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July 27, 2010; 75 (4) Articles

Familial neuromyelitis optica

M. Matiello, H.J. Kim, W. Kim, D.G. Brum, A.A. Barreira, D.J. Kingsbury, G.T. Plant, T. Adoni, B.G. Weinshenker
First published July 26, 2010, DOI: https://doi.org/10.1212/WNL.0b013e3181ea9f15
M. Matiello
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H.J. Kim
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W. Kim
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D.G. Brum
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A.A. Barreira
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D.J. Kingsbury
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G.T. Plant
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T. Adoni
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B.G. Weinshenker
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Citation
Familial neuromyelitis optica
M. Matiello, H.J. Kim, W. Kim, D.G. Brum, A.A. Barreira, D.J. Kingsbury, G.T. Plant, T. Adoni, B.G. Weinshenker
Neurology Jul 2010, 75 (4) 310-315; DOI: 10.1212/WNL.0b013e3181ea9f15

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Abstract

Background: Detection of aquaporin-4–specific immunoglobulin G (IgG) has expanded the spectrum of neuromyelitis optica (NMO). Rare reports of familial aggregation have suggested a component of genetic susceptibility but these reports mostly antedated the discovery of the NMO-IgG biomarker and recently updated diagnostic criteria.

Methods: We report a case series describing the demographic, clinical, neuroimaging, and NMO-IgG serologic status of 12 multiplex NMO pedigrees with a total of 25 affected individuals.

Results: Twenty-one patients (84%) were women. Families were Asian (n = 5), Latino (n = 4), white (n = 1), or African (n = 2). Apparent transmission was either maternal (n = 5) or paternal (n = 2). In 1 family, 3 individuals had NMO; in the others, 2 individuals were affected. Sibling pairs (n = 6), parent-child (n = 4), and aunt-niece (n = 3) pairs were observed. Nineteen patients (76%) were NMO-IgG positive. Twelve (48%) had clinical or serologic evidence of another autoimmune disease. Familial occurrence of NMO occurs in approximately 3% of patients with well-established diagnosis of NMO.

Conclusions: A small proportion of patients with NMO have relatives with this condition, but familial occurrence is more common than would be expected from its frequency in the general population. Familial NMO is indistinguishable from sporadic NMO based on clinical symptoms, age at onset, sex distribution, and frequency of NMO-IgG detection. One or 2 generations were affected and affected individuals represented a small fraction of family members. Taken together, these data suggest complex genetic susceptibility in NMO.

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  • Supplemental data at www.neurology.org

    Study funding: Supported by the Guthy-Jackson Charitable Foundation, National Multiple Sclerosis Society, and by the National Center for Research Resources (NCRR), a component of the National Institutes of Health (NIH), and the NIH Roadmap for Medical Research (NCRR 1 UL1 RR024150).

    Disclosure: Author disclosures are provided at the end of the article.

    Received December 8, 2009. Accepted in final form March 29, 2010.

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