Abstract

The goal of the present proposal is to gain insight into the mechanisms governing homeostatic neuronal plasticity caused by lasting changes in the GAB Aergic inhibition of central neurons. The equilibrium between excitation (E) and inhibition (I) in the CNS (the E/I balance) is widely accepted to depend on the fine-tuning of its individual components, thus preventing it from tipping over. The overall hypothesis of this proposal can be summarized as follows: changes specifically affecting one of the two types of GABAergic inhibition (phasic/synaptic and tonic/extrasynaptic) will result in well-defined homeostatic changes in the other type of inhibition and in the intrinsic and synaptic excitation of neurons. The end result will be an overall change in excitability capable of balancing out the offset inhibition. Distinct changes in the two functionally separate types of inhibition are expected to differentially offset the E/I balance resulting in markedly different compensatory inhibitory and excitatory alterations. Experimentally, the two types of inhibition will be independently altered by pharmacological, molecular biological or genetic means. The resulting offset in the E/I balance will be studied using high resolution electrophysiological recordings in long-term organotypic slice cultures and acute brain slices obtained from mice. Other experimental approaches will include collaborative anatomical, immunocytochemical, pharmacological, and molecular biological techniques. Homeostatic alterations in the E/I balance will be addressed in a highly specific manner using appropriate knockin and knockout mice for specific GABAA receptor (GABAAR) subunits and second messenger systems. The proposed studies will further our understanding of the physiological plasticity in the CNS, and will help form the basis for therapeutical advances rationally aimed at preventing pathological plasticity of GABAARs. Awareness of the excitatory inertia following withdrawal from allosteric GABAAR modulators, knowledge about the site of action and plasticity of neurosteroids, BZ and alcohol, and a fundamental understanding of homeostatic inhibitory plasticity will advance drug discovery for the treatment of many severely incapacitating neurological and psychiatric disorders with known involvement of the GABA system. Our findings could provide the basis for novel and rationally targeted therapeutical approaches for the cure of anxiety, stress, benzodiazepine withdrawal, and epilepsy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
5P01NS035985-08
Application #
7390253
Study Section
National Institute of Neurological Disorders and Stroke Initial Review Group (NSD)
Project Start
Project End
Budget Start
2007-04-01
Budget End
2008-03-31
Support Year
8
Fiscal Year
2007
Total Cost
$231,921
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Wallner, M; Hanchar, H J; Olsen, R W (2014) Alcohol selectivity of ?3-containing GABAA receptors: evidence for a unique extracellular alcohol/imidazobenzodiazepine Ro15-4513 binding site at the ?+?- subunit interface in ??3? GABAA receptors. Neurochem Res 39:1118-26
Cushman, Jesse D; Moore, Mellissa D; Olsen, Richard W et al. (2014) The role of the ? GABA(A) receptor in ovarian cycle-linked changes in hippocampus-dependent learning and memory. Neurochem Res 39:1140-6
Santhakumar, Vijayalakshmi; Meera, Pratap; Karakossian, Movses H et al. (2013) A reinforcing circuit action of extrasynaptic GABAA receptor modulators on cerebellar granule cell inhibition. PLoS One 8:e72976
Gonzalez, Claudia; Moss, Stephen J; Olsen, Richard W (2012) Ethanol promotes clathrin adaptor-mediated endocytosis via the intracellular domain of ?-containing GABAA receptors. J Neurosci 32:17874-81
Tanaka, Miyabi; Bailey, Julia N; Bai, Dongsheng et al. (2012) Effects on promoter activity of common SNPs in 5' region of GABRB3 exon 1A. Epilepsia 53:1450-6
Maiz, Jaione; Karakossian, Movses H; Pakaprot, Narawut et al. (2012) Prolonging the postcomplex spike pause speeds eyeblink conditioning. Proc Natl Acad Sci U S A 109:16726-30
Bissiere, Stephanie; Zelikowsky, Moriel; Ponnusamy, Ravikumar et al. (2011) Electrical synapses control hippocampal contributions to fear learning and memory. Science 331:87-91
Cushman, Jesse D; Moore, Melissa D; Jacobs, Nate S et al. (2011) Behavioral pharmacogenetic analysis on the role of the ?4 GABA(A) receptor subunit in the ethanol-mediated impairment of hippocampus-dependent contextual learning. Alcohol Clin Exp Res 35:1948-59
Meera, Pratap; Wallner, Martin; Otis, Thomas S (2011) Molecular basis for the high THIP/gaboxadol sensitivity of extrasynaptic GABA(A) receptors. J Neurophysiol 106:2057-64
Meera, Pratap; Olsen, Richard W; Otis, Thomas S et al. (2010) Alcohol- and alcohol antagonist-sensitive human GABAA receptors: tracking ? subunit incorporation into functional receptors. Mol Pharmacol 78:918-24

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