Pediatric patients with clinically isolated syndromes at high risk of conversion to multiple sclerosis exhibit brain atrophy while those at low risk of conversion exhibit brain growth

Pediatric patients with clinically isolated syndromes at high risk of conversion to multiple sclerosis exhibit brain atrophy while those at low risk of conversion exhibit brain growth

Background: Accelerated brain atrophy has been observed in all phases of multiple sclerosis (MS), even following the first attack. Measurement of brain atrophy has been suggested as a marker of axonal loss and disease progression. Objective: To determine whether brain volume change is different amon...

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Veröffentlicht in:Multiple sclerosis 2008-09, Vol.14, p.S106-S106
Hauptverfasser: Giacomini, P S, Francis, S J, Narayanan, S, Sled, J G, Sadovnick, D, Bar-Or, A, Banwell, B, Arnold, D L
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container_end_page S106
container_issue
container_start_page S106
container_title Multiple sclerosis
container_volume 14
creator Giacomini, P S
Francis, S J
Narayanan, S
Sled, J G
Sadovnick, D
Bar-Or, A
Banwell, B
Arnold, D L
description Background: Accelerated brain atrophy has been observed in all phases of multiple sclerosis (MS), even following the first attack. Measurement of brain atrophy has been suggested as a marker of axonal loss and disease progression. Objective: To determine whether brain volume change is different among pediatric patients with clinically isolated syndromes (CIS) at high or low risk for progression to MS. Methods: Serial magnetic resonance imaging (MRI) images from 22 children enrolled in the prospective Canadian Pediatric Demyelinating Study were analyzed. Patients were designated as either low risk (n=13) if they remained free of clinical relapse or MRI evidence of new lesions at 12 months, and as high risk (n=9), if new lesions developed on subsequent MRI scans or if they were diagnosed with definite MS based on clinical relapses. Images were acquired using a standardized research protocol on a GE Signa Excite 1.5T scanner at baseline (within 7 days of onset of the initial demyelinating event) and at 3, 6 and 9 months. After pre-processing, percent brain volume change was calculated using SIENA 2.5 from FSL 4.0.1. Brain volume changes were calculated longitudinally relative to the baseline scan. Results: Patient ages were comparable, 10.8 plus or minus 2.3 for the high-risk and 10.2 plus or minus 3.7 for the low-risk groups. Significant differences in brain volume change between the groups were apparent at the 9 month time point relative to the baseline scan. By month 9, the percent brain volume changes were -1.5 plus or minus 1.2% (mean plus or minus SD) in the high-risk group and 0.3 plus or minus 1.1% in the low-risk group. The differences between the low-risk and high-risk groups were statistically significant (p =0.002). Conclusions: In contrast with children with an isolated episode of demyelination who demonstrate stability or age-expected brain growth, brain atrophy can be detected in children at high risk of MS. These findings implicate both a predictive and primary role for neurodegeneration early in the MS disease process and raise concern regarding the implication of brain atrophy on the long-term physical and cognitive outcome in these children.
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Measurement of brain atrophy has been suggested as a marker of axonal loss and disease progression. Objective: To determine whether brain volume change is different among pediatric patients with clinically isolated syndromes (CIS) at high or low risk for progression to MS. Methods: Serial magnetic resonance imaging (MRI) images from 22 children enrolled in the prospective Canadian Pediatric Demyelinating Study were analyzed. Patients were designated as either low risk (n=13) if they remained free of clinical relapse or MRI evidence of new lesions at 12 months, and as high risk (n=9), if new lesions developed on subsequent MRI scans or if they were diagnosed with definite MS based on clinical relapses. Images were acquired using a standardized research protocol on a GE Signa Excite 1.5T scanner at baseline (within 7 days of onset of the initial demyelinating event) and at 3, 6 and 9 months. After pre-processing, percent brain volume change was calculated using SIENA 2.5 from FSL 4.0.1. Brain volume changes were calculated longitudinally relative to the baseline scan. Results: Patient ages were comparable, 10.8 plus or minus 2.3 for the high-risk and 10.2 plus or minus 3.7 for the low-risk groups. Significant differences in brain volume change between the groups were apparent at the 9 month time point relative to the baseline scan. By month 9, the percent brain volume changes were -1.5 plus or minus 1.2% (mean plus or minus SD) in the high-risk group and 0.3 plus or minus 1.1% in the low-risk group. The differences between the low-risk and high-risk groups were statistically significant (p =0.002). Conclusions: In contrast with children with an isolated episode of demyelination who demonstrate stability or age-expected brain growth, brain atrophy can be detected in children at high risk of MS. These findings implicate both a predictive and primary role for neurodegeneration early in the MS disease process and raise concern regarding the implication of brain atrophy on the long-term physical and cognitive outcome in these children.</description><identifier>ISSN: 1352-4585</identifier><language>eng</language><ispartof>Multiple sclerosis, 2008-09, Vol.14, p.S106-S106</ispartof><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,780,784</link.rule.ids></links><search><creatorcontrib>Giacomini, P S</creatorcontrib><creatorcontrib>Francis, S J</creatorcontrib><creatorcontrib>Narayanan, S</creatorcontrib><creatorcontrib>Sled, J G</creatorcontrib><creatorcontrib>Sadovnick, D</creatorcontrib><creatorcontrib>Bar-Or, A</creatorcontrib><creatorcontrib>Banwell, B</creatorcontrib><creatorcontrib>Arnold, D L</creatorcontrib><title>Pediatric patients with clinically isolated syndromes at high risk of conversion to multiple sclerosis exhibit brain atrophy while those at low risk of conversion exhibit brain growth</title><title>Multiple sclerosis</title><description>Background: Accelerated brain atrophy has been observed in all phases of multiple sclerosis (MS), even following the first attack. Measurement of brain atrophy has been suggested as a marker of axonal loss and disease progression. Objective: To determine whether brain volume change is different among pediatric patients with clinically isolated syndromes (CIS) at high or low risk for progression to MS. Methods: Serial magnetic resonance imaging (MRI) images from 22 children enrolled in the prospective Canadian Pediatric Demyelinating Study were analyzed. Patients were designated as either low risk (n=13) if they remained free of clinical relapse or MRI evidence of new lesions at 12 months, and as high risk (n=9), if new lesions developed on subsequent MRI scans or if they were diagnosed with definite MS based on clinical relapses. Images were acquired using a standardized research protocol on a GE Signa Excite 1.5T scanner at baseline (within 7 days of onset of the initial demyelinating event) and at 3, 6 and 9 months. After pre-processing, percent brain volume change was calculated using SIENA 2.5 from FSL 4.0.1. Brain volume changes were calculated longitudinally relative to the baseline scan. Results: Patient ages were comparable, 10.8 plus or minus 2.3 for the high-risk and 10.2 plus or minus 3.7 for the low-risk groups. Significant differences in brain volume change between the groups were apparent at the 9 month time point relative to the baseline scan. By month 9, the percent brain volume changes were -1.5 plus or minus 1.2% (mean plus or minus SD) in the high-risk group and 0.3 plus or minus 1.1% in the low-risk group. The differences between the low-risk and high-risk groups were statistically significant (p =0.002). Conclusions: In contrast with children with an isolated episode of demyelination who demonstrate stability or age-expected brain growth, brain atrophy can be detected in children at high risk of MS. 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Measurement of brain atrophy has been suggested as a marker of axonal loss and disease progression. Objective: To determine whether brain volume change is different among pediatric patients with clinically isolated syndromes (CIS) at high or low risk for progression to MS. Methods: Serial magnetic resonance imaging (MRI) images from 22 children enrolled in the prospective Canadian Pediatric Demyelinating Study were analyzed. Patients were designated as either low risk (n=13) if they remained free of clinical relapse or MRI evidence of new lesions at 12 months, and as high risk (n=9), if new lesions developed on subsequent MRI scans or if they were diagnosed with definite MS based on clinical relapses. Images were acquired using a standardized research protocol on a GE Signa Excite 1.5T scanner at baseline (within 7 days of onset of the initial demyelinating event) and at 3, 6 and 9 months. After pre-processing, percent brain volume change was calculated using SIENA 2.5 from FSL 4.0.1. Brain volume changes were calculated longitudinally relative to the baseline scan. Results: Patient ages were comparable, 10.8 plus or minus 2.3 for the high-risk and 10.2 plus or minus 3.7 for the low-risk groups. Significant differences in brain volume change between the groups were apparent at the 9 month time point relative to the baseline scan. By month 9, the percent brain volume changes were -1.5 plus or minus 1.2% (mean plus or minus SD) in the high-risk group and 0.3 plus or minus 1.1% in the low-risk group. The differences between the low-risk and high-risk groups were statistically significant (p =0.002). Conclusions: In contrast with children with an isolated episode of demyelination who demonstrate stability or age-expected brain growth, brain atrophy can be detected in children at high risk of MS. These findings implicate both a predictive and primary role for neurodegeneration early in the MS disease process and raise concern regarding the implication of brain atrophy on the long-term physical and cognitive outcome in these children.</abstract></addata></record>
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title Pediatric patients with clinically isolated syndromes at high risk of conversion to multiple sclerosis exhibit brain atrophy while those at low risk of conversion exhibit brain growth
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