Impaired Performance of the Q175 Mouse Model of Huntington’s Disease in the Touch Screen Paired Associates Learning Task

Piiponniemi, Tuukka O.; Parkkari, Teija; Heikkinen, Taneli; Puoliväli, Jukka; Park, Larry C.; Cachope, Roger; Kopanitsa, Maksym V.

doi:10.3389/fnbeh.2018.00226

Cited by 9 publications

(2 citation statements)

References 82 publications

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“…Cognitive deficits are a key clinical hallmark of HD, and impaired performance in tasks related to visual discrimination and cognitive flexibility are some of the earliest quantifiable changes observed in premanifest HD patients, occurring up to 20 years before predicted onset of manifest disease and in the absence of detectable motor phenotypes [119][120][121] . Impairments in learning and memory tasks have also been observed in zQ175 mice, but these assessments have been carried out only in older mice after development of striatal atrophy and other pathological hallmarks 17,[71][72][73][122][123][124][125] .…”

Section: Development Of Early Cognitive Deficits Is Prevented By Gene...mentioning

confidence: 99%

Microglia and complement mediate early corticostriatal synapse loss and cognitive dysfunction in Huntington’s disease

Wilton,

Mastro,

Heller

et al. 2023

Nat Med

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Huntington’s disease (HD) is a devastating monogenic neurodegenerative disease characterized by early, selective pathology in the basal ganglia despite the ubiquitous expression of mutant huntingtin. The molecular mechanisms underlying this region-specific neuronal degeneration and how these relate to the development of early cognitive phenotypes are poorly understood. Here we show that there is selective loss of synaptic connections between the cortex and striatum in postmortem tissue from patients with HD that is associated with the increased activation and localization of complement proteins, innate immune molecules, to these synaptic elements. We also found that levels of these secreted innate immune molecules are elevated in the cerebrospinal fluid of premanifest HD patients and correlate with established measures of disease burden.In preclinical genetic models of HD, we show that complement proteins mediate the selective elimination of corticostriatal synapses at an early stage in disease pathogenesis, marking them for removal by microglia, the brain’s resident macrophage population. This process requires mutant huntingtin to be expressed in both cortical and striatal neurons. Inhibition of this complement-dependent elimination mechanism through administration of a therapeutically relevant C1q function-blocking antibody or genetic ablation of a complement receptor on microglia prevented synapse loss, increased excitatory input to the striatum and rescued the early development of visual discrimination learning and cognitive flexibility deficits in these models. Together, our findings implicate microglia and the complement cascade in the selective, early degeneration of corticostriatal synapses and the development of cognitive deficits in presymptomatic HD; they also provide new preclinical data to support complement as a therapeutic target for early intervention.

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Section: Development Of Early Cognitive Deficits Is Prevented By Gene...mentioning

confidence: 99%

Microglia and complement mediate early corticostriatal synapse loss and cognitive dysfunction in Huntington’s disease

Wilton,

Mastro,

Heller

et al. 2023

Nat Med

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“…Cognitive dysfunction is often reported prior to overt motor symptoms in patients with HD (Stout et al 2012, Harrington et al 2012, Paulsen 2011), but it usually manifests after motor symptom onset in murine models of HD (Farrar et al 2014, Heikkinen et al 2012). Cognitive function in heterozygous zQ175 mice progressively decreases with age, beginning as early as 7 months with robust cognitive impairment at 10-12 months of age (Curtin et al 2015, Southwell et al 2016, Piiponniemi et al 2018). To assess whether cognitive behavior was altered as a function of CK2α’ in HD mice, we performed tests to evaluate associative learning (fear conditioning), spatial learning and memory (Barnes maze, BM), cognitive flexibility (BM reversal) and spatial working memory (Y radial arm maze) by comparing zQ175 and zQ175:CK2α’ (+/-) mice at 12 months of age.…”

Section: Resultsmentioning

confidence: 99%

CK2 alpha prime and alpha-synuclein pathogenic functional interaction mediates synaptic dysregulation in Huntington’s disease

Zarate

Cuccu

et al. 2020

Preprint

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Huntington′s Disease (HD) is a neurodegenerative disorder caused a polyglutamine expansion in the HTT protein. This mutation causes HTT misfolding and aggregation, preferentially affecting neurons of the basal ganglia. Other aggregation-prone proteins like alpha-synuclein (α-syn), mostly associated with Parkinson′s disease (PD), has recently been involved in motor deficits in HD, but its mechanism of action is unknown. Here we showed that α-syn serine 129 phosphorylation (α-syn-pS129), a posttranslational modification linked to α-synucleinopathy, is highly phosphorylated in the brain of symptomatic zQ175 HD mice. We demonstrated that such phosphorylation is mediated by Protein Kinase CK2 alpha prime (CK2α′), which is preferentially induced in striatal neurons in HD. Knocking out one allele of CK2α′ in zQ175 mice decreased α-syn-pS129 in the striatum and ameliorated several HD-like symptoms including neuroinflammation, transcriptional alterations, excitatory synaptic transmission dysfunction and motor deficits. Our data suggests CK2α′-mediated synucleinopathy as a key molecular mechanism for striatal neurons degeneration in HD.

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Behavioral shaping of rhesus macaques using the Cambridge neuropsychological automated testing battery

Wither

Boehnke

Lablans

et al. 2020

Journal of Neuroscience Methods

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Impaired Performance of the Q175 Mouse Model of Huntington’s Disease in the Touch Screen Paired Associates Learning Task

Cited by 9 publications

References 82 publications

Microglia and complement mediate early corticostriatal synapse loss and cognitive dysfunction in Huntington’s disease

Microglia and complement mediate early corticostriatal synapse loss and cognitive dysfunction in Huntington’s disease

CK2 alpha prime and alpha-synuclein pathogenic functional interaction mediates synaptic dysregulation in Huntington’s disease

Behavioral shaping of rhesus macaques using the Cambridge neuropsychological automated testing battery

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