Vanishing MS T2-bright lesions before puberty : A distinct MRI phenotype?

Vanishing MS T2-bright lesions before puberty : A distinct MRI phenotype?

Multiple sclerosis (MS) onset before puberty may have a distinct clinical presentation. Pediatric patients with MS may less often meet MRI diagnostic criteria for adults. Whether initial MRI presentation is distinct in prepubertal patients is unknown. We queried the UCSF MS database for pediatric pa...

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Bibliographic Details
Published in:Neurology Vol. 71; no. 14; pp. 1090 - 1093
Main Authors: CHABAS, D, CASTILLO-TRIVINO, T, MOWRY, E. M, STROBER, J. B, GLENN, O. A, WAUBANT, E
Format: Journal Article
Language:English
Published: Hagerstown, MD Lippincott Williams & Wilkins 30-09-2008
Subjects:
Adolescent
Age of Onset
Aging - physiology
Biological and medical sciences
Brain - growth & development
Brain - pathology
Brain - physiopathology
Child
Child, Preschool
Diagnosis, Differential
Diffusion Magnetic Resonance Imaging - methods
Disease Progression
Female
Humans
Male
Medical sciences
Multiple sclerosis and variants. Guillain barré syndrome and other inflammatory polyneuropathies. Leukoencephalitis
Multiple Sclerosis, Relapsing-Remitting - diagnosis
Multiple Sclerosis, Relapsing-Remitting - physiopathology
Nerve Fibers, Myelinated - pathology
Neurology
Phenotype
Predictive Value of Tests
Puberty - physiology
Recurrence
Remission, Spontaneous
Severity of Illness Index
Puberty
Nervous system diseases
Phenotype
Nuclear magnetic resonance imaging
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Summary:Multiple sclerosis (MS) onset before puberty may have a distinct clinical presentation. Pediatric patients with MS may less often meet MRI diagnostic criteria for adults. Whether initial MRI presentation is distinct in prepubertal patients is unknown. We queried the UCSF MS database for pediatric patients with MS (onset <or=18 years) who underwent brain MRI within 3 months of initial symptoms. The overall number of lesions and the number of well-defined and ovoid, large, confluent, and gadolinium-enhancing lesions were compared between patients with earlier-onset (EOPMS) (<11 years) and later-onset (LOPMS) (>or=11 years) pediatric MS. The next available brain MRI scan was used to evaluate lesion resolution. Thirteen children with EOPMS (median age 8.90 years, range [3.58-10.98], 38% girls) and 18 with LOPMS (median age 14.47 years, range [11.78-18.00], 61% girls) were identified. While the overall number of T2-bright lesions was similar in the two groups, patients with EOPMS had fewer well-defined ovoid T2-bright lesions (median = 7, range [0-29] vs 21.5, [4-100]; p = 0.004) and more often had confluent lesions (31% of patients vs 0%; p = 0.02) on their first MRI compared with patients with LOPMS. Ninety-two percent of patients with EOPMS had a reduction in the number of T2-bright lesions on the second scan compared to 29% of patients with LOPMS (p = 0.002). The distinct prepubertal multiple sclerosis (MS) MRI phenotype suggests that underlying biologic processes may differ in earlier-onset pediatric MS compared to later-onset pediatric MS. These findings may delay diagnosis in that age range. MRI criteria for MS diagnosis may need to be revised before puberty.
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ISSN:0028-3878
1526-632X
DOI:10.1212/01.wnl.0000326896.66714.ae