Cell‐surface central nervous system autoantibodies: Clinical relevance and emerging paradigms

Irani, Sarosh R.; Gelfand, Jeffrey M.; Al-Diwani, Adam; Vincent, Angela

doi:10.1002/ana.24200

Cited by 166 publications

(170 citation statements)

References 164 publications

(263 reference statements)

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“…In this study, we evaluated the rituximab responsiveness 1 month after the standard rituximab treatment, based tocilizumab group, at the time of monthly rituximab therapy initiation in the additional rituximab group, and at 1 month after the last cycle of weekly rituximab therapy in the observation group First-line = at initiation of first-line immunotherapies; RTX = at initiation of standardregimen weekly rituximab; RTX 1 mo = at 1 month from the initiation of weekly rituximab therapy; 1 mo = at 1 month from the baseline time points; 2 mo = at 2 months from the baseline time points; last FU = at the last clinical follow-up point on the fact that timely control of disease is essential to improve outcomes in AE [35], and that early discrimination of drug responsiveness is fundamental in the considering further treatment options. In this study, clinical improvement from standard-regimen rituximab was reported in 85/176 (48.3 %) patients [29/55 (52.7 %) for the anti-NMDA-R encephalitis subgroup].…”

Section: Discussionmentioning

confidence: 99%

Tocilizumab in Autoimmune Encephalitis Refractory to Rituximab: An Institutional Cohort Study

et al. 2016

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A considerable portion of autoimmune encephalitis (AE) does not respond to conventional immunotherapies and subsequently has poor outcomes. We aimed to determine the efficacy of tocilizumab, an anti-interleukin-6 antibody, in rituximab-refractory AE compared with other treatment options. From an institutional cohort of AE, 91 patients with inadequate clinical response to first-line immunotherapy and following rituximab were retrospectively reviewed. Patients were grouped according to their further immunotherapy strategies. Thirty (33.0 %) patients were included in the tocilizumab group, 31 (34.0 %) in the additional rituximab group, and 30 (33.0 %) in the observation group. Outcomes were defined as the favorable modified Rankin Scale scores (≤2) at 1 and 2 months from the initiation of each treatment strategy and at the last follow-up. Favorable clinical response (improvement of the modified Rankin Scale scores by ≥ 2 points or achievement of the mRS scores ≤ 2) at the last follow-up was also analyzed. The tocilizumab group showed more frequent favorable mRS scores at 2 months from treatment initiation and at the last follow-up compared with those at the relevant time points of the remaining groups. The majority (89.5 %) of the patients with clinical improvement at 1 month from tocilizumab treatment maintained a long-term favorable clinical response. No serious adverse effects of rituximab or tocilizumab were reported. Therefore, we suggest that tocilizumab might be a good treatment strategy for treating AE refractory to conventional immunotherapies and rituximab. The tocilizumab-mediated clinical improvement manifests as early at 1 month after treatment initiation.

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Section: Discussionmentioning

confidence: 99%

Tocilizumab in Autoimmune Encephalitis Refractory to Rituximab: An Institutional Cohort Study

et al. 2016

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“…Thus the frequency of the entire range of PNDs and neuronal antibodies in SCLC has not been determined systematically. Furthermore, with the recent discovery of a new category of disorder mediated by autoantibodies against neuronal cell surface proteins such as NMDA receptor and LGI1, 8 it is important to determine whether these antibodies are present in SCLC PNDs.…”

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confidence: 99%

Paraneoplastic neurologic disorders in small cell lung carcinoma

et al. 2015

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Objective: To determine the frequency and range of paraneoplastic neurologic disorders (PNDs) and neuronal antibodies in small cell lung carcinoma (SCLC).Methods: Two hundred sixty-four consecutive patients with biopsy-proven SCLC were recruited at the time of tumor diagnosis. All patients underwent full neurologic examination. Serum samples were taken prior to chemotherapy and analyzed for 15 neuronal antibodies. Thirty-eight healthy controls were analyzed in parallel.Results: PNDs were quite prevalent (n 5 24, 9.4%), most frequently Lambert-Eaton myasthenic syndrome (3.8%), sensory neuronopathy (1.9%), and limbic encephalitis (1.5%). Eighty-seven percent of all patients with PNDs had antibodies to SOX2 (62.5%), HuD (41.7%), or P/Q VGCC (50%), irrespective of their syndrome. Other neuronal antibodies were found at lower frequencies (GABAb receptor [12.5%] and N-type VGCC [20.8%]) or very rarely (GAD65, amphiphysin, Ri, CRMP5, Ma2, Yo, VGKC complex, CASPR2, LGI1, and NMDA receptor [all ,5%]). Conclusions:The spectrum of PNDs is broader and the frequency is higher than previously appreciated, and selected antibody tests (SOX2, HuD, VGCC) can help determine the presence of an SCLC. Neurology ® 2015;85:235-239 GLOSSARY HC 5 healthy control; LE 5 limbic encephalitis; LEMS 5 Lambert-Eaton myasthenic syndrome; PCD 5 paraneoplastic cerebellar degeneration; PEM 5 paraneoplastic encephalomyelitis; PND 5 paraneoplastic neurologic disorder; SCLC 5 small cell lung carcinoma; SN 5 sensory neuronopathy.A paraneoplastic neurologic disorder (PND) results from the indirect effect of a tumor on the nervous system or muscle without local invasion or metastasis. PNDs are often associated with antibodies that bind to proteins shared between the tumor and the nervous system.

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“…In adults, autoantibodies to essential neuronal proteins such as the N ‐methyl‐ d ‐aspartate receptor (NMDAR) and the voltage gated potassium channel (VGKC)‐complex antigen, leucine rich glioma inactivated 1 (leucine rich glioma inactivated 1 (LGI1), are now widely recognized as an important treatable cause of encephalitis 1, 2. Patients present with memory loss, confusion, and seizures in limbic encephalitis with predominantly LGI1 antibodies3, 4 and neuropsychiatric features, movement, and autonomic symptoms in NMDAR‐Ab (antibody) encephalitis 5, 6.…”

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Neuronal antibodies in pediatric epilepsy: Clinical features and long‐term outcomes of a historical cohort not treated with immunotherapy

et al. 2016

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SummaryObjectiveIn autoimmune encephalitis the etiologic role of neuronal cell‐surface antibodies is clear; patients diagnosed and treated early have better outcomes. Neuronal antibodies have also been described in patients with pediatric epilepsy without encephalitis. The aim was to assess whether antibody presence had any effect on long‐term outcomes in these patients.MethodsPatients (n = 178) were recruited between 1988 and 1992 as part of the prospective Dutch Study of Epilepsy in Childhood; none received immunotherapy. Healthy age‐matched bone‐marrow donors served as controls (n = 112). All sera were tested for serum N‐methyl‐d‐aspartate receptor (NMDAR), alpha amino‐3‐hydroxy‐5‐methyl‐4‐isoxazolepropionic acid receptor, leucine rich glioma inactivated 1, contactin associated protein like 2 (CASPR2), contactin‐2, glutamic acid decarboxylase, and voltage gated potassium channel (VGKC)‐complex antibodies by standard techniques. No cerebrospinal fluid (CSF) samples were available. Results were correlated with clinical data collected over 15 years.ResultsSeventeen patients (9.5%) were positive for VGKC complex (n = 3), NMDAR (n = 7), CASPR2 (n = 4), and contactin‐2 (n = 3), compared to three (3/112; 2.6%) healthy controls (VGKC complex [n = 1], NMDAR [n = 2]; p = 0.03; Fisher's exact test). Titers were relatively low (≤1:100 for cell‐surface antibodies), but 8 (47%) of the 17 positive samples bound to the surface of live hippocampal neurons consistent with a potential pathogenic antibody. Preexisting cognitive impairment was more frequent in antibody‐positive patients (9/17 vs. 33/161; p = 0.01). Fourteen antibody‐positive patients were treated with standard antiepileptic drugs (AEDs); three (17%) became intractable but this was not different from the 16 (10%) of 161 antibody‐negative patients. In 96 patients with available follow‐up samples at 6 and/or 12 months, 6 of 7 positive antibodies had disappeared and, conversely, antibodies had appeared for the first time in a further 7 patients.SignificanceNeuronal antibodies were found at low levels in 9.5% of patients with new‐onset pediatric epilepsy but did not necessarily persist over time, and the development of antibodies de novo in later samples suggests they could be due to a secondary response to neuronal damage or inflammation. Moreover, as the response to standard AEDs and the long‐term outcome did not differ from those of antibody‐negative pediatric patients, these findings suggest that routine neuronal antibody testing is unlikely to be helpful in pediatric epilepsy. However, the higher incidence of preexisting cognitive problems in the antibody‐positive group, the CASPR2 and contactin‐2 antibodies in 7 of 17 patients, and the binding of 8 of 17 of serum samples to live hippocampal neurons suggest that neuronal antibodies, even if secondary, could contribute to the comorbidities of pediatric epilepsy.

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Cell‐surface central nervous system autoantibodies: Clinical relevance and emerging paradigms

Cited by 166 publications

References 164 publications

Tocilizumab in Autoimmune Encephalitis Refractory to Rituximab: An Institutional Cohort Study

Tocilizumab in Autoimmune Encephalitis Refractory to Rituximab: An Institutional Cohort Study

Paraneoplastic neurologic disorders in small cell lung carcinoma

Neuronal antibodies in pediatric epilepsy: Clinical features and long‐term outcomes of a historical cohort not treated with immunotherapy

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