Results for 'oligodendrocyte'

16 found
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  1.  13
    Myelin Oligodendrocyte Glycoprotein Antibody Associated Cerebral Cortical Encephalitis: Case Reports and Review of Literature.Hang Shu, Manqiu Ding, Pei Shang, Jia Song, Yue Lang & Li Cui - 2022 - Frontiers in Human Neuroscience 15.
    Myelin oligodendrocyte glycoprotein antibody-associated disease is an immune-mediated demyelinating disease of the central nervous system that is present in both adults and children. The most common clinical manifestations are optic neuritis, myelitis, acute disseminated encephalomyelitis, and brainstem syndrome. Cerebral cortical encephalitis is a rare clinical phenotype of myelin oligodendrocyte glycoprotein antibody-associated disease, which usually begins with seizures, headaches, and fever, and may be misdiagnosed as viral encephalitis in the early stages. Herein, we report two typical MOG antibody -positive (...)
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  2.  5
    NMDA receptors expressed in oligodendrocytes.Richard Wong - 2006 - Bioessays 28 (5):460-464.
    Oligodendrocytes are known to express Ca2+-permeable glutamate receptors and to have low resistance to oxidative stress, two factors that make them potentially susceptible to injury. Oligodendrocyte injury is intrinsic to the loss of function experienced in conditions ranging from cerebral palsy to spinal cord injury, focal ischaemia and multiple sclerosis. NMDA receptors, a subtype of glutamate receptors, are vital to the remodeling of synaptic connections during postnatal development and associative learning abilities in adults and possibly in improvements in (...) function. Previous studies had failed to detect NMDA receptor mRNA or current in oligodendrocytes but three new papers1-3 demonstrate NMDA receptor expression in oligodendrocytes and discuss its implications for ischaemia therapy. BioEssays 28: 460–464, 2006. © 2006 Wiley Periodicals, Inc. (shrink)
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  3.  7
    The emerging functions of oligodendrocytes in regulating neuronal network behaviour.Livia de Hoz & Mikael Simons - 2015 - Bioessays 37 (1):60-69.
    Myelin is required for efficient nerve conduction, but not all axons are myelinated to the same extent. Here we review recent studies that have revealed distinct myelination patterns of different axonal paths, suggesting that myelination is not an all or none phenomenon and that its presence is finely regulated in central nervous system networks. Whereas powerful reductionist biology has led to important knowledge of how oligodendrocytes function by themselves, little is known about their role in neuronal networks. We still do (...)
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  4.  7
    A cell-intrinsic timer that operates during oligodendrocyte development.Béatrice Durand & Martin Raff - 2000 - Bioessays 22 (1):64.
    Multicellular organisms develop on a predictable schedule that depends on both cell‐intrinsic timers and sequential cell‐cell interactions mediated by extracellular signals. The interplay between intracellular timers and extracellular signals is well illustrated by the development of oligodendrocytes, the cells that make the myelin in the vertebrate central nervous system. An intrinsic timing mechanism operates in each oligodendrocyte precursor cell to limit the length of time the cell divides before terminally differentiating. This mechanism consists of two components, a timing component, (...)
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  5.  14
    What have tissue culture studies told us about the development of oligodendrocytes?Brenda P. Williams & Jack Price - 1992 - Bioessays 14 (10):693-698.
    One major success of studying neural cell development in tissue culture has been the discovery of the O‐2A cell. This bipotential cell generates oligodendrocytes or, under certain conditions, a type of astrocyte. This essay considers the evidence that the characteristic properties demonstrated by the O‐2A cells in vitro are an accurate reflection of oligodendrocyte development in vivo.
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  6. A cell-intrinsic timer that operates during oligodendrocyte development.Be Atrice Durand & Martin Raff - unknown - Bioessays 22:65.
     
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  7.  7
    A cell‐intrinsic timer that operates during oligodendrocyte development.Béatrice Durand & Martin Raff - 2000 - Bioessays 22 (1):64-71.
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  8.  18
    Leber’s hereditary optic neuropathy companied with multiple-related diseases.Ming-Ming Sun, Huan-fen Zhou, Qiao Sun, Hong-en Li, Hong-Juan Liu, Hong-lu Song, Mo Yang, Shi-hui da TengWei & Quan-Gang Xu - 2022 - Frontiers in Human Neuroscience 16:964550.
    ObjectiveTo elucidate the clinical, radiologic characteristics of Leber’s hereditary optic neuropathy (LHON) associated with the other diseases.Materials and methodsClinical data were retrospectively collected from hospitalized patients with LHON associated with the other diseases at the Neuro-Ophthalmology Department at the Chinese People’s Liberation Army General Hospital (PLAGH) from December 2014 to October 2018.ResultsA total of 13 patients, 24 eyes (10 men and 3 women; mean age, 30.69 ± 12.76 years) with LHON mitochondrial DNA (mtDNA) mutations, were included in the cohort. 14502(5)11778(4)11778 (...)
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  9.  20
    Myelin mutants: Model systems for the study of normal and abnormal myelination.Ian R. Griffiths - 1996 - Bioessays 18 (10):789-797.
    Spontaneous mutations that perturb myelination occur in a range of species including man, and together with engineered mutations have been used to study disease, normal myelination and axon/glial inter‐relationships. Only a minority of the currently defined mutations have an apparently simple pathogenesis due to lack of a functional protein. Mutations in the myelin basic protein gene lead to a lack of protein, resulting in changes in the structure of myelin, which can be rescued by transgenic complementation. The pathogenesis of autosomal (...)
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  10.  22
    Contact inhibition in the failure of mammalian CNS axonal regeneration.Alan R. Johnson - 1993 - Bioessays 15 (12):807-813.
    Anamniote animals, such as fish and amphibians, are able to regenerate damaged CNS nerves following injury, but regeneration in the mammalian CNS tracts, such as the optic nerve, does not occur. However, severed adult mammalian retinal axons can regenerate into peripheral nerve segments grafted into the brain and this finding has emphasized the importance of the environment in explaining regenerative failure in the adult mammalian CNS. Following lesions, regenerating axons encounter the glial cells, oligodendrocytes and astro‐cytes, and their derivatives, respectively (...)
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  11.  32
    An unstructured protein with destructive potential: TPPP/p25 in neurodegeneration.Judit Ovádi & Ferenc Orosz - 2009 - Bioessays 31 (6):676-686.
    TPPP/p25 is a recently discovered, unstructured protein involved in brain function. It is found predominantly in oligodendrocytes in normal brain but is enriched in neuronal and glial inclusions of Parkinson's disease and other synucleinopathies. Its physiological function seems to be the dynamic stabilization of microtubular ultrastructures, as well as the projections of mature oligodendrocytes and ciliary structures. We reappraise the earlier belief that TPPP/p25 is a brain‐specific protein. We have identified and cloned two shorter (N‐terminal‐free) homologs of TPPP/p25 that behave (...)
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  12.  13
    The cellular and molecular events of central nervous system remyelination.Monique Dubois-Dalcq & Regina Armstrong - 1990 - Bioessays 12 (12):569-576.
    Central nervous system (CNS)Abbreviations: CNS=central nervous system; PNS=peripheral nervous system; MS=multiple sclerosis; MBP=myelin basic protein; MHC=major histocompatibility complex; EAE=experimental allergic encephalomyelitis; O‐2A=oligodendrocyte‐type 2 astrocyte; GC=galactocerebroside; GFAP=glial fibrillary acidic protein; FGF=fibroblast growth factor; IGF1=insulin‐like growth factor. regeneration is a subject of great interest, particularly in diseases causing a dramatic loss of neurons. However, some CNS diseases do not affect neurons but damage other cells, such as the myelin‐forming cells — called oligodendrocytes — which are also crucial to the harmonious function (...)
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  13.  5
    Precursor cell types in the germinal zone of the cerebral cortex.Brenda P. Williams - 1995 - Bioessays 17 (5):391-393.
    Retroviral lineage tracing experiments suggest that the cortical ventricular zone is composed of a mixture of precursor cell types. The majority generate a single cell type (neurones, astrocytes or oligodendrocytes) and the remainder generate neurones and a single type of glial cell. Pluripotential precursor cells, that have the ability to generate all three cell types, are not observed. A recent paper, however, reports that when single ventricular zone cells are cultured in isolation, a small percentage of these cells are pluripotential(1). (...)
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  14.  8
    Interactions between neural cells and blood vessels in central nervous system development.Keiko Morimoto, Hidenori Tabata, Rikuo Takahashi & Kazunori Nakajima - 2024 - Bioessays 46 (3):2300091.
    The sophisticated function of the central nervous system (CNS) is largely supported by proper interactions between neural cells and blood vessels. Accumulating evidence has demonstrated that neurons and glial cells support the formation of blood vessels, which in turn, act as migratory scaffolds for these cell types. Neural progenitors are also involved in the regulation of blood vessel formation. This mutual interaction between neural cells and blood vessels is elegantly controlled by several chemokines, growth factors, extracellular matrix, and adhesion molecules (...)
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  15.  11
    MYRF: A unique transmembrane transcription factor‐ from proteolytic self‐processing to its multifaceted roles in animal development.Yingchuan B. Qi, Zhimin Xu, Shiqian Shen, Zhao Wang & Zhizhi Wang - 2024 - Bioessays 46 (4):2300209.
    The Myelin Regulator Factor (MYRF) is a master regulator governing myelin formation and maintenance in the central nervous system. The conservation of MYRF across metazoans and its broad tissue expression suggest it has functions extending beyond the well‐established role in myelination. Loss of MYRF results in developmental lethality in both invertebrates and vertebrates, and MYRF haploinsufficiency in humans causes MYRF‐related Cardiac Urogenital Syndrome, underscoring its importance in animal development; however, these mechanisms are largely unexplored. MYRF, an unconventional transcription factor, begins (...)
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  16.  18
    Function and Mechanism of Myelin Regulation in Alcohol Abuse and Alcoholism.James Rice & Chen Gu - 2019 - Bioessays 41 (7):1800255.
    Excessive alcohol use has adverse effects on the central nervous system (CNS) and can lead to alcohol use disorders (AUDs). Recent studies have suggested that myelin reductions may directly contribute to CNS dysfunctions associated with AUDs. Myelin consists of compact lipid membranes wrapped around axons to provide electrical insulation and trophic support. Regulation of myelin is considered as a new form of neural plasticity due to its profound impacts on the computation of neural networks. In this review, the authors first (...)
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