Clinical and immunologic investigations in patients with stiff-person spectrum disorder

E Martinez-Hernandez; H Ariño; A McKeon; T Iizuka; M J Titulaer; M M Simabukuro; E Lancaster; M Petit-Pedrol; J Planagumà; Y Blanco; Robert J Harvey; A Saiz; F Graus; J Dalmau

doi:10.1001/jamaneurol.2016.0133

Back

Clinical and immunologic investigations in patients with stiff-person spectrum disorder

Journal article

Peer reviewed

Clinical and immunologic investigations in patients with stiff-person spectrum disorder

E Martinez-Hernandez, H Ariño, A McKeon, T Iizuka, M J Titulaer, M M Simabukuro, E Lancaster, M Petit-Pedrol, J Planagumà, Y Blanco, …

JAMA Neurology, Vol.73(6), pp.714-720

2016

DOI: https://doi.org/10.1001/jamaneurol.2016.0133

Files and links (1)

url

https://doi.org/10.1001/jamaneurol.2016.0133View

Published Version

Abstract

IMPORTANCE Symptoms of stiff-person syndrome (SPS), stiff-limb syndrome (SLS), or progressive encephalomyelitis with rigidity, myoclonus, or other symptoms (SPS-plus) can occur with several autoantibodies, but the relative frequency of each antibody, syndrome specificity, and prognostic implications are unclear. OBJECTIVE To report the clinical and immunologic findings of a large cohort of patients with stiff-person spectrum disorder (SPSD), including SPS, SLS, and SPS-plus. DESIGN, SETTING, AND PATIENTS This study retrospectively examined a case series (January 1, 1998, through December 31, 2014) of immunologic investigations performed in a neuroimmunology referral center. The study included 121 patients with clinical features of SPSD. Data analysis was performed from July 1, 2015, through November 1, 2015. MAIN OUTCOMES AND MEASURES Analysis of clinical-immunologic associations, including autoantibodies to 8 proteins expressed in inhibitory synapses. RESULTS The median age of the patients was 51 years (interquartile range, 40-61 years), and 75 (62.0%) were female. Fifty (41.3%) had SPS, 37 (30.6%) had SPS-plus, 24 (19.8%) had SLS, and 10 (8.3%) had SPS or SLS overlapping with ataxia, epilepsy, or encephalitis. Fifty-two patients (43.0%) had glutamic acid decarboxylase (GAD65) antibodies (2 with γ-aminobutyric acid-A [GABA-A] receptor antibodies), 24 (19.8%) had α1-subunit of the glycine receptor (GlyR) antibodies (2 with GAD65 antibodies), 5 (4.1%) had other antibodies, and 40 (33.1%) tested negative for antibodies. None had gephyrin or glycine transporter antibodies. Among the main immunologic groups (GAD65 antibodies, GlyR antibodies, and antibody negative), those with GAD65 antibodies were more likely to be female (45 [86.5%] of 52, 8 [36.4%] of 22, and 18 [45.0%] of 40, respectively; P < .001), have systemic autoimmunity (34 [65.4%] of 52, 7 [31.8%] of 22, and 13 [32.5%] of 40, respectively; P = .004), and have longer delays in being tested for antibodies (median, 3 vs 0.5 and 1 year; P < .001). Patients with GAD65 antibodies were more likely to develop SPS (27 [51.9%] of 52) or overlapping syndromes (8 [15.4%] of 52) than patients with GlyR antibodies (5 [22.7%] and 0 [0%] of 22, respectively), who more often developed SPS-plus (12 [54.5%] of 22 vs 7 [13.5%] in those with GAD65 antibodies); antibody-negative patients had an intermediate syndrome distribution. In multivariable analysis, symptom severity (P = .001) and immunologic group (P = .01) were independently associated with outcome. Compared with patients with GlyR antibodies, those with GAD65 antibodies (odds ratio, 11.1, 95%CI, 2.3-53.7; P = .003) had worse outcome. Patients without antibodies had similar outcome than patients with GlyR antibodies (odds ratio, 4.2, 95%CI, 0.9-20.0; P = .07). CONCLUSIONS AND RELEVANCE In SPSD, symptom severity and presence and type of antibodies are predictors of outcome. Copyright 2016 American Medical Association. All rights reserved.

Details

Title: Clinical and immunologic investigations in patients with stiff-person spectrum disorder
Authors: E Martinez-Hernandez (Author) - University of Barcelona, Spain
H Ariño (Author) - University of Barcelona, Spain
A McKeon (Author) - Mayo Clinic, United States
T Iizuka (Author) - Kitasato University, Japan
M J Titulaer (Author) - Erasmus Medical Centre, Netherlands
M M Simabukuro (Author) - Sao Paulo University, Brazil
E Lancaster (Author) - University of Pennsylvania, United States
M Petit-Pedrol (Author) - Institut d’Investigacions Biomèdiques August Pi i Sunyer, Spain
J Planagumà (Author) - Institut d’Investigacions Biomèdiques August Pi i Sunyer, Spain
Y Blanco (Author) - University of Barcelona, Spain
Robert J Harvey (Author) - University College London, United Kingdom
A Saiz (Author) - University of Barcelona, Spain
F Graus (Author) - University of Barcelona, Spain
J Dalmau (Author) - Institut d’Investigacions Biomèdiques August Pi i Sunyer, Spain
Publication details: JAMA Neurology, Vol.73(6), pp.714-720
Publisher: American Medical Association
Date published: 2016
DOI: 10.1001/jamaneurol.2016.0133
ISSN: 2168-6149
Organisation Unit: School of Health; University of the Sunshine Coast, Queensland; School of Health and Sport Sciences - Legacy; Centre for Bioinnovation; School of Health and Behavioural Sciences - Legacy
Language: English
Record Identifier: 99450524202621
Output Type: Journal article

Metrics

1 File views/ downloads

508 Record Views

128 Times Cited - Web of Science

See more details

InCites Highlights

These are selected metrics from InCites Benchmarking & Analytics tool, related to this output

Collaboration types: Domestic collaboration; International collaboration
Web Of Science research areas: Clinical Neurology

UN Sustainable Development Goals (SDGs)

This output has contributed to the advancement of the following goals:

Source: InCites