Abstract
Huntingtin is a large HEAT repeat protein first identified in humans, where a polyglutamine tract expansion near the amino terminus causes a gain-of-function mechanism that leads to selective neuronal loss in Huntington's disease (HD). Genetic evidence in humans and knock-in mouse models suggests that this gain-of-function involves an increase or deregulation of some aspect of huntingtin's normal function(s), which remains poorly understood. As huntingtin shows evolutionary conservation, a powerful approach to discovering its normal biochemical role(s) is to study the effects caused by its deficiency in a model organism with a short life-cycle that comprises both cellular and multicellular developmental stages. To facilitate studies aimed at detailed knowledge of huntingtin's normal function(s), we generated a null mutant of hd, the HD ortholog in Dictyostelium discoideum. Dictyostelium cells lacking endogenous huntingtin were viable but during development did not exhibit the typical polarized morphology of Dictyostelium cells, streamed poorly to form aggregates by accretion rather than chemotaxis, showed disorganized F-actin staining, exhibited extreme sensitivity to hypoosmotic stress, and failed to form EDTA-resistant cell–cell contacts. Surprisingly, chemotactic streaming could be rescued in the presence of the bivalent cations Ca2+ or Mg2+ but not pulses of cAMP. Although hd − cells completed development, it was delayed and proceeded asynchronously, producing small fruiting bodies with round, defective spores that germinated spontaneously within a glassy sorus. When developed as chimeras with wild-type cells, hd − cells failed to populate the pre-spore region of the slug. In Dictyostelium, huntingtin deficiency is compatible with survival of the organism but renders cells sensitive to low osmolarity, which produces pleiotropic cell autonomous defects that affect cAMP signaling and as a consequence development. Thus, Dictyostelium provides a novel haploid organism model for genetic, cell biological, and biochemical studies to delineate the functions of the HD protein.
Highlights
Huntington’s disease (HD) is an autosomal dominant neurodegenerative disorder whose clinical manifestations include psychiatric disturbances, cognitive decline and characteristic involuntary movements, typically diagnosed in mid-life [1,2]
We have used Dictyostelium discoideum to study the consequences of huntingtin deficiency
We found that hd2 cells were hypersensitive to hypoosmotic stress
Summary
Huntington’s disease (HD) is an autosomal dominant neurodegenerative disorder whose clinical manifestations include psychiatric disturbances, cognitive decline and characteristic involuntary movements, typically diagnosed in mid-life [1,2]. HD is caused by a CAG trinucleotide repeat expansion mutation (.35 units) that produces an elongated version of a normally polymorphic polyglutamine segment in huntingtin [3,4,5], a large 350 kDa ubiquitously expressed HEAT (huntingtin, elongation factor 3, the A subunit of protein phosphatase 2A, and TOR1) repeat protein. Several lines of evidence indicate that the HD mutation confers a CAG length-dependent ‘gain-of-function’ that likely produces its distinctive neuropathology through a modulatory effect on some structural or functional feature of huntingtin [6,7,8,9]. HD homozygote individuals with two mutant HD genes, and no wildtype huntingtin, develop the characteristic movement disorder with timing comparable to that seen in typical HD mutation heterozygote individuals, indicating the absence of a strong dosage effect. Defining the diseaseproducing ‘gain-of-function’ - either a polyglutamine-length dependent increase or deregulation of a normal huntingtin activity or the introduction of a novel polyglutamine-length dependent activity, will require an understanding of the protein’s normal function(s)
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