Publications by authors named "Konstantina Mylonaki"

Epileptic encephalopathies are generally considered to be functional disruptions in the balance between neural excitation and inhibition. Excitatory and inhibitory voltage-gated ion channels are key targets of antiepileptic drugs, playing a critical role in regulating neuronal excitation and synaptic transmission. Recent research has highlighted the significance of ion channels in various aspects of epilepsy, including presynaptic neurotransmitter release, intrinsic neuronal excitability, and neural synchrony.

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The human brain is characterized by the upregulation of synaptic, mainly glutamatergic, transmission, but its evolutionary origin(s) remain elusive. Here we approached this fundamental question by studying mice transgenic (Tg) for , a human gene involved in glutamate metabolism that emerged in the hominoid and evolved concomitantly with brain expansion. We demonstrate that Tg mice express the human enzyme in hippocampal astrocytes and CA1-CA3 pyramidal neurons.

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Article Synopsis
  • Graphene-based materials, particularly reduced graphene oxide (rGO), present exciting opportunities for creating scaffolds in neural tissue engineering, especially when combined with decellularized extracellular matrix from adipose tissue (adECM).
  • The study explores how varying concentrations of rGO in scaffolds affects the structural interactions and properties, impacting cell adhesion and growth.
  • Higher concentrations of rGO not only promote the differentiation of neural precursor cells into neurons but also influence the behavior of astrocytes, enhancing their reactivity without triggering scar formation.
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Glutamate dehydrogenase 1 (GDH1) contributes to glucose-stimulated insulin secretion in murine β-cells, but not to basic insulin release. The implications of these findings for human biology are unclear as humans have two GDH-specific enzymes: hGDH1 (GLUD1-encoded) and hGDH2 (GLUD2-encoded), a novel enzyme that is highly activated by ADP and L-leucine. Here we studied in vivo glucose homeostasis in transgenic (Tg) mice generated by inserting the GLUD2 gene and its putative regulatory elements into their genome.

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