Abstract

Medical drugs used in treatment of schizophrenia or depression exert their action through the modulation of dopaminergic neurotransmission. The exact mechanism of such therapy is unknown, partly because the normal physiological role of dopamine release in the cortex is also not fully understood. Electron microscope studies, performed postmortem on the brains of people who suffered from schizophrenia, revealed microscopic structural abnormalities that affect the dendrites of cortical pyramidal neurons. Changes in cortical thickness and dendritic ultrastructure, detected postmortem, could be due to a very long (lifetime) duration of the mental illness and/or a very long (chronic) drug therapy. However, recent clinical studies revealed clear changes in grey matter volume in schizophrenic patients at the very onset of the disease;during the transition from pre-psychotic to psychotic phase. What is the causal relation between the efficacy of dopaminergic drugs, and impairment in dendritic structure and function? The answer to this question may lie in the anatomical juxtaposition of the glutamatergic and dopaminergic systems in the frontal part of human brain, responsible for cognition, planning, control of emotions and decision making. In the prefrontal cortex (an area strongly implicated in pathophysiology of schizophrenia) individual dendritic spines are occupied by two presynaptic terminals;one axon terminal that secretes the excitatory transmitter (glutamate), and the other one that secretes modulatory transmitter dopamine. Twenty years after the discovery of direct dopamine synapse onto a cortical pyramidal neuron, the exact functional consequence of dopamine release at the postsynaptic membrane, in distal dendrites, is still unknown. In the laboratory, we are mimicking the arrival of glutamatergic and dopaminergic cortical inputs by combining excitatory synaptic stimulation of individual dendritic branches with local application of dopamine through a glass micropipette. This approach allows precise control of the location of excitatory input in the dendritic tree;precise timing and duration. Local applications of exogenous glutamate and dopamine eliminate presynaptic mechanisms in the interpretation of experimental results. With the help of voltage-sensitive dyes, the effects of dopamine on dendritic membrane potential will be analyzed simultaneously at the synaptic stimulation site, as well as in the neighboring dendrites that are exposed to neither glutamate nor dopamine. The proposed experiments are expected to yield a more complete picture of how local fluctuations in dopamine level can shape integration of signals in individual neurons, and provide impetus for new preventive and therapeutic approaches in treatment of psychiatric disorders associated with dopaminergic dysfunction.

Public Health Relevance

Antic, Srdjan, D. Narrative In the prefrontal cortex, a brain area implicated in pathophysiology of schizophrenia, neurons receive numerous synaptic contacts from dopamine-rich fibers. At present, it is not clear how exactly release of dopamine affects the activity of cortical neurons in health or disease. By using electrical and optical recordings from neurons treated with short pulses of dopamine, we attempt to learn more about the nature of dopamine modulatory role in cortical information processing, and obtain new information that might improve preventive and therapeutic strategies in the treatment of mental disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH063503-09
Application #
7816821
Study Section
Neurotransporters, Receptors, and Calcium Signaling Study Section (NTRC)
Program Officer
Asanuma, Chiiko
Project Start
2001-08-10
Project End
2012-04-30
Budget Start
2010-05-01
Budget End
2012-04-30
Support Year
9
Fiscal Year
2010
Total Cost
$395,799
Indirect Cost

  Institution

Name
University of Connecticut
Department
Neurosciences
Type
Schools of Medicine
DUNS #
022254226
City
Farmington
State
CT
Country
United States
Zip Code
06030

  Publications

Antic, Srdjan D; Hines, Michael; Lytton, William W (2018) Embedded ensemble encoding hypothesis: The role of the ""Prepared"" cell. J Neurosci Res 96:1543-1559
Oikonomou, Katerina D; Singh, Mandakini B; Rich, Matthew T et al. (2015) Contribution of extrasynaptic N-methyl-D-aspartate and adenosine A1 receptors in the generation of dendritic glutamate-mediated plateau potentials. Philos Trans R Soc Lond B Biol Sci 370:
Popovic, Marko; Vogt, Kaspar; Holthoff, Knut et al. (2015) Imaging Submillisecond Membrane Potential Changes from Individual Regions of Single Axons, Dendrites and Spines. Adv Exp Med Biol 859:57-101
Zhou, Wen-Liang; Short, Shaina M; Rich, Matthew T et al. (2015) Branch specific and spike-order specific action potential invasion in basal, oblique, and apical dendrites of cortical pyramidal neurons. Neurophotonics 2:021006
Belinsky, Glenn S; Rich, Matthew T; Sirois, Carissa L et al. (2014) Patch-clamp recordings and calcium imaging followed by single-cell PCR reveal the developmental profile of 13 genes in iPSC-derived human neurons. Stem Cell Res 12:101-18
Zhou, Wen-Liang; Oikonomou, Katerina D; Short, Shaina M et al. (2013) Dopaminergic regulation of dendritic calcium: fast multisite calcium imaging. Methods Mol Biol 964:123-38
Oikonomou, Katerina D; Short, Shaina M; Rich, Matthew T et al. (2012) Extrasynaptic glutamate receptor activation as cellular bases for dynamic range compression in pyramidal neurons. Front Physiol 3:334
Zhou, Wen-Liang; Antic, Srdjan D (2012) Rapid dopaminergic and GABAergic modulation of calcium and voltage transients in dendrites of prefrontal cortex pyramidal neurons. J Physiol 590:3891-911
Moore, Anna R; Zhou, Wen-Liang; Potapenko, Evgeniy S et al. (2011) Brief dopaminergic stimulations produce transient physiological changes in prefrontal pyramidal neurons. Brain Res 1370:1-15
Moore, Anna R; Zhou, Wen-Liang; Jakovcevski, Igor et al. (2011) Spontaneous electrical activity in the human fetal cortex in vitro. J Neurosci 31:2391-8

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