Abstract

Malformations of the developing brain are characteristically associated with mental retardation, schizophrenia, and epilepsy. In fact, with recent advances in neuro-imaging it is now clear that cortical malformations are a common feature of therapy-resistant seizure syndromes in children. Unfortunately, since clinical studies are technically limited in the analysis of cellular mechanisms of epileptogenesis, it is not known how dysplastic brain tissue becomes prone to epileptogenesis. To address this problem, we have been studying a unique rodent model of malformation-associated epilepsy i.e., methylazoxymethanol (MAM)-exposed rats. As in humans, malformations in the rat brain consist of disruptions in lamination, aberrant cell clusters, and microdysgenesis. In vivo and in vitro studies indicate that thresholds for generation of seizure activity are markedly reduced in these MAM-exposed rats. Electrophysiological recordings show that displaced cell clusters are capable of independent seizure generation and displaced neurons exhibit abnormal (hyperexcitable) firing properties. As a logical extension of these studies, the planned experiments in the New Investigator proposal will test potential mechanisms by which dysplastic neurons become hyperexcitable. Techniques will involve use of hippocampal slices maintained in vitro, and application of visualized patch-clamp methods to study whole-cell currents and individual ion channels on dysplastic neurons. Pharmacological experiments will be performed to assess how endogenous neurotransmitters modulate the activity of dysplastic neurons. Molecular studies will be performed on tissue from MAM-exposed rats to examine the expression and distribution of potassium channel sub-units. In some studies, simultaneous fluorescent calcium detection and whole-cell voltage-clamp will be used to examine the kinetics of intracellular Ca2+ mobilization in dysplastic tissue.
Three specific aims are proposed: I) to characterize the function of Ca2+-activated channels on dysplastic neurons, II) to examine the expression of K-Ca channels on dysplastic neurons, and the III) to examine intracellular Ca2+ mobilization mechanisms in dysplastic neurons. The results promise to provide new information about cellular mechanisms of epileptogenesis associated with malformations and may lead to the design of novel anticonvulsant treatments for these otherwise intractable forms of epilepsy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS040272-01A1
Application #
6330991
Study Section
Special Emphasis Panel (ZRG1-BDCN-2 (01))
Program Officer
Jacobs, Margaret
Project Start
2001-05-15
Project End
2005-04-30
Budget Start
2001-05-15
Budget End
2002-04-30
Support Year
1
Fiscal Year
2001
Total Cost
$283,125
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Neurosurgery
Type
Schools of Medicine
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Dinday, Matthew T; Girskis, Kelly M; Lee, Sunyoung et al. (2017) PAFAH1B1 haploinsufficiency disrupts GABA neurons and synaptic E/I balance in the dentate gyrus. Sci Rep 7:8269
Toyo-oka, Kazuhito; Wachi, Tomoka; Hunt, Robert F et al. (2014) 14-3-3? and ? regulate neurogenesis and differentiation of neuronal progenitor cells in the developing brain. J Neurosci 34:12168-81
Sebe, Joy Y; Bershteyn, Marina; Hirotsune, Shinji et al. (2013) ALLN rescues an in vitro excitatory synaptic transmission deficit in Lis1 mutant mice. J Neurophysiol 109:429-36
Hunt, Robert F; Dinday, Matthew T; Hindle-Katel, William et al. (2012) LIS1 deficiency promotes dysfunctional synaptic integration of granule cells generated in the developing and adult dentate gyrus. J Neurosci 32:12862-75
Sebe, Joy Y; Baraban, Scott C (2011) The promise of an interneuron-based cell therapy for epilepsy. Dev Neurobiol 71:107-17
Hortopan, Gabriela A; Baraban, Scott C (2011) Aberrant expression of genes necessary for neuronal development and Notch signaling in an epileptic mind bomb zebrafish. Dev Dyn 240:1964-76
Sebe, Joy Y; Looke-Stewart, Elizabeth C; Estrada, Rosanne C et al. (2010) Robust tonic GABA currents can inhibit cell firing in mouse newborn neocortical pyramidal cells. Eur J Neurosci 32:1310-8
Greenwood, Joel S F; Wang, Yanling; Estrada, Rosanne C et al. (2009) Seizures, enhanced excitation, and increased vesicle number in Lis1 mutant mice. Ann Neurol 66:644-53
Battaglia, Giorgio; Becker, Albert J; LoTurco, Joseph et al. (2009) Basic mechanisms of MCD in animal models. Epileptic Disord 11:206-14
Jones, Daniel L; Baraban, Scott C (2009) Inhibitory inputs to hippocampal interneurons are reorganized in Lis1 mutant mice. J Neurophysiol 102:648-58

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