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September 29, 2015; 85 (13) Article

Early-onset bilateral cerebral arteriopathies

Cohort study of phenotype and disease course

Amina Al-Yassin, Dawn E. Saunders, Mark T. Mackay, Vijeya Ganesan
First published August 28, 2015, DOI: https://doi.org/10.1212/WNL.0000000000001969
Amina Al-Yassin
From the Neurosciences Unit (A.A.-Y., V.G.), UCL Institute of Child Health; the Radiology Department (D.E.S.), Great Ormond Street Hospital, NHS Foundation Trust, London, UK; and the Neurology Department (M.T.M.), Royal Children's Hospital, Melbourne, Australia.
MA, MBBS
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Dawn E. Saunders
From the Neurosciences Unit (A.A.-Y., V.G.), UCL Institute of Child Health; the Radiology Department (D.E.S.), Great Ormond Street Hospital, NHS Foundation Trust, London, UK; and the Neurology Department (M.T.M.), Royal Children's Hospital, Melbourne, Australia.
MD, MRCP, FRCR
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Mark T. Mackay
From the Neurosciences Unit (A.A.-Y., V.G.), UCL Institute of Child Health; the Radiology Department (D.E.S.), Great Ormond Street Hospital, NHS Foundation Trust, London, UK; and the Neurology Department (M.T.M.), Royal Children's Hospital, Melbourne, Australia.
MBBS
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Vijeya Ganesan
From the Neurosciences Unit (A.A.-Y., V.G.), UCL Institute of Child Health; the Radiology Department (D.E.S.), Great Ormond Street Hospital, NHS Foundation Trust, London, UK; and the Neurology Department (M.T.M.), Royal Children's Hospital, Melbourne, Australia.
MD
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Citation
Early-onset bilateral cerebral arteriopathies
Cohort study of phenotype and disease course
Amina Al-Yassin, Dawn E. Saunders, Mark T. Mackay, Vijeya Ganesan
Neurology Sep 2015, 85 (13) 1146-1153; DOI: 10.1212/WNL.0000000000001969

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Abstract

Objective: To describe characteristics of young children with arterial ischemic stroke (AIS) and bilateral cerebral arteriopathies.

Methods: Retrospective review of clinical features, course, and outcome. Neuroimaging was analyzed for infarct pattern, cerebrovascular diagnosis (anatomic/Childhood Arterial Ischemic Stroke Standardized Classification and Diagnostic Evaluation [CASCADE] criteria), and disease progression.

Results: In the 31 children (median age, 18 months), presentations included acute hemiparesis (n = 23) and focal seizures (n = 12). Seven had systemic arterial disease; 13 had cardiac abnormalities. Twenty had recurrent AIS or transient ischemic attack (after median of 3 months); 16 had >1 recurrence. Median modified Rankin Scale score was 3, with motor impairments in 20, cognitive impairments in 11, and seizures in 7. At presentation, 17 had old and acute infarcts. Twenty-five had high signal in white matter. A total of 13/23 reimaged patients accrued further infarcts over a median of 39 months. Arteriopathy involved the carotid circulation bilaterally in all; 6 had posterior circulation and 11 had extracranial involvement. Arteriopathy distribution was symmetric in 24/31. CASCADE categories were 3A in 19, 3B in 5, 3C in 5, and 7 in 2. After a median of 35 months, 14 had had progression of arteriopathy. Patients categorized as CASCADE 3A (moyamoya) had significantly shorter time to recurrence than other groups.

Conclusion: Young children with bilateral cerebral arteriopathies (particularly meeting criteria for CASCADE 3A) have a malignant course, with frequent recurrent events, progressive disease, and poor outcomes. Current classifications are limited in characterizing disease in many cases. Symmetric involvement suggests these arteriopathies may be developmentally determined, while systemic involvement suggests potential genetic etiology.

GLOSSARY

ACA=
anterior cerebral artery;
AIS=
arterial ischemic stroke;
BA=
basilar artery;
CA=
catheter angiography;
CASCADE=
Childhood Arterial Ischemic Stroke Standardized Classification and Diagnostic Evaluation;
CCA=
common carotid artery;
CI=
confidence interval;
CTA=
CT angiography;
EC-IC=
external to internal carotid;
ECA=
external carotid artery;
ICA=
internal carotid artery;
MCA=
middle cerebral artery;
MM=
moyamoya;
MRA=
magnetic resonance angiogram;
mRS=
modified Rankin Scale;
PHACES=
posterior fossa malformations, hemangiomas, arterial anomalies, cardiac defects, eye abnormalities, sternal cleft, and supraumbilical raphe syndrome

Footnotes

  • Go to Neurology.org for full disclosures. Funding information and disclosures deemed relevant by the authors, if any, are provided at the end of the article.

  • Supplemental data at Neurology.org

  • Received January 1, 2015.
  • Accepted in final form April 16, 2015.
  • © 2015 American Academy of Neurology
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