TY - JOUR
T1 - CASPR2-IgG-associated autoimmune seizures
AU - Garrido Sanabria, Emilio R.
AU - Zahid, Anza
AU - Britton, Jeffrey William
AU - Kraus, Gregory J.
AU - López-Chiriboga, Alfonso Sebastian
AU - Zekeridou, Anastasia
AU - Flanagan, Eoin P.
AU - McKeon, Andrew
AU - Mills, John R.
AU - Pittock, Sean J.
AU - Dubey, Divyanshu
N1 - Funding Information:
J.B. is a consultant for UCB Pharmaceuticals (investigational drug discussion, rozanolixizumab); a coinvestigator, unpaid, for GW Pharma in a double‐blind, randomized, placebo‐controlled study to investigate the efficacy and safety of cannabidiol (GWP42003‐P) as add‐on therapy in patients with tuberous sclerosis complex who experience inadequately controlled seizures; and a coinvestigator, unpaid, for Grifols Pharmaceuticals in "A Randomized Double‐Blind Placebo Controlled Study of IVIG in Patients With Voltage‐Gated Potassium Channel Complex Antibody Associated Autoimmune Epilepsy." A.M. has a patent pending for KLHL11, septin 5, and MAP1B as markers of neurologic autoimmunity and paraneoplastic disorders. E.P.F. is a site principal investigator in a randomized placebo‐controlled clinical trial of inebilizumab (a cluster of differentiation 19 inhibitor) in neuromyelitis optica spectrum disorders funded by MedImmune/Viela Bio and receives research funding from the National Institutes of Health, National Institute of Neurologic Disorders and Stroke (R01NS113828). S.J.P. is a named inventor on filed patents that relate to functional AQP4/NMO‐IgG assays and NMO‐IgG as a cancer marker; has a patent pending for KLHL11‐IgG, septin 5, and MAP1B IgGs as markers of neurologic autoimmunity and paraneoplastic disorders; has consulted for Alexion and Medimmune; and has received research support from Grifols, Medimmune, and Alexion. All compensation for consulting activities is paid directly to Mayo Clinic. A.Ze. has a patent on PDE10A‐IgG as a biomarker of neurological autoimmunity. D.D. has received research support from Center of Individualized Medicine Welch Award, and Grifols Pharmaceuticals. He has consulted for UCB, Immunovant, and Astellas Pharmaceuticals. All compensation for consulting activities is paid directly to Mayo Clinic. D.D. has a patents pending for KLHL11 and LUZP4 as markers of neurological autoimmunity. None of the other authors has any conflict of interest to disclose.
Publisher Copyright:
© 2022 International League Against Epilepsy.
PY - 2022/3
Y1 - 2022/3
N2 - Objective: This study was undertaken to report clinical presentations and outcomes of CASPR2-IgG-associated seizures. Methods: Mayo Clinic Neuroimmunology database was queried to identify CASPR2-IgG-seropositive (CASPR2-IgG+) patients evaluated at our institution (2009–2019). Results: Of the 53 CASPR2-IgG+ patients (titer ≥ 1:10), 20 had seizures (38%). All seizure patients were male, with median onset age of 68 years. Eighteen (90%) had seizures at initial presentation. One patient was found to have malignancy (colon adenocarcinoma). Two patients had coexisting LGI1-IgG. Twelve patients had archived sera, which on titration had CASPR2-IgG titers ≥ 1:100. Fifteen patients (75%) met criteria for autoimmune encephalitis. Patients most commonly presented with focal onset, nonmotor seizures with impaired awareness (n = 14, 70%). Eleven patients also had focal motor and/or sensory seizures as one of the seizure semiologies. The majority of patients (n = 11, 55%) developed generalized tonic–clonic seizures during their disease course. Seizure clusters occurred in 12 patients. In addition to seizures, patients developed cognitive disturbance (n = 16, 80%), episodic emotional lability (n = 13, 65%), paroxysmal dizziness (n = 9, 45%), episodic ataxia (n = 6, 30%), and chronic ataxia (n = 9, 45%). Only three patients (15%) had coexisting peripheral nervous system involvement. Frontotemporal or temporal ictal and/or interictal electroencephalographic abnormalities were present among nine patients, and three had multifocal epileptiform abnormalities. Eight patients (40%) had medial temporal T2/fluid-attenuated inversion recovery hyperintensity on brain magnetic resonance imaging. Elevated cerebrospinal fluid protein and/or lymphocytic pleocytosis was present in most cases (13/14, 93%). Thirteen patients reached seizure freedom following initiation of antiseizure medication (ASM; n = 4) or a combination of immunotherapy and ASM (n = 9). Median duration of follow-up was 25 months (range = 2–136 months). Significance: CASPR2-IgG evaluation should be considered among older male patients with new onset focal seizures and impaired awareness often occurring in clusters with/without features of encephalitis. Coexisting neurological manifestations, including episodic emotional lability, ataxia, and paroxysmal dizziness, also aid in the diagnosis.
AB - Objective: This study was undertaken to report clinical presentations and outcomes of CASPR2-IgG-associated seizures. Methods: Mayo Clinic Neuroimmunology database was queried to identify CASPR2-IgG-seropositive (CASPR2-IgG+) patients evaluated at our institution (2009–2019). Results: Of the 53 CASPR2-IgG+ patients (titer ≥ 1:10), 20 had seizures (38%). All seizure patients were male, with median onset age of 68 years. Eighteen (90%) had seizures at initial presentation. One patient was found to have malignancy (colon adenocarcinoma). Two patients had coexisting LGI1-IgG. Twelve patients had archived sera, which on titration had CASPR2-IgG titers ≥ 1:100. Fifteen patients (75%) met criteria for autoimmune encephalitis. Patients most commonly presented with focal onset, nonmotor seizures with impaired awareness (n = 14, 70%). Eleven patients also had focal motor and/or sensory seizures as one of the seizure semiologies. The majority of patients (n = 11, 55%) developed generalized tonic–clonic seizures during their disease course. Seizure clusters occurred in 12 patients. In addition to seizures, patients developed cognitive disturbance (n = 16, 80%), episodic emotional lability (n = 13, 65%), paroxysmal dizziness (n = 9, 45%), episodic ataxia (n = 6, 30%), and chronic ataxia (n = 9, 45%). Only three patients (15%) had coexisting peripheral nervous system involvement. Frontotemporal or temporal ictal and/or interictal electroencephalographic abnormalities were present among nine patients, and three had multifocal epileptiform abnormalities. Eight patients (40%) had medial temporal T2/fluid-attenuated inversion recovery hyperintensity on brain magnetic resonance imaging. Elevated cerebrospinal fluid protein and/or lymphocytic pleocytosis was present in most cases (13/14, 93%). Thirteen patients reached seizure freedom following initiation of antiseizure medication (ASM; n = 4) or a combination of immunotherapy and ASM (n = 9). Median duration of follow-up was 25 months (range = 2–136 months). Significance: CASPR2-IgG evaluation should be considered among older male patients with new onset focal seizures and impaired awareness often occurring in clusters with/without features of encephalitis. Coexisting neurological manifestations, including episodic emotional lability, ataxia, and paroxysmal dizziness, also aid in the diagnosis.
KW - autoimmune encephalitis
KW - drug-resistant epilepsy
KW - emotional lability
KW - immunotherapy
UR - http://www.scopus.com/inward/record.url?scp=85122726336&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=85122726336&partnerID=8YFLogxK
U2 - 10.1111/epi.17164
DO - 10.1111/epi.17164
M3 - Article
C2 - 35032032
AN - SCOPUS:85122726336
SN - 0013-9580
VL - 63
SP - 709
EP - 722
JO - Epilepsia
JF - Epilepsia
IS - 3
ER -