Abstract

The proposed research is a direct extension of the research carried out in the previous 3 years. The capacity of magnetoencephalography (MEG) in identifying active tissues in the porcine brain will be evaluated in order to establish a solid empirical basis for interpreting MEG signals from gyrencephalic brains including the human brain. We will determine the subcortical generator responsible for the novel somatic evoked field (SEF) found to be generated by a structure deeper than the thalamus. This generator appears to be the spinal division of the trigeminal -nuclei that carries nociceptive information. If so, we will be demonstrating a capability of MEG with important clinical applications, i.e., the capability of detecting subcortical activities related to pain. Field potentials within the brain associated with this response were quite distinct from those associated with presumably cutaneous responses. We will use mechanical and electrical stimuli to stimulate the cutaneous and nociceptive pathways, and verify the differences in the pathways activated with depth recordings. The cortical areas receiving projections from these two pathways will be found with MEG and ECoG. Our ablation results indicated that the three areas (two areas in the primary somatosensory area (51) and one area in the secondary somatosensory area, 511) can be distinguished with MEG. We will also test whether multiple areas of activation found within the coronal 51 area correspond to areas 3b, 1 and 2 of the primate. In addition to the study of cortical projections from the peripheral afferents, we will study the cortico-cortical connections to determine whether MEG is useful for measuring such connections. The connections between the cortical areas identified from the above study will be investigated by electronically stimulating one area and recording induced activities in connected cortical areas within and across the hemispheres. Our MEG sensor is sensitive enough to record induced, time-locked by phase-unlocked cortical responses during single epochs from a specific cortical areas. Thus, we expect to be able to study the cortical connections. If this is feasible, we will be demonstrating a new capability of MEG for studying brain functions. Finally, we will use MEG to estimate the size of active tissue from the magnitude of SEF for early cortical responses and also by applying a linear estimating algorithm which has been shown to be capable of estimating not only size but also shape of active tissue in a sulcus on stimulated data. If this is the case for empirical data, we can demonstrate that size and perhaps shape of active tissue may be estimated with MEG.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
3R01NS030968-06S1
Application #
6202666
Study Section
Neurology A Study Section (NEUA)
Program Officer
Heetderks, William J
Project Start
1993-08-01
Project End
2001-01-31
Budget Start
1999-02-01
Budget End
2001-01-31
Support Year
6
Fiscal Year
2000
Total Cost
$61,168
Indirect Cost

  Institution

Name
University of New Mexico
Department
Neurology
Type
Schools of Medicine
DUNS #
829868723
City
Albuquerque
State
NM
Country
United States
Zip Code
87131

  Publications

Murakami, Shingo; Okada, Yoshio (2015) Invariance in current dipole moment density across brain structures and species: physiological constraint for neuroimaging. Neuroimage 111:49-58
Tanosaki, Masato; Ishibashi, Hideaki; Zhang, Tongsheng et al. (2014) Effective connectivity maps in the swine somatosensory cortex estimated from electrocorticography and validated with intracortical local field potential measurements. Brain Connect 4:100-11
Zhang, Tongsheng; Okada, Yoshio (2006) Recursive artifact windowed-single tone extraction method (RAW-STEM) as periodic noise filter for electrophysiological signals with interfering transients. J Neurosci Methods 155:308-18
Mun-Bryce, Sheila; Roberts, Lisa; Bartolo, Anton et al. (2006) Transhemispheric depolarizations persist in the intracerebral hemorrhage swine brain following corpus callosal transection. Brain Res 1073-1074:481-90
Flemming, Lars; Wang, Yaozhi; Caprihan, Arvind et al. (2005) Evaluation of the distortion of EEG signals caused by a hole in the skull mimicking the fontanel in the skull of human neonates. Clin Neurophysiol 116:1141-52
Wang, Yaozhi; Hosler, Gregory; Zhang, Tongsheng et al. (2005) Effects of temporary bilateral ligation of the internal carotid arteries on the low- and high-frequency somatic evoked potentials in the swine. Clin Neurophysiol 116:2420-8
Ikeda, Hiroaki; Wang, Yaozhi; Okada, Yoshio C (2005) Origins of the somatic N20 and high-frequency oscillations evoked by trigeminal stimulation in the piglets. Clin Neurophysiol 116:827-41
Okada, Y; Ikeda, I; Zhang, T et al. (2005) High-frequency signals (> 400 hz): a new window in electrophysiological analysis of the somatosensory system. Clin EEG Neurosci 36:285-92
Mun-Bryce, Sheila; Wilkerson, Arika; Pacheco, Bernadette et al. (2004) Depressed cortical excitability and elevated matrix metalloproteinases in remote brain regions following intracerebral hemorrhage. Brain Res 1026:227-34
Mun-Bryce, Sheila; Roberts, Lisa J M; Hunt, W Curtis et al. (2004) Acute changes in cortical excitability in the cortex contralateral to focal intracerebral hemorrhage in the swine. Brain Res 1026:218-26

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