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Towards a neuroimaging consensus for the workup of adult genetic leukoencephalopathies on behalf of the White Matter Rounds Network: State of Practice




TekijätWong, Alexander D.; Airas, Laura; Alvarez, Enrique; Antel, Jack; Araujo, David; Bernard, Geneviève; Boudjani, Hayet; Brais, Bernard; Cocozza, Sirio; Corboy, John R.; Fadda, Giulia; Imitola, Jaime; Lacasse, Marie-Constance; Longbrake, Erin E.; Macaron, Gabrielle; Narayanan, Sridar; Orthmann-Murphy, Jennifer; Ortiz, Jimenez Johanna; Shor, Natalia; Uggetti, Carla; Venkateswaran, Sunita; Wilson, Nagwa; Miller, Elka; La Piana, Roberta

KustantajaAmerican Society of Neuroradiology (ASNR)

Julkaisuvuosi2025

Lehti: American Journal of Neuroradiology

ISSN0195-6108

eISSN1936-959X

DOIhttps://doi.org/10.3174/ajnr.A9127

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Julkaisukanavan avoimuus Osittain avoin julkaisukanava

Verkko-osoitehttps://doi.org/10.3174/ajnr.a9127


Tiivistelmä

Adult-onset genetic leukoencephalopathies (AGL) are frequently misdiagnosed due to overlap with more common acquired white matter (WM) diseases. The WM Rounds Network includes clinicians/scientists from more than 15 centers around the world who meet monthly to discuss undiagnosed WM diseases. MRI remains a central tool in narrowing the differential diagnosis of WM diseases; however, a key barrier to optimizing diagnosis was the lack of protocol standardization between institutions. We aimed to 1. assess the state of practice of current protocols for investigating suspected AGLs and 2. propose a core standard protocol.

We used a modified Delphi method to facilitate group judgements. We developed a survey and submitted it for feedback to a panel of neuroimaging experts. The final survey was circulated to the entire WM Rounds Network. The results were analyzed, and specific recommendations were put forward during Delphi rounds, for which the stop criterion was >75% agreement.

The average summed sequence time of our MR protocols was 40 minutes (range 25-60) and included the following sequences: 3D T1 MPRAGE and 3D FLAIR obtained in the sagittal plane, axial T2 and T2-FLAIR, axial DWI/ADC, and axial SWI. Cervical and thoracic spine imaging (T1 sagittal, T2 sagittal and axial) were also frequently performed. A standardized core imaging protocol inclusive of the above-listed sequences would help harmonize sequence acquisition across institutions and promote cost-effective optimization of the imaging workup of AGLs. Four additional recommendations were proposed: 1) Contrast-enhanced T1 sequences should be performed for patients with demonstrable clinical or radiological evidence of AGL. 2) Lumbar MR spine imaging has limited utility. 3) Head CT is of little added value and should not be included routinely. 4) MRS, DTI, and other advanced imaging techniques are not yet ready to be implemented in the protocol but may be helpful in supporting a working diagnosis.


Julkaisussa olevat rahoitustiedot
Roberta La Piana has received a Research Scholar Junior 1 award from the Fonds de Recherche du Québec en Santé (FRQS), and research funds from the Canadian Radiological Foundation, Canadian Institutes of Health Research (grant 506913), Ataxia Canada, the Spastic Paraplegia Foundation and Roche Canada. Geneviève Bernard has received the Clinical Research Scholar Junior 1 Award from the FRQS (2012-2016), the New Investigator Salary Award from the CIHR (2017-2022), the Clinical Research Scholar Senior Award from the FRQS (2022-2025), and the Chercheur de Mérite Award from the FRQS (2025-2029). Laura Airas has obtained funding from the InFLAMES Flagship Program of the Research Council of Finland (Decision numbers: 337530, 357910 and 358823), US National MS Society (RFA-2203-39281) and Jane and Aatos Erkko Foundation. Fanny M. Elahi has received funding from National Institute on Aging and Department of Veterans Affair (IK2CX002180).


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