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ASNR 53rd Annual Meeting, Chicago, April 25-30, 2015
EP-144 Pediatric brain MRI: Is axial T2-weighted imaging enough for a diagnosis? Matthias W. Wagner ¹, Marinos Kontzialis ¹, Daniel Seeburg ¹, Steven E. Stern 2, Alexander Oshmyansky 1,2, Andrea Poretti ¹, Thierry A.G.M. Huisman ¹ ¹Section of Pediatric Neuroradiology, Division of Pediatric Radiology, Russell H. Morgan Department of Radiology and Radiological Science, The Johns Hopkins University School of Medicine, Baltimore, MD, USA; ²School of Mathematical Sciences, Faculty of Science and Engineering, Queensland University of Technology, Brisbane, QLD, Australia ASNR 53rd Annual Meeting, Chicago, April 25-30, 2015
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Disclosure We have nothing to disclose
No relevant financial relations interfering with the presentation
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Introduction ↑ financial constraints in health care need for rapid imaging protocols Our experience: T2w images most helpful in children: ↑ water content of pediatric brain ↑ signal/noise + contrast/noise ratio ↑ anatomical resolution + ↑ high sensitivity for many pediatric brain diseases Consequently: T2w images ↑ potential for an initial screening tool in pediatric neuroradiology
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Purpose To determine the sensitivity and specificity of axial T2 weighted images in the evaluation of pediatric brain MRI studies versus Axial T2 Full study
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Inclusion criteria Age at MRI < 18 years
Consecutively acquired head MRIs at the Johns Hopkins Hospital only Studies with final diagnoses confirmed by neuroimaging, laboratory tests, genetic analysis, and/or pathology
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Methods 1 Evaluation of axial T2 weighted images alone
first diagnosis noted Without time lapse: Evaluation of the full study second diagnosis noted Diagnoses noted as “normal” or “abnormal” Calculation of sensitivity and specificity for abnormal studies
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Methods 2 Standard of reference: final report of neuroradiology attendings as available in the PACS Three readers with different levels of experience Reader 1: 20 years pediatric neuroradiology Reader 2: neuroradiology fellow Reader 3: 4th year radiology resident Readers were blinded for clinical diagnoses and study indication 161 children (6 children scanned twice) 167 studies per reader
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Results 1 Mean age of children: 7.44 ± 5.71 years
Standard of reference: 91 studies “abnormal” 76 studies “normal” Normal study: absence of any pathology except sinus / mastoid effusion
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Results 2 <0.001 All readers T2 Full study p-Value Specificity
92.1% 90.4% 0.343 Sensitivity 83.2% 92.3% <0.001 NPV 82.0% 90.7% PPV 92.7% 92.0%
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Results 3 Individually T2 Full study p-Value 0.041 0.013 0.003
Reader 1 (20 years) Specificity 92.1% 93.4% 1.00 Sensitivity 87.9% 94.5% 0.041 NPV 86.4% PPV 93.0% Reader 2 (2 years) 84.6% 0.013 83.3% 92.8% Reader 3 (4th year resident) 85.5% 0.131 76.9% 89.0% 0.003 86.7% 88.0%
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Results 4 3 groups of false negative studies:
Group 1: lack of an additional plane Sagittal: Chiari 1 / hypoplastic corpus callosum Group 2: lack of additional sequences DWI: acute stroke SWI/T2*: blood products Group 3: limited reader experience
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False negatives on axial T2 Group 1: additional plane
Chiari malformation type 1 Axial T2w “Unremarkable” Sagittal T1w Tonsillar herniation
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False negatives on axial T2 Group 2: additional sequences
Hemorrhagic diffuse axonal injury Axial T2w Unremarkable Axial T2*w Hypointense lesions
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False negatives on axial T2 Group 3: reader experience
Axial T2w: moyamoya disease Axial T2w: systemic lupus with cerebral atrophy
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Results 5 Classification of 14 clinical indications in 2 groups:
Group 1: acute clinical findings potentially immediate consequences for patient care Group 2: non-acute clinical indications 4 false negative diagnoses in Group 1 (acute stroke, diffuse axonal injury, intraaxial hemorrhage) 2 non-acute clinical indications without misread on axial T2-screening (including >1 study): Question of malformation Follow-up for hypoxic-ischemic encephalopathy (HIE)
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Studies divided by indication
Number of studies False negative studies on axial T2 only Reader 1 Reader 2 Reader 3 Group 1: Acute clinical indication 19 1. Question of stroke 8 1 2. Question of tumor 7 3. Trauma 4 3 2 Group 2: Non-acute clinical indication 148 4. Non-acute neurological findings 34 5. Tumor follow-up 26 6. Seizure correlate 7. Question of malformation 18 8. Malformation follow-up 9. Phakomatosis follow-up 12 10. Developmental delay 11 11. HIE follow-up 12. Infectious disease follow-up 13. Question of phakomatosis 14. Stroke follow-up
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Conclusion 1 1a. Axial T2-weighted images alone can identify abnormal studies with high reliability 1b. High level of experience further increases sensitivity and specificity
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Conclusion 2 2a. False negative results make introduction of solitary axial T2-screening currently unfeasible 2b. Additional DWI + SWI sequences to a 3D- T2w sequence: ↑ imaging time, but still faster than standard protocols possible new screening tool in children with neurologic symptoms (as alternative to CT)
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