Top Abstracts

T1 Poster Session I - VIII - Finalists:

Student Competition Finalists

T1-01

EARLY HINDLIMB UNLOADING PRODUCES CHRONIC

BIOMECHANICAL, PHYSIOLOGICAL AND MOLECULAR

SIGNATURES OF MALADAPTIVE PLASTICITY IN SCI

Kazuhito Morioka

1,2

, Toshiki Tazoe

2,3

, J. Russell Huie

1

, Cristian F.

Guandique

1

, Xiaokui Ma

1

, Jeffrey A. Sacramento

1

, Sakae Tanaka

4

,

Jacqueline C. Bresnahan

1

, Michael S. Beattie

1

, Toru Ogata

2

, Adam R.

Ferguson

1

1

Brain and Spinal Injury Center (BASIC), University of California,

San Francisco, Department of Neurological Surgery, San Francisco,

USA

2

Research Institute, National Rehabilitation Center for the Persons

With Disabilities, Department of Rehabilitation for the Movement

Functions, Saitama, Japan

3

University of Pittsburgh, Department of Physical Medicine and Re-

habilitation, Pittsburgh, USA

4

Faculty of Medicine, The University of Tokyo, Department of Or-

thopaedic Surgery, Tokyo, Japan

Appropriate limb loading is essential for neurorehabilitation after

SCI, in part, because it guides spinal cord neuroplasticity. Complete

unloading such as prolonged bed rest may interfere with functional

recovery, whereas appropriate afferent information through reha-

bilitation may improve function by modulating spinal plasticity.

The impact of limb loading on synaptic plasticity in SCI remains

poorly understood. We investigated long-term biological, biome-

chanical and physiological consequence of hindlimb unloading

(HU) in the acute phase of SCI. Adult female SD rats received a

mild SCI (T9; 50 kdyn, IH). Three days post-injury, subjects were

randomized to two experimental groups: 1) HU by tail suspension,

or 2) normal-loading control. After two weeks, the HU group was

returned to normal loading condition. Animals were monitored until

8 weeks post-injury. Assessments included: 1) BBB locomotor re-

covery; 2) kinematic gait analysis; 3) electrophysiological H-reflex

testing at 8 weeks-post injury; 4) spinal cord tissue analysis using

biomolecular and robotic confocal microscopy assessments of

plasticity-related changes in ventral motorneurons. Results indi-

cated that: 1) HU early after SCI impaired recovery of coordinated

gait characteristics and produced excessive excitation of spinal re-

flex circuits; 2) Chronically increased synaptic glutamate AMPA

receptors on the plasma membrane of spinal motor neurons pro-

viding a cellular mechanism. Our findings suggest that limb un-

loading early after SCI induces maladaptive spinal cord plasticity

that persists to impair functional recovery in chronic phase, pro-

viding a novel mechanistic target for early intervention after SCI to

enhance the effect of rehabilitation in the chronic phase following

injury.

This works was supported by NS088475, NS067092, Wings for

Life Spinal Cord Research Foundation, Craig H. Neilsen Founda-

tion.

Keywords: AMPA, Synaptic Plasticity, Loading, Rehabilitation

T1-02

DENDRITIC MORPHOLOGY AND NEUROTRANSMITTER

TYPE OF THORACIC DESCENDING PROPRIOSPINAL

NEURONS IN SHAM, AXOTOMY, AND GDNF TREATMENT

Lingxiao Deng

1

, Yiwen Ruan

1

, Chen Chen

1

, Christian Corbin Frye

1

,

Dale Sengelaub

1

, Wenhui Xiong

1

, Xiaoming Jin

1

, Xiao-Ming Xu

1

1

Indiana University, Neurosurgery Department, Indianapolis, USA

2

Indiana University, Department of Psychological and Brain Sci-

ences, Bloomington, USA

After spinal cord injury, descending propriospinal neurons (DPSNs)

greatly contributed to spontaneous functional recoveries. However, little

is known regarding their normal dendritic morphology and plasticity

after injury. We applied a G-mutated rabies virus (G-Rabies virus) co-

expressing green fluorescence protein (GFP) to reveal Golgi-like

dendritic morphology of DPSNs, and their response to axotomy and

glial derived neurotrophic factor (GDNF) treatment. We also in-

vestigated their neurotransmitter type. The animals were divided into

three groups: sham or spinal transection injuries (with or without

GDNF). Each group was further divided into injection subgroup A

(Fluorescence Gold, FG) and B (G-Rabies virus), with injection into

the 2

nd

lumbar cord. Three days post-injection, transection was

performed at the 11

th

thoracic level, with gelfoam containing saline

or GDNF transplanted into the lesion gap. Four days post-injury, the

rats were sacrificed. The GFP signal of dendrites in the T7-T9 cord

was visualized via two-photon microscopy, then traced and ana-

lyzed. Our results indicated that the majority of FG labeled DPSNs

in T7-T9 spinal cords were located in the Rexed Lamina VII, with

greater than 90 percent glutamatergic neurons and the remaining 10

percent comprised of choline acetyltransferase, glycine, and GABA.

Uninjured DPSNs had a predominantly dorsal-ventral distribution of

dendrites. However, transection altered this dendritic distribution,

with dorsal-ventral retraction and lateral-medial extension, and in-

creased the density of spine-like structures. Transection caused

cellular death closest to the lesion. Short-term GDNF treatment did

not increase the number of surviving DPSNs but increased the ter-

minal dendritic length and enhanced the transection effect on spine-

like density. To our knowledge this is the first report describing the

neurotransmitter expression and morphologic characteristics of

DPSNs, as well as the dendritic response after transection injury and

GDNF treatment.

Keywords: Descending propriospinal neuron, dendrite, spine, rabies

virus, neurotransmitter, glial derived neurotrophic factor

A-2