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Scott Baraban, PhD
Neurobiology of Epilepsy

Epilepsy is one of the most common neurological disorders, affecting nearly 2.5 million Americans - many of them children. Because the hallmark feature of an epileptic brain is the occurrence of abnormal electrical discharge (seizure), our laboratory is focused on intrinsic, synaptic and non-synaptic mechanisms that regulate neuronal excitability. By studying animal models of epilepsy and tissue obtained from patients undergoing surgery for intractable epilepsy we hope to obtain a better understanding of the neurobiological basis of epilepsy. Techniques include the use of in vitro brain slices for patch-clamp recording of membrane properties and synaptic function; molecular analysis of gene expression using in situ hybridization; immunohistochemical and morphological studies of neuronal structure and protein expression; pharmacological analysis of seizure modulation in knockout mice; and a forward-genetic screening strategy to uncover novel epilepsy-related gene mutations. Our current research interests lie in three general areas:

Epilepsy Associated with a Malformed Brain: The methylazoxymethanol-exposed (MAM) rat model, developed in our laboratory, mimics abnormal neuronal migration disorders observed in the cortex and hippocampus of children with intractable epilepsy. MAM rats with hippocampal heterotopia exhibit rare spontaneous seizures, are more susceptible to induced seizures, and are resistant to standard anticonvulsant medications. We have also demonstrated that heterotopic cell clusters (i) contain "epileptic" neurons capable of acting as burst generators in vitro, (ii) exhibit a neocortical phenotype, and (iii) lack a functional Kv4.2 fast-transient type K channel. Similar studies using animal models of Type-I Lissencephaly and Tuberous Sclerosis Complex are underway. As a correlate to animal studies, we also perform research using tissue samples obtained during resective surgery.

Seizures and Seizures Resistance in Zebrafish: Genetic screening approaches wherein mutagen treatment introduces random mutations into the genome and resultant mutants are recovered in subsequent generations is a powerful and un-biased method to identify epilepsy genes. We have developed novel electrophysiological, molecular and behavioral techniques to initiate and characterize epileptic seizure activity in zebrafish. A forward-genetic mutagenesis screen (in collaboration with Herwig Baier) to isolate and characterize "seizure-resistant" mutants is currently underway.

Anticonvulsant Strategies: Neuropeptides, Astrocytes and Stem Cells: Additional areas of investigation in the laboratory are focused on novel anticonvulsant strategies. Specifically, we have studied the anticonvulsant properties of neuropeptide Y (an endogenous modulator of presynaptic excitation) and furosemide (a common diuretic). Each of these agents exhibits powerful anticonvulsant actions in vitro and in vivo. In a new research direction, we are beginning to explore the potential of embryonic progenitor cells (in collaboration with Arturo Alvarez-Buylla) to develop functional and "anticonvulsant" neurons following transplantation.


Selected Publications

Castro PA, Cooper EC, Lowenstein DH, Baraban SC (2001) Hippocampal heterotopia lack functional Kv4.2 potassium channels in the methylazoxymethanol model of cortical malformations and epilepsy. J Neurosci 21:6626-34.

Baraban SC (2002) Antiepileptic actions of neuropeptide Y in the mouse hippocampus require Y5 receptors. Epilepsia 43 Suppl 5:9-13.3.

Calcagnotto ME, Paredes MF, Baraban SC (2002) Heterotopic neurons with altered inhibitory synaptic function in an animal model of malformation-associated epilepsy. J Neurosci 22:7596-605.

Castro PA, Pleasure SJ, Baraban SC (2002) Hippocampal heterotopia with molecular and electrophysiological properties of neocortical neurons. Neuroscience 114:961-72.

Alvarez-Dolado M , Calcagnotto ME , Karkar KM , Southwell DG , Jones-Davis DM , Estrada RC , Rubenstein JL , Alvarez-Buylla A , Baraban SC (2006) Cortical inhibition modified by embryonic neural precursors grafted into the postnatal brain. Journal of Neuroscience 26, 7380-7389.

Wang Y , Greenwood JS , Calcagnotto ME , Kirsch HE , Barbaro NM , Baraban SC (2007) Neocortical hyperexcitability in a human case of tuberous sclerosis complex and mice lacking neuronal expression of TSC1. Annals of Neurology 61, 139-152.

information last updated June 2008
Featured Paper
Baraban Lab
Neocortical hyperexcitability in a human case of tuberous sclerosis complex and mice lacking neuronal expression of TSC1. Annals of Neurology 61, 139-152.
download the paper
Featured Paper
Baraban Lab
Cortical inhibition modified by embryonic neural precursors grafted into the postnatal brain. Journal of Neuroscience 26, 7380-7389.
download the paper


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