A multicenter comparison of MOG-IgG cell-based assays

Waters, Patrick; Komorowski, Lars; Woodhall, Mark; Lederer, Sabine; Majed, Masoud; Fryer, Jim; Mills, John R.; Flanagan, Eoin P.; Irani, Sarosh R.; Kunchok, Amy; McKeon, Andrew

doi:10.1212/wnl.0000000000007096

Cited by 135 publications

(172 citation statements)

References 10 publications

Supporting

Mentioning

161

Contrasting

Unclassified

Order By: Relevance

“…Overall, the median age of the patients at disease onset was 28 years, and the median disease duration at serum sampling was 11.5 years. Only 2 patients (0.03%) had MOG antibodies, consistent with the antibody specificity reported in previous studies, 9,10 although the current study included different subtypes of MS. Besides noting the high specificity of the methods used, the authors conclude that in clinical practice, patients fulfilling the 2010 McDonald criteria of MS (with typical features) do not need MOG antibody testing.…”

supporting

confidence: 91%

How DIRS is refining concepts

Dalmau

2020

Neurol Neuroimmunol Neuroinflamm

View full text Add to dashboard Cite

Like the elaboration of good wine, which is dependent on excellent materials, well-honed techniques, and the passage of time, the evolution of our understanding of diseases and syndromes is dependent on similar features. The recognition of many neuroimmunologic diseases associated with autoantibodies is relatively recent. With time and experience (e.g., more patients and controls), concepts about disease mechanisms or even the syndromes associated with some autoantibodies are being refined or manifest the need for an extensive redefinition. In the current issue of N2, we have some articles on this theme.

show abstract

supporting

confidence: 91%

How DIRS is refining concepts

Dalmau

2020

Neurol Neuroimmunol Neuroinflamm

View full text Add to dashboard Cite

show abstract

“…A recent large study of MOG antibodies in MS showed it is detected in only 0.2%, highlighting its utility in discriminating from MS [8]. While in our study we used two sites for MOG-IgG detection, our multi-center collaborative studies have shown the live-cell based MOG assay cut-offs show consistent results across centers for a non-MS phenotype [77]. The frequency of MOG-IgG and AQP4-IgG coexistence was reported at 0.06% which suggests a distinct immunopathogenesis to MOGAD and AQP4-IgG seropositive NMOSD, rather than MOG-IgG representing an epiphenomenon [37].…”

Section: Discussionmentioning

confidence: 67%

The pathology of central nervous system inflammatory demyelinating disease accompanying myelin oligodendrocyte glycoprotein autoantibody

et al. 2020

Self Cite

View full text Add to dashboard Cite

We sought to define the pathological features of myelin oligodendrocyte glycoprotein (MOG) antibody associated disorders (MOGAD) in an archival autopsy/biopsy cohort. We histopathologically analyzed 2 autopsies and 22 brain biopsies from patients with CNS inflammatory demyelinating diseases seropositive for MOG-antibody by live-cell-based-assay with full length MOG in its conformational form. MOGAD autopsies (ages 52 and 67) demonstrate the full spectrum of histopathological features observed within the 22 brain biopsies (median age, 10 years; range, 1-66; 56% female). Clinical, radiologic, and laboratory characteristics and course (78% relapsing) are consistent with MOGAD. MOGAD pathology is dominated by coexistence of both perivenous and confluent white matter demyelination, with an over-representation of intracortical demyelinated lesions compared to typical MS. Radially expanding confluent slowly expanding smoldering lesions in the white matter as seen in MS, are not present. A CD4+ T-cell dominated inflammatory reaction with granulocytic infiltration predominates. Complement deposition is present in all active white matter lesions, but a preferential loss of MOG is not observed. AQP4 is preserved, with absence of dystrophic astrocytes, and variable oligodendrocyte and axonal destruction. MOGAD is pathologically distinguished from AQP4-IgG seropositive NMOSD, but shares some overlapping features with both MS and ADEM, suggesting a transitional pathology. Complement deposition in the absence of selective MOG protein loss suggest humoral mechanisms are involved, however argue against endocytic internalization of the MOG antigen. Parallels with MOG-EAE suggest MOG may be an amplification factor that augments CNS demyelination, possibly via complement mediated destruction of myelin or ADCC phagocytosis.

show abstract

“…Recently, a commercial CBA for MOG-Abs detection relying on fixed cells has become available. In a three-center comparison, the fixed CBA showed rather good concordance with the live CBAs, with slightly lower specificity (30).…”

Section: Background Of the Assaymentioning

confidence: 89%

Autoantibody Diagnostics in Neuroimmunology: Experience From the 2018 Italian Neuroimmunology Association External Quality Assessment Program

et al. 2020

View full text Add to dashboard Cite

Results: Three-quarter of the tests were commercial. Median accuracy for the laboratories was 75% (range 50-100). In 8/10 schemes, at least one sample provided discrepant results. Inter-laboratory "substantial agreement" was found in 6/10 schemes (AChR, MuSK, MAG, AQP4, MOG, and NS-Abs), whereas the worst agreements regarded OCBs and ganglioside-Abs. Both commercial and in-house assays performed better in experienced laboratories.Conclusions: Assays could be divided in (a) robust commercial tests with substantial inter-laboratory agreement (MAG-Abs; AChR-and MuSK-Abs); commercial/"in-house" tests with (b) partial inter-laboratory agreement (AQP4-Abs, MOG-Abs, NS-Abs, Gastaldi et al.AINI 2018 EQA Program ICN-Abs), and (c) with large inter-laboratory disagreement (OCBs, ganglioside-Abs). This real-life snapshot of the neuroimmunology test performances highlights shortcomings attributable to technician-dependent performances, assay structural limitations, and errors in test interpretations.

show abstract

A multicenter comparison of MOG-IgG cell-based assays

Cited by 135 publications

References 10 publications

How DIRS is refining concepts

How DIRS is refining concepts

The pathology of central nervous system inflammatory demyelinating disease accompanying myelin oligodendrocyte glycoprotein autoantibody

Autoantibody Diagnostics in Neuroimmunology: Experience From the 2018 Italian Neuroimmunology Association External Quality Assessment Program

Contact Info

Product

Resources

About