Abnormal cerebellar function and tremor in a mouse model for non-manifesting partially penetrant dystonia type 6.
Meike E Van der HeijdenDominic J KizekRoss PerezElena K RuffMichelle E EhrlichRoy V SillitoePublished in: The Journal of physiology (2021)
Loss-of-function mutations in the Thanatos-associated domain-containing apoptosis-associated protein 1 (THAP1) gene cause partially penetrant autosomal dominant dystonia type 6 (DYT6). However, the neural abnormalities that promote the resultant motor dysfunctions remain elusive. Studies in humans show that some non-manifesting DYT6 carriers have altered cerebello-thalamo-cortical function with subtle but reproducible tremor. Here, we uncover that Thap1 heterozygote mice have action tremor that rises above normal baseline values even though they do not exhibit overt dystonia-like twisting behaviour. At the neural circuit level, we show using in vivo recordings in awake Thap1+/- mice that Purkinje cells have abnormal firing patterns and that cerebellar nuclei neurons, which connect the cerebellum to the thalamus, fire at a lower frequency. Although the Thap1+/- mice have fewer Purkinje cells and cerebellar nuclei neurons, the number of long-range excitatory outflow projection neurons is unaltered. The preservation of interregional connectivity suggests that abnormal neural function rather than neuron loss instigates the network dysfunction and the tremor in Thap1+/- mice. Accordingly, we report an inverse correlation between the average firing rate of cerebellar nuclei neurons and tremor power. Our data show that cerebellar circuitry is vulnerable to Thap1 mutations and that cerebellar dysfunction may be a primary cause of tremor in non-manifesting DYT6 carriers and a trigger for the abnormal postures in manifesting patients.
Keyphrases
- deep brain stimulation
- parkinson disease
- cell cycle arrest
- induced apoptosis
- high fat diet induced
- spinal cord
- oxidative stress
- mouse model
- endoplasmic reticulum stress
- newly diagnosed
- ejection fraction
- machine learning
- functional connectivity
- gene expression
- multiple sclerosis
- resting state
- spinal cord injury
- adipose tissue
- chronic kidney disease
- electronic health record
- cell proliferation
- patient reported