4.6 Article

Characterization of kinesin switch I mutations that cause hereditary spastic paraplegia

Journal

PLOS ONE
Volume 12, Issue 7, Pages -

Publisher

PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0180353

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Funding

  1. Louisiana Cancer Research Consortium
  2. NIH-RCMI from the National Institutes on Minority Health and Health Disparities [2G12MD007595-06]
  3. Institutional Development Award (IDeA) from the National Institute of General Medical Sciences of the National Institutes of Health [P20GM103424]
  4. National Institute of General Medical Sciences of the National Institutes of Health [5UL1GM118967, R01GM066328]

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Kif5A is a neuronally-enriched isoform of the Kinesin-1 family of cellular transport motors. 23 separate mutations in the motor domain of Kif5A have been identified in patients with the complicated form of hereditary spastic paraplegia (HSP). We performed in vitro assays on dimeric recombinant Kif5A with HSP-causing mutations in the Switch I domain, which participates in the coordination and hydrolysis of ATP by kinesin. We observed a variety of significantly reduced catalytic and mechanical activities as a result of each mutation, with the shared phenotype from each that motility was significantly reduced. Substitution of Mn (2+) for Mg (2+) in our reaction buffers provides a dose-dependent rescue in both the catalytic and ensemble mechanical properties of the S203C mutant. This work provides mechanistic insight into the cause of HSP in patients with these mutations and points to future experiments to further dissect the root cause of this disease.

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