A humanized Caenorhabditis elegans model of hereditary spastic paraplegia-associated variants in KLC4

Author:

Gümüşderelioğlu Selin1,Resch Lauren2,Brock Trisha2,Luxton G. W. Gant1ORCID,Cope Heidi3,Tan Queenie K.-G.3,Hopkins Christopher2,Starr Daniel A.1ORCID,

Affiliation:

1. University of California, Davis 1 Department of Molecular and Cellular Biology , , Davis, CA 95616 , USA

2. InVivo Biosystems 2 , Eugene, OR 97402 , USA

3. Duke University Medical Center 4 Division of Medical Genetics, Department of Pediatrics , , Durham, NC 27710 , USA

Abstract

ABSTRACT Hereditary spastic paraplegia (HSP) is a group of degenerative neurological disorders. We identified a variant in human kinesin light chain 4 (KLC4) that is suspected to be associated with autosomal-dominant HSP. How this and other variants relate to pathologies is unknown. We created a humanized Caenorhabditis elegans model in which klc-2 was replaced by human KLC4 (referred to as hKLC4) and assessed the extent to which hKLC4 retained function in the worm. We observed a slight decrease in motility but no nuclear migration defects in the humanized worms, suggesting that hKLC4 retains much of the function of klc-2. Five hKLC4 variants were introduced into the humanized model. The clinical variant led to early lethality, with significant defects in nuclear migration when homozygous and a weak nuclear migration defect when heterozygous, possibly correlating with the clinical finding of late-onset HSP when the proband was heterozygous. Thus, we were able to establish humanized C. elegans as an animal model for HSP and to use it to test the significance of five variants of uncertain significance in the human gene KLC4.

Funder

Office of Strategic Coordination

NIH Office of the Director

National Institutes of Health

University of California, Davis

Publisher

The Company of Biologists

Subject

General Biochemistry, Genetics and Molecular Biology,Immunology and Microbiology (miscellaneous),Medicine (miscellaneous),Neuroscience (miscellaneous)

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