Mitochondrial immobilization mediated by syntaphilin facilitates survival of demyelinated axons

Ohno, Nobuhiko; Hao, Cui; Mahad, Don J.; Kidd, Grahame J.; Liu, Liping; Ransohoff, Richard M.; Sheng, Zu Hang; Komuro, Hitoshi; Trapp, Bruce D.

doi:10.1073/pnas.1401155111

Cited by 98 publications

(107 citation statements)

References 49 publications

(84 reference statements)

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“…Mitochondria undergo continuous fission and fusion cycles 26 , are mobile and trafficked along the neurite processes 21 . Defects in mitochondrial trafficking and dynamics which are not purely numerical or structural can be easily missed by this approach, although, by looking at the number of mitochondria in an anatomically defined space such as presynapse one can interpret if the transport of mitochondria may be altered 39 . A second disadvantage is that it is performed only in a small portion of the brain, therefore circuitry specific defects in mitochondrial distribution may be missed.…”

Section: Discussionmentioning

confidence: 99%

“…Earlier SBFSEM analysis was greatly hindered due to lower resolution, however newer sample preparation techniques involving enhanced staining methods 40 have considerably improved the resolution to an extent that even a single synaptic vesicle can be easily resolved. At this resolution ultrastructural defects in mitochondria such as vacuolation, membrane disruption, and loss of cristae can be easily observed, and the distribution of defective mitochondria within cells can be determined 38,39 . The high resolution of this technique provides a major advantage over light microscopy where the resolution is limited to ~200 nm in XY axis and ~500 nm in Z-axis.…”

Section: Discussionmentioning

confidence: 99%

“…Multiple studies since then have established this technique as a major tool in reconstruction analysis of neuronal circuitry 34 . Furthermore, for many smaller scale projects, it provides reconstruction analysis to identify cellular organelles 27,[35][36][37][38][39] . Since, the acquired images are derived from low voltage back scatter electrons, new staining protocols which combine different known heavy metal staining techniques were developed to increase the resolution 40 .…”

mentioning

confidence: 99%

“…In this paper, we provide a protocol for utilizing 3D electron microscopy imaging and volumetric analysis of brain mitochondria based on methods that have previously been used by us and others 38,39,41 . The tissue post-processing methods used were as previously described by Deerinck et al 40 .…”

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confidence: 99%

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Analysis of Brain Mitochondria Using Serial Block-Face Scanning Electron Microscopy

Mukherjee

Clark

Chavan

et al. 2016

JoVE

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Human brain is a high energy consuming organ that mainly relies on glucose as a fuel source. Glucose is catabolized by brain mitochondria via glycolysis, tri-carboxylic acid (TCA) cycle and oxidative phosphorylation (OXPHOS) pathways to produce cellular energy in the form of adenosine triphosphate (ATP). Impairment of mitochondrial ATP production causes mitochondrial disorders, which present clinically with prominent neurological and myopathic symptoms. Mitochondrial defects are also present in neurodevelopmental disorders (e.g. autism spectrum disorder) and neurodegenerative disorders (e.g. amyotrophic lateral sclerosis, Alzheimer's and Parkinson's diseases). Thus, there is an increased interest in the field for performing 3D analysis of mitochondrial morphology, structure and distribution under both healthy and disease states. The brain mitochondrial morphology is extremely diverse, with some mitochondria especially those in the synaptic region being in the range of <200 nm diameter, which is below the resolution limit of traditional light microscopy. Expressing a mitochondrially-targeted green fluorescent protein (GFP) in the brain significantly enhances the organellar detection by confocal microscopy. However, it does not overcome the constraints on the sensitivity of detection of relatively small sized mitochondria without oversaturating the images of large sized mitochondria. While serial transmission electron microscopy has been successfully used to characterize mitochondria at the neuronal synapse, this technique is extremely time-consuming especially when comparing multiple samples. The serial block-face scanning electron microscopy (SBFSEM) technique involves an automated process of sectioning, imaging blocks of tissue and data acquisition. Here, we provide a protocol to perform SBFSEM of a defined region from rodent brain to rapidly reconstruct and visualize mitochondrial morphology. This technique could also be used to provide accurate information on mitochondrial number, volume, size and distribution in a defined brain region. Since the obtained image resolution is high (typically under 10 nm) any gross mitochondrial morphological defects may also be detected. Video LinkThe video component of this article can be found at

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Analysis of Brain Mitochondria Using Serial Block-Face Scanning Electron Microscopy

Mukherjee

Clark

Chavan

et al. 2016

JoVE

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“…Using knockout mice, Ohno et al recently identifi ed that syntaphilin is necessary to increase mitochondrial content in demyelinated axons in vivo and that its absence leads to an increase in axonal beading and degeneration [ 91 ].…”

Section: G93amentioning

confidence: 99%

Mitochondrial Function and Dynamics Imaged In Vivo

Chisholm

Peters

Schiza

et al. 2016

Mitochondrial Dysfunction in Neurodegenerative Disorders

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The previous chapters have described the extraordinary depth of knowledge of mitochondrial biology revealed by in vitro observations where the environment can be closely controlled. However, in recent years there has been increased interest in the study of mitochondria in vivo, where their properties can be studied with high spatial and temporal resolution while ensuring that key factors such as the oxygen and glucose concentrations are physiologically accurate. Advances facilitating such in vivo research include improved microscope systems and mitochondrially targeted dyes, as well as a wide range of transgenic animals expressing fl uorescent proteins. Such in vivo observations provide a more realistic picture of mitochondrial involvement in health and disease and also offer the potential to reveal novel targets for therapeutic interventions. For example, loss of mitochondrial membrane potential and alterations in mitochondrial morphology and traffi cking have been reported in mouse models of multiple sclerosis and Alzheimer's disease, and redox potential changes have been reported during (patho)physiological changes in oxygen supply and demand.In this chapter we summarise some techniques used in imaging of mitochondria in vivo, followed by a summary of key fi ndings and recent advances in the study of mitochondrial function and dynamics. We aim to provide insight into the benefi ts and limitations of intravital imaging of mitochondria in the nervous system.

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Mitochondrial dysfunction and axon degeneration in progressive multiple sclerosis

Campbell

Mahad

2018

FEBS Letters

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The neuron is the target of inflammatory demyelinating processes in multiple sclerosis (MS). In progressive MS, however, there is a gathering body of evidence indicating that molecular changes converge on mitochondria within neuronal cell bodies. The most reproducible change relates to mitochondrial respiratory chain complex deficiency, which compromises the capacity of neurons to generate ATP. The resulting energy failure state is coupled with an increase in demand for energy by the demyelinated axon, being particularly relevant to the long tracts such as corticospinal tracts with long projection axons. Recent work in our laboratory and that of our collaborators indicates the limited reflection of the mitochondria changes within neurons in experimental disease models. The mitochondrial changes within neuronal compartments are likely to offer novel targets for the improvement in neuronal function in patients with progressive MS.

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Mitochondrial immobilization mediated by syntaphilin facilitates survival of demyelinated axons

Cited by 98 publications

References 49 publications

Analysis of Brain Mitochondria Using Serial Block-Face Scanning Electron Microscopy

Analysis of Brain Mitochondria Using Serial Block-Face Scanning Electron Microscopy

Mitochondrial Function and Dynamics Imaged In Vivo

Mitochondrial dysfunction and axon degeneration in progressive multiple sclerosis

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