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Novel Autoantibody Against DAGLA Discovered in Cerebellitis

By LabMedica International staff writers
Posted on 17 Apr 2025

Autoimmune cerebellar ataxias are strongly disabling disorders characterized by an impaired ability to coordinate muscle movement. Cerebellar autoantibodies serve as useful biomarkers to support rapid disease diagnosis, but in many cases the autoantibody target has not yet been identified. Now, researchers have identified diacylglycerol lipase alpha (DAGLA) as a novel autoantibody target in patients with rapid progressive cerebellar ataxia.

The autoantibodies were characterized as part of a collaborative study between scientists at EUROIMMUN (Lübeck, Germany), the Hannover Medical School (Hannover, Germany and collaborative institutes and clinics. In this study published in the journal Neurology, Neurosurgery & Psychiatry, DAGLA was identified as the autoantibody target in four young patients aged 18 to 34, who suffered from pronounced gait ataxia, dysarthria and visual impairments. In three of the four patients, severe cerebellar atrophy developed within 6 months. None of the patients had a malignancy. To identify the antigen, serum and cerebrospinal fluid (CSF) from the four index patients were subjected to comprehensive autoantibody screening by indirect immunofluorescence assays (IIFA). The four patients’ samples all showed a characteristic IgG reactivity with the molecular layer of cerebellum cryosections.


Image: Anti-DAGLA antibodies in cerebellitis (Photo courtesy of EUROIMMUN)
Image: Anti-DAGLA antibodies in cerebellitis (Photo courtesy of EUROIMMUN)

The autoantibodies bound exclusively to the dendrites of the Purkinje cells, whereas the somata remained unstained. Immunoprecipitation and mass spectrometry were used to identify the target antigen. Results were confirmed by competitive inhibition experiments and recombinant-cell (RC) IIFA based on transfected HEK293 cells expressing DAGLA. Sera and CSF from the index patients reacted strongly positive in the anti-DAGLA RC-IIFA, whereas the control cells did not demonstrate any specific antibody binding. Sera from 101 patients with various neurological symptoms and sera from 102 healthy blood donors were additionally analyzed using the anti-DAGLA RC-IIFA. Serum reactivity against DAGLA was found in 17 disease controls and 1 healthy donor.

Epitope characterization revealed that 17 of these 18 sera reacted with a linear intracellular epitope between amino acids 583 and 1042, whereas the CSF of the index patients targeted a conformational epitope between amino acids 1 and 157. These data indicate the existence of at least two subtypes of anti-DAGLA autoantibodies targeting distinct epitopes, which should be taken into consideration in the antibody detection. The proposed testing strategy comprises RC-IIFA using full-length DAGLA protein, with confirmation of positive results using RC-IIFA based on a DAGLA 1-582 fragment. The scientists concluded that anti-DAGLA autoantibodies detected in CSF with a characteristic tissue IIFA pattern represent novel biomarkers for rapidly progressing cerebellitis. They surmised that earlier diagnosis of the associated neurological disorder followed by more aggressive and prolonged immunotherapy could inhibit dramatic disease progression.


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