key: cord-1041652-20mvr8r3
authors: Mergenthaler, Philipp; Stetefeld, Henning R.; Dohmen, Christian; Kohler, Siegfried; Schönenberger, Silvia; Bösel, Julian; Gerner, Stefan T.; Huttner, Hagen B.; Schneider, Hauke; Reichmann, Heinz; Fuhrer, Hannah; Berger, Benjamin; Zinke, Jan; Alberty, Anke; Kleiter, Ingo; Schneider-Gold, Christiane; Roth, Christian; Dunkel, Juliane; Steinbrecher, Andreas; Thieme, Andrea; Lee, De-Hyung; Linker, Ralf A.; Angstwurm, Klemens; Meisel, Andreas; Neumann, Bernhard
title: Seronegative myasthenic crisis: a multicenter analysis
date: 2022-04-07
journal: J Neurol
DOI: 10.1007/s00415-022-11023-z
sha: 2d636cd9d5df593289fab5ee50c38e46635859f3
doc_id: 1041652
cord_uid: 20mvr8r3

Myasthenic crisis (MC) is a life-threatening condition for patients with myasthenia gravis (MG). Seronegative patients represent around 10–15% of MG, but data on outcome of seronegative MCs are lacking. We performed a subgroup analysis of patients who presented with MC with either acetylcholine-receptor-antibody-positive MG (AChR-MG) or seronegative MG between 2006 and 2015 in a retrospective German multicenter study. We identified 15 seronegative MG patients with 17 MCs and 142 AChR-MG with 159 MCs. Seronegative MCs were younger (54.3 ± 14.5 vs 66.5 ± 16.3 years; p = 0.0037), had a higher rate of thymus hyperplasia (29.4% vs 3.1%; p = 0.0009), and were more likely to be female (58.8% vs 37.7%; p = 0.12) compared to AChR-MCs. Time between diagnosis of MG and MC was significantly longer in seronegative patients (8.2 ± 7.6 vs 3.1 ± 4.4 years; p < 0.0001). We found no differences in duration of mechanical ventilation (16.2 ± 15.8 vs 16.5 ± 15.9 days; p = 0.94) and length of stay at intensive care unit (17.6 ± 15.2 vs 17.8 ± 15.4 days; p = 0.96), or in-hospital mortality (11.8% vs. 10.1%; p = 0.69). We conclude that MC in seronegative MG affects younger patients after a longer period of disease, but that crisis treatment efficacy and outcome do not differ compared to AChR-MCs.

Myasthenia gravis (MG) is an autoimmune disease with antibodies (Abs) targeting the postsynaptic neuromuscular junction. Ultimately, muscle fatigability and weakness are caused by disrupted neuromuscular signaling. Nearly 90% of all MG patients have positive test results for AChR, Muscle-specific kinase (MuSK), or low-density lipoprotein receptor-related protein (LRP4) autoantibodies, with the majority tested positive for AChR-Abs [1] . However, in around 10-15% of MG patients no specific autoantibodies can be found. This group of seronegative patients is also thought to include patients with very low antibody titers, low-affinity antibodies and yet to be defined autoantigens [1] .

Myasthenic crisis (MC) is the most severe form of MG and is potentially life threatening. MC is mostly provoked by infections, but also fever, aspiration, inadequate treatment, various medications, or following surgery [2] . In the first two years after diagnosis, around 15-20% of MG patients suffer from a MC [2, 3] . Characteristic symptoms are extensive weakness, dysphagia, and dyspnea which can result in respiratory insufficiency. The clinical management of MC is well defined and has led to a significant decline in mortality from around 40% in the early 1960s to 5% to 12% in recent studies [2] [3] [4] [5] [6] [7] [8] .

However, to date little is known about the management of MC in seronegative MG. Here, we therefore investigated seronegative patients with MC and compared their crises to AChR-MCs regarding clinical features, therapeutic management, and outcome. Bernhard Neumann: on behalf of the Initiative of German NeuroIntensive Trial Engagement (IGNITE) and with support from the German Neurocritical Care Society (DGNI)

We performed a subgroup analysis of seronegative MC needing mechanical ventilation (MV) compared to AChR-MC treated at eight German Departments of Neurology with specialized Neuro-Intensive Care Units (NICU) or neurologically associated interdisciplinary ICU [2] . For identification, records of all patients discharged with the diagnosis of MG according to the International Classification of Diseases (ICD10: G70.0-70.3) who were treated and ventilated on an ICU between 2006 and 2015 were reviewed. MC was defined as an exacerbation of myasthenic symptoms with bulbar and/or general weakness requiring MV. Seronegative MG was defined as absence of AChR and MuSK autoantibodies. Per protocol, antibody status was confirmed by routine laboratory testing using certified assays. Most AChR-Abs and MuSK-Abs were tested by radio-receptor assay, but the method is not known in all cases due to the retrospective character. Diagnosis of MG had to be established clinically according to national guidelines and confirmed by specific tests (antibody testing or repetitive stimulation or improvement after cholinergic medication) [9] . New episodes of MC were counted separately if patients were discharged in their prehospital status and if new triggers for the next crisis could be determined. For this analysis, we only included AChR-MCs treated at the same centers as the seronegative MCs to reduce treatment and data acquisition bias.

Data on baseline demographics, clinical information, medication and comorbidities were obtained through review of medical records and institutional databases. Characteristics reviewed included antibody-status, evidence of thymoma and Myasthenia Gravis Foundation of America (MGFA) Score prior to MC. Assessed treatment regimens were intravenous immunoglobulins (IVIG), plasma exchanging therapy (PE), immunoadsorption (IA), use of intravenous pyridostigmine, and continuous potassium infusion. Analyzed data regarding the MC included time at intensive care unit (ICU-LOS), days in hospital, duration of MV, in-hospital mortality and referral/discharge. In addition, we performed a survey about LRP4-and Agrin-antibody-positive MGs in our study group in June 2021.

GraphPad Prism 5® (GraphPad Software, La Jolla, USA) was used for statistical analysis. Data were presented as mean with standard deviation or range (as indicated) or total number with percentage. Group comparison was tested with either Student's t test or Fisher's exact test (with odds ratios (OR)). The significance level was set to α = 0.05 both sided.

The cohort consisted of 15 patients with 17 seronegative MCs and 142 AChR antibody-positive patients with 159 MCs requiring MV. Patients from both groups were treated at the same centers (Table 1 ). Seronegative patients were responsible for 6.8% of the crises in our whole cohort (n = 250 crises). Patients with seronegative MC were significantly younger (54.3 ± 14.5 vs 66.5 ± 16.3; p = 0.0037) and more likely to be female (58.8 vs 37.7%; p = 0.12) than AChR-MCs. AChR-MCs were significantly more often late-onset MGs (85.5% vs 41.2%; p = 0.0001; OR = 0.12), whereas seronegative MCs belonged mainly to the earlyonset group (Table 1 ) and had significantly more frequently a thymus hyperplasia (29.4% vs 3.1%; p = 0.0009; OR 12.83). Thymus hyperplasias were resected in all patients prior to crisis, except in one patient in the AChR-group. Importantly, the time between diagnosis of MG and onset of MC was significantly longer in seronegative patients (8.2 ± 7.6 vs 3.1 ± 4.4 years; p < 0.0001) (Fig. 1A ). Due to the higher age, patients with AChR-MCs had more comorbidities, yet without reaching statistical significance (Table 1) . We also did not find statistically significant differences in the status before crisis, MGFA classification before crisis, dosage of pyridostigmine treatment before crisis (252.4 ± 243.3 vs 251.1 ± 206.6 mg/d; p = 0.99) or number of myasthenic worsening/crises before present MC ( Table 1 ). The number of days between first symptoms of MC and hospitalization were similar (9.9 ± 13.1 vs 9.6 ± 14.9; p = 0.95).

To further characterize the patients with seronegative MCs, we surveyed all participating centers on retesting for LRP4 and Agrin antibodies in these seronegative patients. 6 of 15 seronegative MGs were tested for LRP4-antibodies and 5 of 15 for Agrin-antibodies. However, all tests remained negative. At the centers of our study group 28 patients with LRP4 and 0 patients with Agrin-antibodies are treated, but none developed an MC needing ICU-treatment within the period of observation.

Seronegative MCs were significantly less frequently treated with IVIGs (23.5% vs 58.5%; p = 0.009; OR = 0.22) ( Table 1) , and although they received PE or IA more frequently than AChR-MCs, no statistically significant Table 1 Comparison of episodes of myasthenic crisis with AChR-Abs and seronegative patients Age, "Days of mechanical ventilation at ICU", "Days at ICU", "Days in hospital" and "Time between first diagnosis and crisis (years)"are depicted as mean ± Standard Deviation and range, other parameters are total number with percentage in brackets. MGFA Myasthenia Gravis Foundation of America, MG Myasthenia Gravis, IVIG Intravenous Immunoglobulin, PE Plasma exchange, IA Immunoadsorption, CPR Cardio Table 2 . We found no difference between the treatment options IVIG and PE/IA or the additional use of intravenous pyridostigmine regarding the endpoint duration of MV in seronegative MCs.

Here, we investigated clinical features of seronegative MC compared to AChR-MC requiring mechanical ventilation based on our multicenter cohort of MC [2] . In contrast to MuSK-MCs, which are as old as AChR-MCs [5] , we found that in seronegative MC, patients were younger but that the time between diagnosis of MG and onset of MC was longer compared to AChR-MC. Interestingly, 8 of 17 seronegative MCs had thymic abnormalities. Although seronegative MCs Pulmonal Resuscitation, n.s. not significant. t test was used for statistical analysis of age-differences and for comparison of "Days of mechanical ventilation at ICU", "Days at ICU" and "Days in hospital". For other parameters Fisher`s exact test with odds ratio was used. Significant result (p ≤ 0.05) are shown in bold letters were less frequently treated with IVIg, there was no difference in other MC treatments. Furthermore, we did not find any difference in baseline characteristics, in the rate of complications or outcome between the patient groups, which is in contrast to more severely affected MuSK MC patients [5] . Seronegative patients represent 10-15% of all MGs. However, there are only very limited data on the clinical management and outcome of MC. In our cohort of MCs, 17 of 250 (6.8%) events were from seronegative patients [2] , which may indicate that MC is less prevalent in seronegative patients. Yet, our study was not designed to unambiguously address this question. While MC occurs in most MG patients within the first 2 years after diagnosis [3] , seronegative patients in our cohort developed MC significantly later compared to AChR-MG thus suggesting a less severe disease onset in these patients.

Interestingly, LRP4-positive MGs treated at our centers until now never experienced a MC and all retested seronegative patients in our cohort (40%) were negative for LRP4. Moreover, we did not find any publication about a LRP4-MC suggesting that this subgroup is even less severely affected than seronegative MG.

Seronegative MG patients are a heterogeneous group of patients and although we had stringent inclusion criteria, we cannot rule out that some seronegative patients have lowaffinity antibodies or would be positive for complement deposition at the neuromuscular junction [10, 11] . Especially the high portion of thymus hyperplasia in our cohort might argue for low-affinity antibodies since thymic pathologies in MG are known to produce AChR-antibodies [12] , but 75% of double negative patients (AChR and MuSK) showed lymph node-type infiltrates in thymus similar to AChR-MG [13] .

Limitations of this study arise from its retrospective nature and the relatively small sample size. Nevertheless, our study is by far the largest analysis of seronegative MCs and therefore provides important evidence on the treatment of this understudied patient population. Nevertheless, large prospective multicenter studies are needed to further elucidate the character of seronegative myasthenic crisis and whether specific treatment is warranted compared to AChR-MC or MuSK-MC. Another limitation is that antibody tests were done in different labs and therefore false negative or false positive results due to unspecificity of the test technique or positive/negative results near the threshold range cannot be ruled out in every case, like in previous studies in myasthenia gravis.

We conclude that patients with seronegative MC are younger, with a longer course of disease until first crisis needing MV than AChR-MC but that there is no difference in outcome between these patient groups. Funding Open Access funding enabled and organized by Projekt DEAL. PM is Einstein Junior Fellow of the Einstein Foundation Berlin and has been supported by the Charité-BIH Clinician Scientist Program and the Bundesministerium für Bildung und Forschung (Grant nos. 16GW0191 and NUM-COVID 19-Organo-Strat 01KX2021). This research did not receive further specific grant from any funding agency in the public, commercial, or not-for-profit sectors.

Data availability Anonymized data will be made available upon reasonable request. Ethical approval All procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and/or national research committee and with the 1964 Helsinki Declaration and its later amendments or comparable ethical standards. Local ethic committees and institutional review boards of the participating centers approved the study based on the central vote of the ethics committee at University of . Due to the retrospective character of the study, patient`s consent was not necessary according to the decisions of the ethic committees and institutional review boards.

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IgG1 antibodies to acetylcholine receptors in 'seronegative' myasthenia gravis

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Authors and Affiliations

18 · Juliane Dunkel 17 · Andreas Steinbrecher 19 · Andrea Thieme 19 · De-Hyung Lee 20 · Ralf A. Linker 20 · Klemens Angstwurm 20 · Andreas Meisel 1,2,21 · Bernhard Neumann 20,22 · for The

Gerner stefan.gerner@neuro.med.uni-giessen

Huttner direktion@neuro.med.uni-giessen

Hauke Schneider hauke.schneider@uk-augsburg