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Abstract Details

Radiographic Clues in Myelitis due to Neurosarcoidosis
Autoimmune Neurology
P8 - Poster Session 8 (11:45 AM-12:45 PM)
2-006

To identify radiographic clues in myelitis suggestive of neurosarcoidosis.

Inflammatory myelitis is challenging to differentiate during the acute evaluation, especially in those disorders lacking a biomarker. Understanding the specific radiographic abnormalities in myelitis from neurosarcoidosis may improve diagnosis.

Patients with biopsy-proven sarcoidosis with radiographic evidence of spinal cord parenchymal involvement were included. Those without images for review by the authors were excluded. 

Twenty-nine patients (21 males, 8 females; 22 Black, 6 white, 1 unknown; median age 45 years) were included. Myelitis was the initial manifestation of neurosarcoidosis in 27 (93.1%). A longitudinally-extensive lesion was observed on post-contrasted T1 in 12 (41.4%) and non-contrasted T2 in 25 (86.2%). The median lengths of the longest sagittal enhancing lesion and T2 hyperintensity were 2 (range 0.5-21) and 9.5 vertebral bodies (range 0.5-21), respectively. Enhancing lesions were present in 28 (96.6%) and located in the cervical (24, 82.8%), thoracic (16, 55.2%), and conus medullaris (6, 20.7%) segments. On T2, lesions were expansile in 26 (89.7%) and located axially in the anterolateral (23, 79.3%), lateral (19, 65.5%), and dorsal (26, 89.7%) columns and central canal (23, 79.3%). A partial or full enhancing trident sign was seen dorsally in 14 (48.3%) and ventrally in 4 (13.8%). Additional findings included leptomeningeal disease (10, 34.5%), cauda equina involvement (6, 20.7%), vertebral disease (3, 10.3%), and lymphadenopathy (9, 31.0%). On brain MRI, intracranial inflammation was present in 8/27 (29.6%) with involvement of the optic nerves (4/27, 14.8%), leptomeninges (3/27, 11.1%), and brain parenchyma (3/27, 11.1%) being most common.

MRI lesions are usually longer on sagittal T2 than post-contrasted T1-weighted imaging. They typically involve the subpial cord parenchyma with extension towards the central canal, producing a dorsal or ventral trident sign. Involvement of the leptomeninges and lymph nodes, unusual for demyelinating disorders, may support the diagnosis.

Authors/Disclosures
Evan Hoopingarner
PRESENTER
Mr. Hoopingarner has nothing to disclose.
Valerie Jeanneret Lopez, MD Dr. Jeanneret Lopez has nothing to disclose.
Diana Vargas, MD (Emory Healthcare) Dr. Vargas has nothing to disclose.
Spencer Hutto, MD (Emory University: Neurology Residency Program) Dr. Hutto has nothing to disclose.