To investigate the role of the neurofilament heavy (NF-H) subunit in neuronal function, we generated mice bearing a targeted disruption of the gene coding for the NF-H subunit. Surprisingly, the lack of NF-H subunits had little effect on axonal calibers and electron microscopy revealed no significant changes in the number and packing density of neurofilaments made up of only the neurofilament light (NF-L) and neurofilament medium (NF-M) subunits. However, our analysis of NF-H knockout mice revealed an ∼2.4-fold increase of microtubule density in their large ventral root axons. This finding was further corroborated by a corresponding increase in the ratio of assembled tubulin to NF-L protein in insoluble cytoskeletal preparations from the sciatic nerve. Axonal transport studies carried out by the injection of [35S]methionine into spinal cord revealed an increased transport velocity of newly synthesized NF-L and NF-M proteins in motor axons of NF-H knockout mice. When treated with β,β′-iminodipropionitrile (IDPN), a neurotoxin that segregates microtubules and retards neurofilament transport, mice heterozygous or homozygous for the NF-H null mutation did not develop neurofilamentous swellings in motor neurons, unlike normal mouse littermates. These results indicate that the NF-H subunit is a key mediator of IDPN-induced axonopathy.
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5 October 1998
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October 05 1998
Disruption of the NF-H Gene Increases Axonal Microtubule Content and Velocity of Neurofilament Transport: Relief of Axonopathy Resulting from the Toxin β,β′-Iminodipropionitrile
Qinzhang Zhu,
Qinzhang Zhu
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
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Michael Lindenbaum,
Michael Lindenbaum
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
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Françoise Levavasseur,
Françoise Levavasseur
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
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Hélène Jacomy,
Hélène Jacomy
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
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Jean-Pierre Julien
Jean-Pierre Julien
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
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Qinzhang Zhu
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
Michael Lindenbaum
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
Françoise Levavasseur
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
Hélène Jacomy
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
Jean-Pierre Julien
Centre for Research in Neuroscience, McGill University, The Montreal General Hospital Research Institute, Montréal, Qúebec, Canada H3G 1A4
The technical assistance of P. Hince, D. Altshuller, D. Houle, and G. Gagnon is gratefully acknowledged.
Address all correspondence to Jean-Pierre Julien, The Montreal General Hospital Research Institute, 1650 Cedar Avenue, Montréal, Québec, Canada H3G 1A4. Tel.: (514) 937-6011 ext. 2361. Fax: (514) 934-8265. E-mail: [email protected]
Received:
February 05 1998
Revision Received:
June 25 1998
Online ISSN: 1540-8140
Print ISSN: 0021-9525
1998
J Cell Biol (1998) 143 (1): 183–193.
Article history
Received:
February 05 1998
Revision Received:
June 25 1998
Citation
Qinzhang Zhu, Michael Lindenbaum, Françoise Levavasseur, Hélène Jacomy, Jean-Pierre Julien; Disruption of the NF-H Gene Increases Axonal Microtubule Content and Velocity of Neurofilament Transport: Relief of Axonopathy Resulting from the Toxin β,β′-Iminodipropionitrile . J Cell Biol 5 October 1998; 143 (1): 183–193. doi: https://doi.org/10.1083/jcb.143.1.183
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