Abstract

The study of neuronal activity in awake, freely moving animals is the most representative view of `normal'neuronal function. Anesthetics and restraint have profound effects on neuronal physiology and the correlate animal behavior. The study of real time neuronal event processing requires recording methods with high temporal bandwidth (>500 kHz) and the ability to detect physiologically relevant events (i.e. voltage changes or calcium flux). Currently only microelectrode recording of single neuronal units, multiunit activity and field potentials have sufficient temporal resolution and portability to allow recording of neuronal activity in freely moving animals. The current project will produce a miniature microscope/imaging chip which can be head mounted and will allow the recording of optical signals of changes in membrane voltage and calcium concentration in neurons in freely moving rodents. We have developed a prototype device that can collect wide field image sequences of fluorescent voltage dye signals. The current application will re-engineer and significantly improve this prototype device. We will systematically engineer each component to maximize excitation light delivery, fluorescent light collection and optical resolution while minimizing weight, volume, and heat generation. The device will be capable of recording rapid (1 kHz) fluorescent image sequences of a 2-3 mm2 area of cortex and detect small changes in F/F (0.1%). The device will contain a custom designed and built excitation light source, dichroic excitation and emission filters, dichroic mirror, collector lens, objective lens and imaging chip. The device will be small (<1.8 cm2) and light weight enough (10g) to be mounted on the head of a freely moving rat and possibly a mouse. The device will be developed and validated in studies of i) barrel cortex activity during active whisking and object discrimination as well as ii) olfactory bulb activity during active sniffing and scent recognition. The device is intended as a precursor to devices that can translate neuronal activity into actions in real time (optical brain machine interface).

Public Health Relevance

This project will develop a device to study brain function in awake, behaving mammals. The device represents the first step in the development of a neuroprosthetic device to capture information from neuronal tissue regarding intended function. Such a device can ultimately be used to allow direct brain control of robotics, computers and instrumentation to allow paralyzed patients a way to exert conscience control of their environment.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS065110-01
Application #
7635195
Study Section
Microscopic Imaging Study Section (MI)
Program Officer
Gnadt, James W
Project Start
2009-08-01
Project End
2011-07-31
Budget Start
2009-08-01
Budget End
2010-07-31
Support Year
1
Fiscal Year
2009
Total Cost
$584,932
Indirect Cost

  Institution

Name
John B. Pierce Laboratory, Inc.
Department
Type
DUNS #
010139210
City
New Haven
State
CT
Country
United States
Zip Code
06519

  Publications

Dundar, Aysegul; Jin, Jonghoon; Martini, Berin et al. (2017) Embedded Streaming Deep Neural Networks Accelerator With Applications. IEEE Trans Neural Netw Learn Syst 28:1572-1583
Barbera, Giovanni; Liang, Bo; Zhang, Lifeng et al. (2016) Spatially Compact Neural Clusters in the Dorsal Striatum Encode Locomotion Relevant Information. Neuron 92:202-213
Han, Zhou; Jin, Lei; Chen, Fuyi et al. (2014) Mechanistic studies of the genetically encoded fluorescent protein voltage probe ArcLight. PLoS One 9:e113873
Sparks, John S; Schelly, Robert C; Smith, W Leo et al. (2014) The covert world of fish biofluorescence: a phylogenetically widespread and phenotypically variable phenomenon. PLoS One 9:e83259
Han, Zhou; Jin, Lei; Platisa, Jelena et al. (2013) Fluorescent protein voltage probes derived from ArcLight that respond to membrane voltage changes with fast kinetics. PLoS One 8:e81295
Tang, Wei; Osman, Ahmad; Kim, Dongsoo et al. (2013) Continuous Time Level Crossing Sampling ADC for Bio-Potential Recording Systems. IEEE Trans Circuits Syst I Regul Pap 60:1407-1418
Jin, Lei; Han, Zhou; Platisa, Jelena et al. (2012) Single action potentials and subthreshold electrical events imaged in neurons with a fluorescent protein voltage probe. Neuron 75:779-85
Barnett, Lauren; Platisa, Jelena; Popovic, Marko et al. (2012) A fluorescent, genetically-encoded voltage probe capable of resolving action potentials. PLoS One 7:e43454
Baker, Bradley J; Jin, Lei; Han, Zhou et al. (2012) Genetically encoded fluorescent voltage sensors using the voltage-sensing domain of Nematostella and Danio phosphatases exhibit fast kinetics. J Neurosci Methods 208:190-6
Osman, Ahmad; Park, Joon Hyuk; Dickensheets, David et al. (2012) Design constraints for mobile, high-speed fluorescence brain imaging in awake animals. IEEE Trans Biomed Circuits Syst 6:446-53

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