Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model

Hereditary spastic paraplegias (HSPs) comprise a group of genetically heterogeneous neurodegenerative disorders characterized by spastic weakness of the lower extremities. We have generated a Drosophila model for HSP type 10 (SPG10), caused by mutations in KIF5A. KIF5A encodes the heavy chain of kin...

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Autores principales: Füger, Petra, Sreekumar, Vrinda, Schüle, Rebecca, Kern, Jeannine V., Stanchev, Doychin T., Schneider, Carola D., Karle, Kathrin N., Daub, Katharina J., Siegert, Vera K., Flötenmeyer, Matthias, Schwarz, Heinz, Schöls, Ludger, Rasse, Tobias M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3510046/
https://www.ncbi.nlm.nih.gov/pubmed/23209432
http://dx.doi.org/10.1371/journal.pgen.1003066
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author Füger, Petra
Sreekumar, Vrinda
Schüle, Rebecca
Kern, Jeannine V.
Stanchev, Doychin T.
Schneider, Carola D.
Karle, Kathrin N.
Daub, Katharina J.
Siegert, Vera K.
Flötenmeyer, Matthias
Schwarz, Heinz
Schöls, Ludger
Rasse, Tobias M.
author_facet Füger, Petra
Sreekumar, Vrinda
Schüle, Rebecca
Kern, Jeannine V.
Stanchev, Doychin T.
Schneider, Carola D.
Karle, Kathrin N.
Daub, Katharina J.
Siegert, Vera K.
Flötenmeyer, Matthias
Schwarz, Heinz
Schöls, Ludger
Rasse, Tobias M.
author_sort Füger, Petra
collection PubMed
description Hereditary spastic paraplegias (HSPs) comprise a group of genetically heterogeneous neurodegenerative disorders characterized by spastic weakness of the lower extremities. We have generated a Drosophila model for HSP type 10 (SPG10), caused by mutations in KIF5A. KIF5A encodes the heavy chain of kinesin-1, a neuronal microtubule motor. Our results imply that SPG10 is not caused by haploinsufficiency but by the loss of endogenous kinesin-1 function due to a selective dominant-negative action of mutant KIF5A on kinesin-1 complexes. We have not found any evidence for an additional, more generalized toxicity of mutant Kinesin heavy chain (Khc) or the affected kinesin-1 complexes. Ectopic expression of Drosophila Khc carrying a human SPG10-associated mutation (N256S) is sufficient to disturb axonal transport and to induce motoneuron disease in Drosophila. Neurofilaments, which have been recently implicated in SPG10 disease manifestation, are absent in arthropods. Impairments in the transport of kinesin-1 cargos different from neurofilaments are thus sufficient to cause HSP–like pathological changes such as axonal swellings, altered structure and function of synapses, behavioral deficits, and increased mortality.
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spelling pubmed-35100462012-12-03 Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model Füger, Petra Sreekumar, Vrinda Schüle, Rebecca Kern, Jeannine V. Stanchev, Doychin T. Schneider, Carola D. Karle, Kathrin N. Daub, Katharina J. Siegert, Vera K. Flötenmeyer, Matthias Schwarz, Heinz Schöls, Ludger Rasse, Tobias M. PLoS Genet Research Article Hereditary spastic paraplegias (HSPs) comprise a group of genetically heterogeneous neurodegenerative disorders characterized by spastic weakness of the lower extremities. We have generated a Drosophila model for HSP type 10 (SPG10), caused by mutations in KIF5A. KIF5A encodes the heavy chain of kinesin-1, a neuronal microtubule motor. Our results imply that SPG10 is not caused by haploinsufficiency but by the loss of endogenous kinesin-1 function due to a selective dominant-negative action of mutant KIF5A on kinesin-1 complexes. We have not found any evidence for an additional, more generalized toxicity of mutant Kinesin heavy chain (Khc) or the affected kinesin-1 complexes. Ectopic expression of Drosophila Khc carrying a human SPG10-associated mutation (N256S) is sufficient to disturb axonal transport and to induce motoneuron disease in Drosophila. Neurofilaments, which have been recently implicated in SPG10 disease manifestation, are absent in arthropods. Impairments in the transport of kinesin-1 cargos different from neurofilaments are thus sufficient to cause HSP–like pathological changes such as axonal swellings, altered structure and function of synapses, behavioral deficits, and increased mortality. Public Library of Science 2012-11-29 /pmc/articles/PMC3510046/ /pubmed/23209432 http://dx.doi.org/10.1371/journal.pgen.1003066 Text en © 2012 Füger et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Füger, Petra
Sreekumar, Vrinda
Schüle, Rebecca
Kern, Jeannine V.
Stanchev, Doychin T.
Schneider, Carola D.
Karle, Kathrin N.
Daub, Katharina J.
Siegert, Vera K.
Flötenmeyer, Matthias
Schwarz, Heinz
Schöls, Ludger
Rasse, Tobias M.
Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model
title Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model
title_full Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model
title_fullStr Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model
title_full_unstemmed Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model
title_short Spastic Paraplegia Mutation N256S in the Neuronal Microtubule Motor KIF5A Disrupts Axonal Transport in a Drosophila HSP Model
title_sort spastic paraplegia mutation n256s in the neuronal microtubule motor kif5a disrupts axonal transport in a drosophila hsp model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3510046/
https://www.ncbi.nlm.nih.gov/pubmed/23209432
http://dx.doi.org/10.1371/journal.pgen.1003066
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