Cognitive deficits in episodic ataxia type 2 mouse models.
Pauline BohneDamian Boden-El MourabitMareike JostenMelanie D MarkPublished in: Human molecular genetics (2022)
Episodic ataxia type 2 (EA2) is a rare autosomal dominant disorder characterized by motor incoordination, paroxysmal dystonia, vertigo, nystagmus and more recently cognitive deficits. To date over 100 mutations in the CACNA1A gene have been identified in EA2 patients leading to a loss of P/Q-type channel activity, dysfunction of cerebellar Purkinje cells and motor incoordination. To determine if the cerebellum is contributing to these cognitive deficits, we examined two different EA2 mouse models for cognition impairments where CACNA1A was removed specifically from cerebellar Purkinje or granule cells postnatally. Both mutant mouse models showed anxiolytic behavior to lighted, open areas in the open field and light/dark place preference tests but enhanced anxiousness in the novel suppressed feeding test. However, EA2 mice continued to show augmented latencies in the light/dark preference test and when the arena was divided into two dark zones in the dark/dark preference test. Moreover, increased latencies were also displayed in the novel object recognition test, indicating that EA2 mice are indecisive and anxious to explore new territories and objects and may have memory recognition deficits. Exposure to a foreign mouse led to deficiencies in attention and sniffing as well as in social and genital sniffing. These data suggest that postnatal removal of the P/Q type calcium channel from the cerebellum regulates neuronal activity involved in anxiety, memory, decision making and social interactions. Our EA2 mice will provide a model to identify the mechanisms and therapeutic agents underlying cognitive and psychiatric disorders seen in EA2 patients.
Keyphrases
- mouse model
- end stage renal disease
- working memory
- ejection fraction
- newly diagnosed
- chronic kidney disease
- healthcare
- early onset
- decision making
- prognostic factors
- minimally invasive
- traumatic brain injury
- high fat diet induced
- mental health
- oxidative stress
- cell cycle arrest
- peritoneal dialysis
- type diabetes
- multiple sclerosis
- machine learning
- atrial fibrillation
- physical activity
- deep learning
- mild cognitive impairment
- insulin resistance
- white matter
- metabolic syndrome
- subarachnoid hemorrhage
- wild type