A large portion of the estimated $2.2 trillion stroke-related costs estimated in the U.S. between 2005 and 2050 pertains to the cost of care during the recovery period after the brain trauma, which in turn is highly correlated with the level of disability. These figures point to the urgency of improving post stroke neurorehabilitation, particularly since there are no drugs available, nor are there any in the pipeline, to facilitate functional recovery after stroke. Until recently, only few studies focused on the basic mechanisms and potential improvement of post stroke functional recovery. Previous findings from our laboratory, and some promising human data about non-invasive brain stimulation in recovering stroke patients, point to an imbalance between excitatory/inhibitory cortical circuits as a major obstacle in post stroke functional recovery. We will use a mouse model of stroke to examine how the outcome of brain stimulation after the injury can be improved. Photothrombotic stroke will be induced in the motor cortices of mice using a novel stroke model developed for focal ischemia induction in awake freely moving animals. We will test the hypothesis that the modulation of a highly specific component of the affected cortical microcircuits will provide the best outcome on functional recovery after stroke. Four different transgenic mouse lines will be used for specific optogenetic manipulations of excitatory and inhibitory cortical microcircuits in the peri-infarct region, or in the equivalent cortical area on the contralateral hemisphere. 1) Cortical pyramidal cells will be stimulated in the peri-infarct zone to test the effects of ipsilesonal stimulation of excitatory circuits;2) The activity of inhibitory GABAergic cells will be suppresse in the peri-infarct zone to reduce the enhanced inhibition observed after stroke, previously shown by our lab to obstruct the path to functional recovery;3) Peri-infarct glial cells will be stimulated to test whether impaired glial activity and a secondarily reduced GABA uptake may contribute to the observed enhancement in inhibition and the ensuing delayed functional recovery;4) Contralateral to the infarct, GABAergic cells will be stimulated to dampen the output of the healthy motor cortex which may act to lower the activity of the lesioned side. Optical stimulation will be carried out for 5 days after stroke induction in daily 1-hour sessions, based o protocols of non-invasive, but non-specific brain simulation in human subjects. In addition to more traditional measures of functional motor recovery in mice, we will use a novel automated measurement of the mouse's movements on an air-supported sphere, which can be subjected to better quantification than previously used measures of motor recovery. By introducing novel approaches in stroke induction, stimulation therapy, and outcome metrics, the project addresses scientific questions related to the enormous economical and health burdens of stroke in both the U.S. and worldwide. The project will also identify specific target systems for promoting rehabilitation in the clinical practice, to result in a healthier life and an earlier functional reovery of stroke victims.

Public Health Relevance

Stroke is the major cause of chronic disability worldwide and it is estimated to cost the U.S. $2.2 trillion between 2005 to 2050. A large portion of this amount pertains to the cost of care during the recovery period, which in turn is highly correlated with th level of disability. These figures point to the urgency of improving post-stroke neurorehabilitation, particularly since there are no drugs available, nor are there any in the pipeline to facilitate functional recovery after stroke. Experimental approaches in humans geared to facilitate post-stroke recovery include non-invasive and highly non-specific brain simulation. We will use a mouse model of stroke to examine how we can improve on the outcome of brain stimulation after stroke. Optical stimulation (or dampening) of the activities of specific elements of injured cortical microcircuits will be tested to find out the most effective intervention for stroke recovery. By introducing novel approaches in stroke research, the project will addresses scientific questions related to the enormous health and economical burdens of stroke in both the US and worldwide. The project will identify specific target systems that can be translated in the future into clinical practice, to accomplish a better and speedier recovery of function in stroke victims.

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21NS081438-01
Application #
8426660
Study Section
Brain Injury and Neurovascular Pathologies Study Section (BINP)
Program Officer
Chen, Daofen
Project Start
2012-09-01
Project End
2014-08-31
Budget Start
2012-09-01
Budget End
2013-08-31
Support Year
1
Fiscal Year
2012
Total Cost
$231,000
Indirect Cost
$81,000
Name
University of California Los Angeles
Department
Neurology
Type
Schools of Medicine
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095
Barth, Albert M I; Mody, Istvan (2014) Novel test of motor and other dysfunctions in mouse neurological disease models. J Neurosci Methods 221:151-8