Background Image
Table of Contents Table of Contents
Previous Page  105 / 162 Next Page
Information
Show Menu
Previous Page 105 / 162 Next Page
Page Background

targeted 1-MHz pulsed high intensity focused ultrasound (pHIFU)

system was applied to adult ZF to create the first closed-head injury

model in ZF.

Results:

Automated behavioural testing and Western blot analysis

of susceptible white matter proteins expression demonstrated dose-

dependent response to ultrasound injury. The model also demon-

strated responsiveness to two interventions (hypothermia and hypoxic

preconditioning) shown to be effective in other models of TBI.

Conclusions:

Our results indicate that the ZF response to brain

trauma exhibits similar mechanisms of secondary injury to mammalian

pathophysiology. Our model can be used to rapidly screen potential

therapeutic candidates. This is an important novel tool for investigating

the mechanisms of downstream neuronal death, and for the rapid im-

plementation of large-scale preclinical drug evaluation for TBI.

Keywords: Zebrafish

D2-13

IMMUNE CELL ACTIVATION UNDERLYING LEARNING

AND MEMORY IMPAIRMENT IN THE JUVENILE FEMALE

RAT AFTER REPEAT CLOSED HEAD INJURY

Alicia Meconi

, Brian Christie

University of Victoria, Division of Medical Sciences, Victoria, Ca-

nada

It is well understood that sustaining multiple mild traumatic brain injuries

(mTBI) can increase risk for suffering more persistent and severe

symptoms, yet the physiological cause of this increased risk remains

unclear. Recent work on this problem has focused primarily on adult

male subjects, despite clinical evidence suggesting that that mTBI out-

comes may be worse in females and in children. To investigate this

critical issue in these populations of interest, we developed a clinically-

relevant closed head injury model to induce repeat mild traumatic brain

injury in rodents. This model was used to induce single and repeat mTBI

in juvenile female rats in order to characterize the pathophysiological

processes underlying learning and memory impairment, a common

mTBI symptom. Postnatal day 25–28 female rats received a single closed

head mTBI, or four mTBIs over 26 hours, and a control group received

sham mTBIs. Spatial learning and memory were assessed in the Morris

water maze on the second to seventh day after the final impact. At seven

days post-impact these rats were sacrificed and their brains were ex-

tracted for histological assessment. FluoroJade-C staining and caspase3

immunohistochemistry were used to detect necrotic and apoptotic cell

death in the hippocampus. Immunohistochemical staining of GFAP and

Iba1 were used detect activation and recruitment of astrocytes and mi-

croglia, respectively, in the hippocampus. Preliminary findings show that

repeat mTBI leads to impaired learning and memory in the Morris water

maze, accompanied by immune cell activation and cell death in the

hippocampus. These findings show that this closed head injury model is

able to reliably produce mTBI symptoms and pathology that reflect those

seen in clinical populations. Future investigations will characterise a time

course of these processes in the first week after single and repeat mTBI.

Keywords: repeat mTBI, closed head injury, learning and memory,

pediatric mTBI

D2-14

MECHANICAL RESPONSE OF SWINE EXPOSED TO FREE-

FIELD BLASTS

Liying Zhang

, Ke Feng, Chaoyang Chen, Xin Jin, Srinivas Kallakuri,

John Cavanaugh, Albert King

Wayne State Univ, Biomedical Engineering, Detroit, USA

The mechanism of blast induced traumatic brain injury (BTBI) is not

well understood. BTBI caused by explosion represents the response of

brain to the initial blast waveform. Experimental data on live animals

provides indispensable information of brain neurotrauma caused by

blast exposure. However, there is little knowledge on the biome-

chanical responses of the brain subjected to primary free-field blast

waves in large

in vivo

animal models. This study presents a swine

model of primary blast injury to the brain. The incident blast over-

pressure (IOP) was generated using 8 lbs of C4 charges detonated at

various stand-off distances to the forward facing anesthetized male

Yucatan swine (50–60 kg, ages 6–8 months). The average peak IOP in

the three free-field blast groups were 148.8 kPa (low), 278.9 kPa

(medium), and 409.2 kPa (high). The mechanical responses of the

brain were recorded with intracranial pressure (ICP) sensors placed on

the surface of the brain at 4 locations (frontal, parietal, left and right

temporal, occipital lobe) and the center of the brain. The head kine-

matics were recorded with tri-axial linear accelerometers and tri-axial

angular rate sensors installed on a block with rigid attachment to the

skull. ICP peak values (94–140 kPa, 210–282 kPa, and 312–420 kPa)

at the various brain locations were increased with IOP levels. None-

theless, there was no significant difference in peak values at different

locations of the brain at the same IOP level. Peak resultant head

acceleration (175–636 g) correlated well with peak IOP. The durations

of the linear acceleration and angular velocity were typically less than

3 ms with very little head motion. The results of this model provide

initial detailed response data of swine brain during exposure to pri-

mary blast waves. The experimental data can be used to validate

computer models. When combined with injury data in parallel studies

the ICP responses at different blast levels can be used to help deter-

mine injury mechanisms and thresholds of the brain subjected to

primary blast.

Keywords: Primary blast induced brain injury, Swine model, Open-

field blast, Intracranial pressure measurement, Head acceleration and

velocity,

D3 Poster Session VII - Group D:

Neurotransplantation

D3-01

SURVIVAL AND BIODISTRIBUTION OF HUMAN FETAL

NEURAL STEM CELL TRANSPLANTS IN PENETRATING

BALLISTIC BRAIN INJURY (PBBI)

Shyam Gajavelli

1

, Markus Spurlock

1

, Aminul Ahmed

1

, Karla

Rivera

1

, Lai Yee Leung

3

, Deborah Shear

3

, Shoji Yokobori

2

, Frank

Tortella

3

, Tom Hazel

4

, Ross Bullock

1

1

University of Miami, Miami Project to Cure Paralysis, Miami, USA

2

Department of Emergency and Critical Care Medicine, Nippon

Medical School, Tokyo, Japan

3

Brain Trauma Neuroprotection and Neurorestoration, Center for

Military Psychiatry and Neuroscience, Walter Reed Army Institute of

Research, Silver Spring, USA

4

Neuralstem Inc, Neuralstem Inc, Germantown, USA

Introduction:

Penetrating traumatic brain injuries (PTBI) are asso-

ciated with the worst outcomes with both high mortality and severe

disability. While no treatment strategies are available, neural stem cell

transplantations have emerged as putative therapeutic approach. In

this rodent study, we evaluated the biodistribution of FDA approved

human fetal neural stem cells (hNSC; Neuralstem Inc.) in a rat model

of PTBI: Penetrating ballistic brain injury (PBBI).

Methods:

Adult Sprague-Dawley rats underwent a unilateral pen-

etrating ballistic brain injury (PBBI). Immunosuppression was es-

A-105