92][93]. Therefore, replacing GALC in oligodendrocytes and Schwann cells, either endogenously or exogenously, is critical as a therapeutic approach in Krabbe disease.…”

Section: Transplantation Of Cells Into the Twi Mousementioning

confidence: 99%

“…The alternative is to supply an exogenous source of OPCs or immature OLs to initiate repair. Cell transplantation and endogenous cell recruitment may not be mutually exclusive, however, as the cells are transplanted, they may supply the missing or defective enzyme or protein to endogenous OPCs or OLs [6].…”

Section: Introductionmentioning

confidence: 99%

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The Myelin Mutants as Models to Study Myelin Repair in the Leukodystrophies

2011

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The leukodystrophies are rare and serious genetic disorders of the central nervous system that primarily affect children who frequently die early in life or have significantly delayed motor and mental milestones that result in long-term disability. Although with some of these disorders, early intervention with bone marrow or cord blood transplantation has been proven useful, it has not yet been determined that such therapies promote myelin repair of the central nervous system. Research on experimental therapies aimed at myelin repair is aided by the ability to test cell replacement strategies in genetic models in which the mutations and neuropathology match the human disorder. Thus, models exist of Pelizaeus-Merzbacher disease and the lysosomal storage disorder, Krabbe disease, which reflect the clinical and pathological course of the human disorders. Collectively, animals with mutations in myelin genes are called the myelin mutants, and they include rodent models such as the shiverer mouse that have been extensively used to study myelination by exogenous cell transplantation. These studies have encompassed many permutations of the age of the recipient, type of transplanted cell, site of engraftment, and so forth, and they offer hope that the scaling up of myelin produced by transplanted cells will have clinical significance in treating patients. Here we review these models and discuss their relative importance and use in such translational approaches. We discuss how grafts are identified and functional outcomes are measured. Finally, we briefly discuss the cells that have been successfully transplanted, which may be used in future clinical trials.

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Section: The Plp Mutantsmentioning

confidence: 81%

Section: Myelinationmentioning

confidence: 99%

Section: Tracking Cells and Their Fate After Transplantationmentioning

confidence: 99%

Section: Transplantation Of Cells Into the Twi Mousementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The Myelin Mutants as Models to Study Myelin Repair in the Leukodystrophies

2011

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Morphology and electrophysiological properties of hamster spinal dorsal horn neurons that express VGLUT2 and enkephalin

Schneider

Walker

2007

J of Comparative Neurology

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The excitatory amino acid glutamate mediates transmission at spinal synapses, including those formed by sensory afferent fibers and by intrinsic interneurons. The identity and physiological properties of glutamatergic dorsal horn neurons are poorly characterized despite their importance in spinal sensory circuits. Moreover, many intrinsic spinal glutamatergic synapses colocalize the opioid peptide enkephalin (ENK), but the neurons to which they belong are yet to be identified. Therefore, we used immunohistochemistry and confocal microscopy to investigate expression of the VGLUT2 vesicular glutamate transporter, an isoform reported in nonprimary afferent spinal synapses, and ENK in electrophysiologically identified neurons of hamster spinal dorsal horn. VGLUT2 immunoreactivity was localized in restricted fashion to axon varicosities of neurons recorded from laminae II-V, although the occurrence of immunolabeling in individual varicosities varied widely between cells (39 +/- 36%, n = 31 neurons). ENK colocalized with VGLUT2 in up to 77% of varicosities (17 +/- 21%, n = 21 neurons). The majority of neurons expressing VGLUT2 and/or ENK had axons with dense local terminations or projections consistent with propriospinal functions. VGLUT2 and ENK labeling were not correlated with cellular morphology, intrinsic membrane properties, firing patterns, or synaptic responses to sensory afferent stimulation. However, VGLUT2 expression was significantly higher in neurons with depolarized resting membrane potential. The results are new evidence for a population of dual-function dorsal horn interneurons that might provide another mechanism for limiting excitation within dorsal horn circuits during periods of strong sensory activation.

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MMP‐3 mediates psychosine‐induced globoid cell formation: Implications for leukodystrophy pathology

Ijichi

Brown

Moore

et al. 2013

Glia

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Globoid cell leukodystrophy (GLD) or Krabbe disease, is a fatal demyelinating disease attributed to mutations in the galactocerebrosidase (GALC) gene. Loss of function mutations in GALC result in accumulation of the glycolipid intermediate, galactosylsphingosine (psychosine). Due to the cytotoxicity of psychosine, it has been hypothesized that accumulated psychosine underlie the pathophysiology of GLD. However, the cellular mechanisms of GLD pathophysiology remain unclear. Globoid cells, multinucleated microglia/macrophages in the central nervous system (CNS), are a defining characteristic of GLD. Here we report that exposure of primary glial cultures to psychosine induces the expression and the production of matrix metalloproteinase (MMP)-3 that mediated a morphological transformation of microglia into a multinucleated globoid cell type. Additionally, psychosine-induced globoid cell formation from microglia was prevented by either genetic ablation or chemical inhibition of MMP-3. These effects are microglia-specific as peripheral macrophages exposed to psychosine did not become activated or express increased levels of MMP-3. In the brain from twitcher mice, a murine model of human GLD, elevated MMP-3 expression relative to wild-type littermates was contemporaneous with disease onset and further increased with disease progression. Further, bone marrow transplantation (BMT), currently the only therapeutically beneficial treatment for GLD, did not mitigate the elevated expression of MMP-3 in twitcher mice. Hence, elevated expression of MMP-3 in GLD may promote microglial responses to psychosine that may represent an important pathophysiological process in this disease and its treatment.

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Galactocerebrosidase-deficient oligodendrocytes maintain stable central myelin by exogenous replacement of the missing enzyme in mice

Cited by 56 publications

References 38 publications

The Myelin Mutants as Models to Study Myelin Repair in the Leukodystrophies

The Myelin Mutants as Models to Study Myelin Repair in the Leukodystrophies

Morphology and electrophysiological properties of hamster spinal dorsal horn neurons that express VGLUT2 and enkephalin

MMP‐3 mediates psychosine‐induced globoid cell formation: Implications for leukodystrophy pathology

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