Isolation of the murine Glut1 deficient thalamocortical circuit: wavelet characterization and reverse glucose dependence of low and gamma frequency oscillations.
Elysandra M SolisLevi B GoodRafael Granja VázquezSourav S PatnaikAna G Hernandez-ReynosoQian MaGustavo AnguloAksharkumar DobariyaStuart F CoganJoseph J PancrazioJuan M PascualVikram JakkamsettiPublished in: bioRxiv : the preprint server for biology (2023)
Glucose represents the principal brain energy source. Thus, not unexpectedly, genetic glucose transporter 1 (Glut1) deficiency (G1D) manifests with encephalopathy. G1D seizures, which constitute a prominent disease manifestation, often prove refractory to medications but may respond to therapeutic diets. These seizures are associated with aberrant thalamocortical oscillations as inferred from human electroencephalography and functional imaging. Mouse electrophysiological recordings indicate that inhibitory neuron failure in thalamus and cortex underlies these abnormalities. This provides the motivation to develop a neural circuit testbed to characterize the mechanisms of thalamocortical synchronization and the effects of known or novel interventions. To this end, we used mouse thalamocortical slices on multielectrode arrays and characterized spontaneous low frequency oscillations and less frequent 30-50 Hz or gamma oscillations under near-physiological bath glucose concentration. Using the cortical recordings from layer IV, we quantified oscillation epochs via an automated wavelet-based algorithm. This method proved analytically superior to power spectral density, short-time Fourier transform or amplitude-threshold detection. As expected from human observations, increased bath glucose reduced the lower frequency oscillations while augmenting the gamma oscillations, likely reflecting strengthened inhibitory neuron activity. This approach provides an ex vivo method for the evaluation of mechanisms, fuels, and pharmacological agents in a crucial G1D epileptogenic circuit.
Keyphrases
- working memory
- blood glucose
- endothelial cells
- high resolution
- metabolic syndrome
- induced pluripotent stem cells
- machine learning
- convolutional neural network
- magnetic resonance imaging
- skeletal muscle
- high frequency
- white matter
- gene expression
- computed tomography
- genome wide
- weight loss
- insulin resistance
- brain injury
- contrast enhanced