Erschienen in:
23.04.2019 | Original Communication
Pathologic and MRI analysis in acute atypical inflammatory demyelinating lesions
verfasst von:
Xavier Ayrignac, Valérie Rigau, Benoit Lhermitte, Thierry Vincent, Nicolas Menjot de Champfleur, Clarisse Carra-Dalliere, Mahmoud Charif, Nicolas Collongues, Jérôme de Seze, Sonia Hebbadj, Guido Ahle, Hélène Oesterlé, François Cotton, Françoise Durand-Dubief, Romain Marignier, Sandra Vukusic, Frédéric Taithe, Mikael Cohen, Anne-Marie Guennoc, Anne Kerbrat, Gilles Edan, Béatrice Carsin-Nicol, Thibaut Allou, Denis Sablot, Eric Thouvenot, Aurélie Ruet, Laurent Magy, Marie-Paule Boncoeur-Martel, Pierre Labauge, Stéphane Kremer
Erschienen in:
Journal of Neurology
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Ausgabe 7/2019
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Abstract
Background
The diagnosis of atypical inflammatory demyelinating lesions can be difficult. Brain biopsy is often required to exclude neoplasms. Moreover, the relationship between these lesions and multiple sclerosis and NMOSD is not clear.
Objectives
Our objectives were to describe radiological and pathological characteristics of patients with acute inflammatory demyelinating lesions.
Methods
We retrospectively identified patients with brain biopsy performed for diagnostic uncertainty revealing a demyelinating lesion. A complete clinical, biological, radiological and pathological analysis was performed.
Results
Twenty patients (15 with a single lesion) were included. MRI disclosed a wide range of lesions including infiltrative lesions (40%), ring-like lesion (15%) Baló-like lesion (15%) and acute haemorrhagic leukoencephalitis (20%). In spite of a marked heterogeneity, some findings were common: a peripheral B1000 hyperintense rim (70%), a slight oedema with mild mass effect (75%) and an open-rim peripheral enhancement (75%). Histopathology revealed that all cases featured macrophages distributed throughout, extensive demyelination, axonal preservation and absence of haemorrhagic changes. In the majority of cases, macrophages were the predominant inflammatory infiltrate and astrocytes were reactive and dystrophic. Aquaporin-4 staining was systematically preserved. After a mean follow-up of 5 years (1–12), 16/20 patients had a diagnosis of monophasic acute atypical inflammatory demyelinating lesion. One patient was diagnosed with MS and 3 with AQP4 negative NMOSD.
Discussion
Although imaging findings in patients with atypical inflammatory demyelinating lesions are heterogeneous, some common features such as peripheral DWI hyperintense rim with open-rim enhancement and absence of oedema argue in favour of a demyelinating lesion and should preclude a brain biopsy. In this context, AQP4 staining is systematically preserved and argues against an AQP4-positive NMOSD. Moreover, long-term follow-up is characterized by low recurrence rate.