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Research ArticlePediatric Neuroimaging

Imaging Findings and MRI Patterns in a Cohort of 18q Chromosomal Abnormalities

Prateek Malik, Helen Branson, Grace Yoon, Manohar Shroff, Susan Blaser and Pradeep Krishnan
American Journal of Neuroradiology October 2024, 45 (10) 1578-1585; DOI: https://doi.org/10.3174/ajnr.A8361
Prateek Malik
aFrom the Department of Diagnostic Imaging (P.M., H.B., M.S., S.B., P.K.), The Hospital for Sick Children, Toronto, Canada.
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Helen Branson
aFrom the Department of Diagnostic Imaging (P.M., H.B., M.S., S.B., P.K.), The Hospital for Sick Children, Toronto, Canada.
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Grace Yoon
bDivision of Clinical and Metabolic Genetics (G.Y.), The Hospital for Sick Children, Toronto, Canada.
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Manohar Shroff
aFrom the Department of Diagnostic Imaging (P.M., H.B., M.S., S.B., P.K.), The Hospital for Sick Children, Toronto, Canada.
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Susan Blaser
aFrom the Department of Diagnostic Imaging (P.M., H.B., M.S., S.B., P.K.), The Hospital for Sick Children, Toronto, Canada.
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Pradeep Krishnan
aFrom the Department of Diagnostic Imaging (P.M., H.B., M.S., S.B., P.K.), The Hospital for Sick Children, Toronto, Canada.
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Abstract

BACKGROUND AND PURPOSE: The abnormalities of the long arm of chromosome 18 (18q) constitute a complex spectrum. We aimed to systematically analyze their MR imaging features. We hypothesized that there would be variable but recognizable white matter and structural patterns in this cohort.

MATERIALS AND METHODS: In this retrospective cohort study, we included pediatric patients with a proved abnormality of 18q between 2000–2022. An age- and sex-matched control cohort was also constructed.

RESULTS: Thirty-six cases, median MR imaging age 19.6 months (4.3–59.3), satisfied our inclusion criteria. Most were female (25, 69%, F:M ratio 2.2:1). Fifty MR imaging studies were analyzed, and 35 (70%) had delayed myelination. Two independent readers scored brain myelination with excellent interrater reliability. Three recognizable evolving MR imaging patterns with distinct age distributions and improving myelination scores were identified: Pelizaeus-Merzbacher disease–like (9.9 months, 37), intermediate (22 months, 48), and washed-out pattern (113.6 months, 53). Etiologically, MRIs were analyzed across 3 subgroups: 18q deletion (34, 69%), trisomy 18 (10, 21%), and ring chromosome 18 (5, 10%). Ring chromosome 18 had the highest myelination lag (27, P = .005) and multifocal white matter changes (P = .001). Trisomy 18 had smaller pons and cerebellar dimensions (anteposterior diameter pons, P = .002; corpus callosum vermis, P < .001; and transverse cerebellar diameter, P = .04).

CONCLUSIONS: In this cohort of 18q chromosomal abnormalities, MR imaging revealed recognizable patterns correlating with improving brain myelination. Imaging findings appear to be on a continuum with more severe white matter abnormalities in ring chromosome 18 and greater prevalence of structural abnormalities of the pons and cerebellum in trisomy 18.

ABBREVIATIONS:

18q-
18q deletion
18q
long arm of chromosome 18
APD
anteroposterior diameter
CC
corpus callosum
CCD
craniocaudal diameter
FOD
fronto-occipital diameter
GWMD
gray-white matter differentiation
PMD
Pelizaeus-Merzbacher disease
TCD
transverse cerebellar diameter
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American Journal of Neuroradiology: 45 (10)
American Journal of Neuroradiology
Vol. 45, Issue 10
1 Oct 2024
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Cite this article
Prateek Malik, Helen Branson, Grace Yoon, Manohar Shroff, Susan Blaser, Pradeep Krishnan
Imaging Findings and MRI Patterns in a Cohort of 18q Chromosomal Abnormalities
American Journal of Neuroradiology Oct 2024, 45 (10) 1578-1585; DOI: 10.3174/ajnr.A8361

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MRI Patterns in 18q Chromosomal Abnormalities
Prateek Malik, Helen Branson, Grace Yoon, Manohar Shroff, Susan Blaser, Pradeep Krishnan
American Journal of Neuroradiology Oct 2024, 45 (10) 1578-1585; DOI: 10.3174/ajnr.A8361
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