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cSP du
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cSP lengthening was expected to be propor7onal to the total amount of damage throughout the brain. Lower cSP and sICI were predicted to be correlated with more extensive damage to the cor7cal motor hand area.
Neurology and Neurosurgery, McGill University McGill University Health Centre
1. Caramia MD, Palmieri MG, Desiato MT, Boffa L, Galizia P, Rossini PM, Centonze D, Bernardi G: Brain excitability changes in the relapsing and remi4ng phases of mul8ple sclerosis: a study with transcranial magne8c s8mula8on. Clinical neurophysiology : official journal of the Interna7onal Federa7on of Clinical Neurophysiology 2004, 115(4):956-‐965.
2. Fisher E, Lee JC, Nakamura K, Rudick RA: Gray ma>er atrophy in mul8ple sclerosis: a longitudinal study. Annals of neurology 2008, 64(3):255-‐265. 3. Vucic S, Burke T, Lenton K, Ramanathan S, Gomes L, Yannikas C, Kiernan MC: Cor8cal dysfunc8on underlies disability in mul8ple sclerosis. Mul7ple sclerosis (Houndmills, Basingstoke,
England) 2012, 18(4):425-‐432. MTR damage paper 4. Ziemann U. Pharmaco-‐transcranial magne8c s8mula8on studies of motor excitability. Handbook of clinical neurology. 2013;116C:387-‐97.
Nantes JC*, Zhong J, Whatley B, & Koski L
Magne7c resonance imaging techniques provide es7mates of the severity of neural atrophy and demyelina7on occurring the in the brains of people living with MS.
9-hole peg test (9HPT)
Among RRMS pa7ents experiencing a period of clinical remission, we sought to es7mate the extent to which intracor7cal inhibi7on (sICI, cSP) is related to white and grey mader damage.
Despite persis7ng brain damage, pa7ents with RRMS experience periods of clinical remission between periods of symptom exacerba7ons (relapses).
t(27) = 2.35 p < .05
*
Email: [email protected] Lab phone: 514-‐934-‐1934 ext. 34439 Website: hdp://koskilab.mcgill.ca
Thank you to members of the McConnell Brain Imaging Center (BIC) of the Montreal Neurological Ins7tute, for training and assistance with the neuroimaging components of this project.
Lesion analysis
T1 T2 FLAIR PDW Volumetric analysis (normalized to size of skull)
T1
Cortical silent period (cSP) GABAB receptor activity biomarker
Short-interval intracortical inhibition (sICI) GABAA receptor activity biomarker
DEMYELINATION & NEURODEGENERATION
RELAPSING-REMITTING MULTIPLE SCLEROSIS (RRMS)
MAGNETIC RESONANCE IMAGING (MRI)
TRANSCRANIAL MAGNETIC STIMULATION (TMS)
MULTIPLE SCLEROSIS FUNCTIONAL COMPOSITE (MSFC)
NEUROIMAGING OUTCOMES
INTRACORTICAL INHIBITION OUTCOMES
White maFer
INTRACORTICAL INHIBITION CHANGES
C
MTR & INTRACORTICAL INHIBITION
Magnetization Transfer Ratio (MTR)
B RRMS pa7ent (in remission)
Timed 25-foot walk (T25FW) Paced Auditory Serial Addition Test (PASAT)
FIGURE 1. Examples of cSP traces are shown from a control (A) and from a RRMS pa7ent par7cipa7ng during a period of clinical remission (B). Compared to controls, RRMS par7cipants had significantly longer cSP dura7ons (C). From the sICI protocol, an example of a motor-‐evoked poten7al (MEP) induced by a single supra-‐threshold TMS-‐pulse (D) and an inhibited MEP (due to a sub-‐threshold TMS pulse preceding the supra-‐threshold TMS pulse) (E) are shown. Groups did not differ in sICI (F).
0
1
2
3
4
5
6
7
8
9
10
White mader
Grey mader
Brain volume
(normalize
d voxels)
x 100000
0
5
10
15
20
25
30
35
40
45
50
Normal appearing white mader
White mader lesions
Grey mader M1 hand area
MTR
(percent units)
CLINICAL OUTCOMES
FIGURE 2. Compared to controls, RRMS par7cipants had lower volumes of white mader (t(27) = -‐2.75, p < .01) and grey mader (t(27) = -‐2.07, p < .05) (A). Compared to white mader MTR of controls, RRMS par7cipants had significantly lower MTR within both lesioned (t(24) = -‐5.48, p < .0001) and normal appearing white mader (t(24) = -‐1.96, p > .05). Cor7cal MTR within the primary motor cortex (M1) hand area was lower among RRMS par7cipants compared to controls (t(24) = -‐1.99, p < .05), although total brain grey mader MTR did not differ (t(24) = 0.87, p > .05) (B).
Table 1. Mean ± SD score on the Mul7ple Sclerosis Func7onal Composite (MSFC) and raw scores on each MSFC subscale. * p < .01 **p < .05
BRAIN VOLUME & INTRACORTICAL INHIBITION SIENAx
0
20
40
60
80
100
120
140
-‐6 -‐5 -‐4 -‐3 -‐2 -‐1 0 1 2
cSP du
ra7o
n
(ms)
White mader volume (z-‐score)
0
20
40
60
80
100
120
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33
35
37
39
41
43
45
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0 50 100 150 Magne
7za7
on Transfer R
a7o
(percent units)
cSP (ms)
FIGURE 4. Trends toward nega7ve correla7ons were observed between cSP dura7on and white mader MTR signal within normal appearing white mader (r(15) = -‐0.25, p = 0.18), lesioned white mader 7ssue (r(15) = -‐0.31, p = 0.12), grey mader volume (r(15) = -‐0.26, p = 0.17), and grey mader MTR (r(15) = -‐0.23, p = 0.20). Conversely, MTR within the M1 hand area trended in a posi7ve direc7on with cSP (r(15) = 0.23, p = 0.19).
FIGURE 5. Qualita7ve model of interac7ons between intracor7cal inhibi7on and brain damage of persons with mul7ple sclerosis.
0 10 20 30 40 50 60 70 80 90 100
Controls RRMS
sICI (%
inhibi7o
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METHODS
DISCUSSION
BACKGROUND RESULTS
OBJECTIVE
INTRACORTICAL INHIBITION ALTERATION DURING THE REMISSION PHASE OF MULTIPLE SCLEROSIS: RELATION TO WHITE AND GREY MATTER DAMAGE
HYPOTHESIS
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REFERENCES
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sICI & cSP are biomarkers of intracor7cal inhibitory neurotransmission resul7ng from ac7vity at GABAA and GABAB receptors, respec7vely. Ziemann (2013)
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• RRMS par7cipants (in clinical remission) have cSP prolonga7on, indica7ng that ac7vity at intracor7cal GABAB receptors may be abnormally high.
• Low white mader volume is related to cSP prolonga7on during RRMS clinical remission phases.
• Preliminary evidence that damage within the primary motor cortex hand region lowers intracor7cal inhibi7on.
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Caramia et al. (2004) Fisher et al. (2008) Vucic et al (2012)
FIGURE 3. Lower white mader volume predicted longer cSP dura7on (A). The rela7onship between grey mader volume and cSP dura7on did not reach significance (B). Z-‐scores compare individual RRMS par7cipants to the mean ± SD of the control group.
Motor hand area
