Elsevier

Brain Research

Volume 156, Issue 2, 10 November 1978, Pages 213-225
Brain Research

Regeneration of motor axons in the rat sciatic nerve studied by labeling with axonally transported radioactive proteins

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Summary

Labeling regenerating axons with axonally transported radioactive proteins provides information about the location of the entire range of axons from the fastest growing ones to those which are trapped in the scar. We have used this technique to study the regeneration of motor axons in the rat sciatic nerve after a crush lesion. From 2 to 14 days after the crush the lumbar spinal cord was exposed by laminectomy and multiple injections of [3H]proline were made stereotactically in the ventral horn. Twenty-four hours later the nerves were removed and the distribution of radioactivity along the nerve was measured by liquid scintillation counting. There was a peak of radioactivity in the regenerating axons distal to the crush due to an accumulation of label in the tips of these axons. After a delay of3.2 ± 0.2 (S.E.) days, this peak advanced down the nerve at a rate of3.0 ± 0.1 (S.E.) mm/day. The leading edge of this peak, which marks the location of the endings of the most rapidly growing labeled fibers, moved down the nerve at a rate of4.4 ± 0.2 mm/day after a delay of2.1 ± 0.2 days; this is the same time course as that of the most rapidly regenerating sensory axons in the rat sciatic nerve, measured by the pinch test. Another peak of radioactivity at the crush site, presumed to represent the ends of unregenerated axons or misdirected sprouts, declined rapidly during the first week, and more slowly thereafter.

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  • Cited by (0)

    The experiments conducted herein were conducted according to the principles set forth in the ‘Guide for the Care and Use of Laboratory Animals’, Institute of Laboratory Resources, National Research Council, DHEW, Publ. No. (NIH) 74-23.

    *

    Present address: Department of Neurology, Northwestern University School of Medicine, Chicago III. 60611, U.S.A.

    **

    Naval Medical Research and Development Command, Research Work Unit No. MF51.524.013. 1016. The opinions and assertions contained herein are the private ones of the writers and are not to be construed as official or reflecting the views of the Navy Department or the naval service at large.

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