Oligodendrocyte

Oligodendrocyte

Oligodendrocyte

Oligodendrocytes form the electrical insulation around the axons of CNS nerve cells.
Details
Identifiers
Latin oligodendrocytus
Code TH H2.00.06.2.01018

Anatomical terminology

Oligodendrocytes (from Greek, meaning cells with a few branches), or oligodendroglia (Greek, few tree glue),[1] are a type of neuroglia. Their main functions are to provide support and insulation to axons in the central nervous system of some vertebrates, equivalent to the function performed by Schwann cells in the peripheral nervous system. Oligodendrocytes do this by creating the myelin sheath, which is 80% lipid and 20% protein.[2] A single oligodendrocyte can extend its processes to 50 axons, wrapping approximately 1 μm of myelin sheath around each axon; Schwann cells, on the other hand, can wrap around only one axon. Each oligodendrocyte forms one segment of myelin for several adjacent axons.[2]

Origin

Oligodendroglia, types of glial cells, arise during development from oligodendrocyte precursor cells,[3] which can be identified by their expression of a number of antigens, including the ganglioside GD3,[4] the NG2 chondroitin sulfate proteoglycan, and the platelet-derived growth factor-alpha receptor subunit (PDGF-alphaR).[5] Most oligodendrocytes develop during embryogenesis and early postnatal life from restricted periventricular germinal regions.[6]

Oligodendrocytes are found only in the central nervous system which comprises the brain and spinal cord. These cells were originally thought to have been produced in the ventral neural tube; however, research now shows oligodendrocytes originate from the ventral ventricular zone of the embryonic spinal cord and possibly have some concentrations in the forebrain.[7] They are the last cell type to be generated in the CNS.[8]

Myelination is only prevalent in a few brain regions at birth and continues into adulthood. The entire process is not complete until about 25–30 years of age.[9]

The group of Prof. Arturo Alvarez-Buylla[10] demonstrate that oligodendrocyte formation in the adult brain is associated with glial-restricted progenitor cells, known as oligodendrocyte progenitor cells (OPCs).[11] SVZ cells migrate away from germinal[11] zones to populate both developing white and gray matter, where they differentiate and mature into myelin-forming oligodendroglia.[12] However, it is not clear whether all oligodendroglial progenitors undergo this sequence of events. It has been suggested that some undergo apoptosis [13] and others fail to differentiate into mature oligodendroglia but persist as adult oligodendroglial progenitors.[14] Remarkably, oligodendrocyte population originated in the subventricular zona can be dramatically expanded by administering epidermal growth factor (EGF).[15][16]

Function

An oligodendrocyte seen myelinating several axons.

As part of the nervous system, oligodendrocytes are closely related to nerve cells, and, like all other glial cells, oligodendrocytes provide a supporting role for neurons as well as trophic support by the production of glial cell line-derived neurotrophic factor (GDNF), brain-derived neurotrophic factor (BDNF), or insulin-like growth factor-1 (IGF-1).[17] In addition, the nervous system of mammals depends crucially on myelin sheaths, which reduce ion leakage and decrease the capacitance of the cell membrane.[18] Myelin also increases impulse speed, as saltatory propagation of action potentials occurs at the nodes of Ranvier in between Schwann cells (of the PNS) and oligodendrocytes (of the CNS). Furthermore, impulse speed of myelinated axons increases linearly with the axon diameter, whereas the impulse speed of unmyelinated cells increases only with the square root of the diameter. The insulation must be proportional to the diameter of the fiber inside. The optimal ratio of axon diameter divided by the total fiber diameter (which includes the myelin) is 0.6.[9]

In contrast, satellite oligodendrocytes are functionally distinct from other oligodendrocytes. They are not attached to neurons and, therefore, do not serve an insulating role. They remain apposed to neurons and regulate the extracellular fluid.[19] Satellite oligodendrocytes are considered to be a part of the gray matter whereas myelinating oligodendrocytes are a part of the white matter.

Myelination is an important component of intelligence. Neuroscientist Vincent J. Schmithorst suggests that there is a correlation with white matter and intelligence. People with greater white matter had higher IQ's.[9] A study done with rats by Janice M. Juraska showed that rats that were raised in an enriched environment had more myelination in their corpus callosum.[20]

Oligodendrocytes in rat cerebellum stained with antibody to myelin basic protein in red and for DNA in blue. Two oligodendrocyte cell bodies are clearly visible as well as several myelinated axons. These are hollow tubes and so appear as "tramlines" in this confocal image. Most of the DNA is in the nuclei of cerebellum granule cells, which are small interneurons. Image and antibody stain from EnCor Biotechnology Inc.

Pathology

Diseases that result in injury to the oligodendroglial cells include demyelinating diseases such as multiple sclerosis and various leukodystrophies. Trauma to the body, e.g. spinal cord injury, can also cause demyelination. Cerebral palsy, (sometimes developing from periventricular leukomalacia), is largely congenital and caused by damage to the newly forming brain. In cerebral palsy, spinal cord injury, stroke and possibly multiple sclerosis, oligodendrocytes are thought to be damaged by excessive release of the neurotransmitter, glutamate.[21] Damage has also been shown to be mediated by N-methyl-D-aspartate receptors.[21] Oligodendrocyte dysfunction may also be implicated in the pathophysiology of schizophrenia and bipolar disorder.[22]

Oligodendroglia are also susceptible to infection by the JC virus, which causes progressive multifocal leukoencephalopathy (PML), a condition that specifically affects white matter, typically in immunocompromised patients. Tumors of oligodendroglia are called oligodendrogliomas. The chemotherapy agent Fluorouracil (5-FU) causes damage to the oligodendrocytes in mice, leading to both acute central nervous system (CNS) damage and progressively worsening delayed degeneration of the CNS.[23] [24]

See also

Notes

  1. (Ragheb 1999, p. 14).
  2. 1 2 Carlson, Physiology of Behavior, 2010
  3. Cameron-Curry, Patrizia; Le Douarin, Nicole M. (December 1995). "Oligodendrocyte precursors originate from both the dorsal and the ventral parts of the spinal cord". Neuron 15 (6): 1299–1310. doi:10.1016/0896-6273(95)90009-8. PMID 8845154.
  4. Curtis et al., 1988; LeVine and Goldman, 1988; Hardy and Reynolds, 1991
  5. Pringle, NP; Mudhar, HS; Collarini, EJ; Richardson, WD (Jun 1992). "PDGF receptors in the rat CNS: during late neurogenesis, PDGF alpha-receptor expression appears to be restricted to glial cells of the oligodendrocyte lineage." (PDF). Development (Cambridge, England) 115 (2): 535–51. PMID 1425339.
  6. Vallstedt et al., 2004
  7. Richardson, WD; Kessaris, N; Pringle, N (Jan 2006). "Oligodendrocyte wars.". Nature reviews. Neuroscience 7 (1): 11–8. doi:10.1038/nrn1826. PMID 16371946.
  8. Thomas, JL; Spassky, N; Perez Villegas, EM; Olivier, C; Cobos, I; Goujet-Zalc, C; Martínez, S; Zalc, B (Feb 15, 2000). "Spatiotemporal development of oligodendrocytes in the embryonic brain". Journal of neuroscience research 59 (4): 471–6. doi:10.1002/(SICI)1097-4547(20000215)59:4<471::AID-JNR1>3.0.CO;2-3. PMID 10679785.
  9. 1 2 3 Fields, 2008
  10. Gonzalez-Perez, O; Alvarez-Buylla, A (2011). "Oligodendrogenesis in the subventricular zone and the role of epidermal growth factor". Brain Research Reviews 67 (1–2): 147–56. doi:10.1016/j.brainresrev.2011.01.001. PMC 3109119. PMID 21236296.
  11. 1 2 Menn, B; Garcia-Verdugo, JM; Yaschine, C; Gonzalez-Perez, O; Rowitch, D; Alvarez-Buylla, A (Jul 26, 2006). "Origin of oligodendrocytes in the subventricular zone of the adult brain.". The Journal of neuroscience : the official journal of the Society for Neuroscience 26 (30): 7907–18. doi:10.1523/JNEUROSCI.1299-06.2006. PMID 16870736.
  12. Hardy and Reynolds, 1991; Levison and Goldman, 1993
  13. Barres et al., 1992
  14. Wren et al., 1992
  15. Gonzalez-Perez, O, B; Romero-Rodriguez, R,; Soriano-Navarro, M; Garcia-Verdugo, JM; Alvarez-Buylla, A (2009). "Epidermal growth factor induces the progeny of subventricular zone type B cells to migrate and differentiate into oligodendrocytes". Stem Cells 27 (8): 2032–43. doi:10.1002/stem.119. PMC 3346259. PMID 19544429.
  16. Gonzalez-Perez, O, B; Alvarez-Buylla, A (Jun 24, 2011). "Oligodendrogenesis in the subventricular zone and the role of epidermal growth factor". Brain Research Reviews 67 (1–2): 147–56. doi:10.1016/j.brainresrev.2011.01.001. PMC 3109119. PMID 21236296.
  17. Bradl (2010). "Oligodendrocytes: biology and pathology". Acta Neuropathol. 119: 37–53. doi:10.1007/s00401-009-0601-5. PMC 2799635. PMID 19847447. ...oligodendrocytes can provide trophic support for neurons by the production of glial cell line-derived neurotrophic factor (GDNF), brain-derived neurotrophic factor (BDNF), or insulin-like growth factor-1 (IGF-1).
  18. Sokol, 2009
  19. Baumann and Pham-Dinh, 2001
  20. Juraska J. M., Kopcik J. R.; Kopcik (1988). "Sex and environmental influences on the size and ultrastructure of the rat corpus callosum". Brain Research 450 (1–2): 1–8. doi:10.1016/0006-8993(88)91538-7. PMID 3401704.
  21. 1 2 Káradóttir et al., 2007
  22. Tkachev et al., 2003
  23. "Chemotherapy-induced Damage to the CNS as a Precursor Cell Disease" by Dr. Mark D. Noble, University of Rochester
  24. Han, R; Yang, Y. M.; Dietrich, J; Luebke, A; Mayer-Pröschel, M; Noble, M (2008). "Systemic 5-fluorouracil treatment causes a syndrome of delayed myelin destruction in the central nervous system". Journal of Biology 7 (4): 12. doi:10.1186/jbiol69. PMC 2397490. PMID 18430259.

References

  • Raine, C.S. (1991). Oligodendrocytes and central nervous system myelin. In Textbook of Neuropathology, second edition, R.L. Davis and D.M. Robertson, eds. (Baltimore, Maryland: Williams and Wilkins), pp. 115–141.
  • Tkachev D, Mimmack ML, Ryan MM; et al. (September 2003). "Oligodendrocyte dysfunction in schizophrenia and bipolar disorder". Lancet 362 (9386): 798–805. doi:10.1016/S0140-6736(03)14289-4. PMID 13678875. 
  • Carlson, Neil (2010). Physiology of Behavior. Boston, MA: Allyn & Bacon. pp. 38–39. ISBN 0-205-66627-2. 
  • Vallstedt, A; Klos JM, Ericson F (6 January 2005). "Multiple dorsoventral origins of oligodendrocyte generation in the spinal cord and hindbrain". Neuron. 1 45 (1): 55–67. doi:10.1016/j.neuron.2004.12.026. PMID 15629702. 
  • Richardson, W; D., Kessaris, Pringle, N (2006). "Oligodendrocyte wars". Nature Neuroscience Reviews. 1 7 (1): 11–18. doi:10.1038/nrn1826. PMID 16371946. 

External links

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