Summary
The phenomenon termed ‘double myelination’, present in sympathetic nerve of normal adult rats and mice, comprises regions of a myelinated axon which are concentrically ensheathed by additional (outer) myelinating Schwann cells. Evidence has been presented that in some instances the outer Schwann cell fails to make contact with an axon, yet its myelin sheath characteristically remains ultrastructurally intact. The present study has sought to identify and analyse configurations intermediate between single and double myelination, in order to determine the mechanism(s) underlying the formation of double ensheathment. Superior cervical ganglia from normal male mice aged 12–24 months were prepared for electron microscopy by systemic aldehyde perfusion. Regions of interest were extensively serial-sectioned for detailed electron microscopical analysis and reconstruction. The earliest evidence for alteration to the expected intimate ensheathment of axons by myelinating Schwann cells involved invasion of supernumerary Schwann cells and their processes at the node of Ranvier, resulting in displacement of the paranodal pockets from axonal contact. Similar paranodal displacement occurred at heminodes as a result of lateral extension and invasion of processes from the adjacent Schwann cell (i.e. the cell investing the unmyelinated domain of the axon). Subsequently, processes of the invading cell extended progressively into internodal regions, located at all times between the plasma membranes of the axon and displaced Schwann cell. The cytoplasmic pockets at the remaining paranode were then subject to invasion. At various stages of displacement myelin formation commenced within the invading cell, representing the first acquisition of double myelin ensheathment in the development of the configuration. Involvement of haematogenous cells in displacement was not detected. There was also evidence consistent with paranodal displacement by adjacent pre-existing myelinating cells, but this additional mechanism appeared minor relative to the involvement of (initially) non-myelinating Schwann cells. We found no evidence for the alternative possibility that Schwann cells could synthesize a myelin sheath around a pre-existing myelinated axonde novo, independent of any direct axonal contact. These results are consistent with the well-established requirement for axonal contact by Schwann cells engaging in initial myelin formation, in the sense that the myelin sheath of the outer cell was synthesized prior to its displacement, and that a myelin sheath was not formed by the invading cell until it had invested the axon in a 1:1 relationship. In addition, the emergence of several key features of double myelination (infolding and continuing integrity of the outer sheath, sites of presence/absence of basal lamina on the outer cell) further supports the view that double myelination represents a culmination of these developmental stages.
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References
AGUAYO, A. J., EPPS, J., CHARRON, L. & BRAY, G. M. (1976) Multipotentiality of Schwann cells in cross anastomosed and grafted myelinated and unmyelinated nerves: Quantitative microscopy and autoradiography.Brain Research 104, 1–20.
BALLIN, R. H. M. & THOMAS, P. K. (1969) Electron microscope observations on demyelination and remyelination in experimental allergic neuritis. Part 2. Remyelination.Journal of the Neurological Sciences 8, 225–37.
BERTHOLD, C. H. & SKOGLUND, S. (1968) Postnatal development of feline paranodal myelin-sheath segments. II. Electron microscopy.Acta Societatis Medicorum Upsaliensis 73, 127–44.
BONNAUD-TOULZE, E. N. & RAINE, C. S. (1980) Remodelling during remyelination in the peripheral nervous system.Neuropathology and Applied Neurobiology 6, 273–90.
BUNGE, R. P. (1986) The cell of Schwann. InDiseases of the Nervous System. Clinical Neurobiology (edited by ASBURY, A. K., MCKHANN, G. M. & MCDONALD, W. I.), pp. 153–62. Heinemann Medical: London.
DINN, J. J. (1970) Transnodal remyelination.Journal of Pathology 102, 51–3.
ELFVIN, L. G. (1961) The ultrastructure of the nodes of Ranvier in cat sympathetic nerve fibers.Journal of Ultrastructural Research 5, 374–87.
FRIED, K. & HILDEBRAND, C. (1982) Qualitative structural development of the feline inferior alveolar nerve.Journal of Anatomy 134, 517–31.
GRIFFIN, J. W. DRUCKER, N., GOLD, B. G., ROSENFELD, J., BENZAQUEN, M., CHARNAS, L. R., FAHNESTOCK, K. E. & STOCKS, E. A. (1987) Schwann cell proliferation and migration during paranodal demyelination.Journal of Neuroscience 7, 682–99.
HEATH, J. W. (1982) Double myelination of axons in the sympathetic nervous system.Journal of Neurocytology 11, 249–62.
HEATH, J. W. (1983) The sympathetic nervous system: A novel perspective on the control of myelinating Schwann cells. InMolecular Pathology of Nerve and Muscle (edited by KIDMAN, A. D., TOMKINS, J. K., MORRIS, C. A. & COOPER, N. A.). Humana Press: Clifton, NJ.
HILDEBRAND, C., KOCSIS, J. D., BERGLUND, S. & WAXMAN, S. G. (1985) Myelin sheath remodelling in regenerated rat sciatic nerve.Brain Research 358, 163–70.
HILDEBRAND, C., MUSTAFA, G. Y. & WAXMAN, S. G. (1986) Remodelling of internodes in regenerated rat sciatic nerve: Electron microscope observations.Journal of Neurocytology 15, 681–92.
INUZUKA, T., QUARLES, R. H., TRAPP, B. D. & HEATH, J. W. (1987) Analysis of myelin proteins in sympathetic peripheral nerve of adult rats.Developmental Brain Research 38, 191–9.
KIDD, G. J. & HEATH, J. W. (1987) Mechanism of double myelination in the superior cervical ganglion of the mouse.Journal of Anatomy 155, 245 p.
KIDD, G. J. & HEATH, J. W. (1988) Double myelination of axons in the sympathetic nervous system of the mouse. I. Ultrastructural features and distribution.Journal of Neurocytology 17, 245–261.
KIDD, G. J., HEATH, J. W. & DUNKLEY, P. R. (1986) Degeneration of myelinated sympathetic nerve fibers following treatment with guanethidine.Journal of Neurocytology 15, 561–72.
KING, R. H. M., POLLARD, J. D. & THOMAS, P. K. (1975) Aberrant remyelination in chronic relapsing experimental neuritis.Neuropathology and Applied Neurobiology 1, 367–78.
LANDON, D. N. (1981) Structure of normal peripheral myelinated nerve fibres.Advances in Neurology 31, 25–49.
POLLARD, J. D., KING, R. H. M. & THOMAS, P. K. (1975) Recurrent experimental allergic neuritis. An electron microscope study.Journal of the Neurological Sciences 24, 365–83.
RAINE, C. S. (1982) Differences between the nodes of Ranvier of large and small diameter fibers of the P.N.S.Journal of Neurocytology 11, 935–47.
RAINE, C. S. (1984) Morphology of myelin and myelination. InMyelin (edited by MORELL, P.), pp. 1–50. New York: Plenum.
SMITH, R. S., CHAN, H. & SCHAAP, C. J. (1985) Intermittent myelination of small diameter sciatic axons inXenopus laevis.Journal of Neurocytology 14, 269–78.
SPENCER, P. S. (1979) Neuronal regulation of myelinating cell function. InSociety for Neuroscience Symposia Vol. 4: Aspects of Developmental Neurobiology (edited by FERRENDELLI, J. A. & GURVITCH G.), pp. 275–321. Bethesda: Society for Neuroscience.
VIZOSO, A. D. & YOUNG, J. Z. (1948) Internode length and fibre diameter in developing and regenerating nerves.Journal of Anatomy 82, 110–34.
WEBSTER, H. de F. (1975) Development of peripheral myelinated and unmyelinated nerve fibres. InPeripheral Neuropathy (edited by DYCK, P. J., THOMAS, P. K. & LAMBERT, E. H.), Vol. 1, pp. 37–61. Philadelphia: Saunders.
WEINBERG, H. J. & SPENCER, P. S. (1976) Studies on the control of myelinogenesis. II. Evidence for neuronal regulation of myelin production.Brain Research 113, 363–78.
YOKOTA, R. (1984) Occurrence of long non-myelinated axonal segments intercalated in myelinated, presumably sensory axons: electron microscope observations in the dog atrial endocardium.Journal of Neurocytology 13, 127–43.
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Kidd, G.J., Heath, J.W. Double myelination of axons in the sympathetic nervous system of the mouse. II. Mechanisms of formation. J Neurocytol 17, 263–276 (1988). https://doi.org/10.1007/BF01674212
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DOI: https://doi.org/10.1007/BF01674212