Your search keyword '"Leonhard, S.E."' showing total 11 results

1. Proposal for a screening protocol for Candida auris colonization

Author

Leonhard, S.E., Chong, G.M., Foudraine, D.E., Bode, L.G.M., Croughs, P., Popping, S., Schaftenaar, E., Klaassen, C.H.W., and Severin, J.A.

Published

2024

2. Predicting Outcome in Guillain-Barre Syndrome International Validation of the Modified Erasmus GBS Outcome Score

Author

Doets, A.Y., Lingsma, H.F., Walgaard, C., Islam, B., Papri, N., Davidson, A., Yamagishi, Y., Kusunoki, S., Dimachkie, M.M., Waheed, W., Kolb, N., Islam, Z., Mohammad, Q.D., Harbo, T., Sindrup, S.H., Chavada, G., Willison, H.J., Casasnovas, C., Bateman, K., Miller, J.A.L., Berg, B. van den, Verboon, C., Roodbol, J., Leonhard, S.E., Benedetti, L., Kuwabara, S., Bergh, P. van den, Monges, S., Marfia, G.A., Shahrizaila, N., Galassi, G., Pereon, Y., Burmann, J., Kuitwaard, K., Kleyweg, R.P., Marchesoni, C., Tous, M.J.S., Querol, L., Illa, I., Wang, Y.Z., Nobile-Orazio, E., Rinaldi, S., Schenone, A., Pardo, J., Vermeij, F.H., Lehmann, H.C., Granit, V., Cavaletti, G., Gutierrez-Gutierrez, G., Barroso, F.A., Visser, L.H., Katzberg, H.D., Dardiotis, E., Attarian, S., Kooi, A.J. van der, Eftimov, F., Wirtz, P.W., Samijn, J.P.A., Gilhuis, H.J., Hadden, R.D.M., Holt, J.K.L., Sheikh, K.A., Karafiath, S., Vytopil, M., Antonini, G., Feasby, T.E., Faber, C.G., Gijsbers, C.J., Busby, M., Roberts, R.C., Silvestri, N.J., Fazio, R., Dijk, G.W. van, Garssen, M.P.J., Straathof, C.S.M., Gorson, K.C., Jacobs, B.C., IGOS Consortium, Neurology, ANS - Neuroinfection & -inflammation, EURO-NMD, Klinische Neurowetenschappen, MUMC+: MA Med Staf Spec Neurologie (9), RS: MHeNs - R1 - Cognitive Neuropsychiatry and Clinical Neuroscience, Doets, A, Lingsma, H, Walgaard, C, Islam, B, Papri, N, Davidson, A, Yamagishi, Y, Kusunoki, S, Dimachkie, M, Waheed, W, Kolb, N, Islam, Z, Mohammad, Q, Harbo, T, Sindrup, S, Chavada, G, Willison, H, Casasnovas, C, Bateman, K, Miller, J, van den Berg, B, Verboon, C, Roodbol, J, Leonhard, S, Benedetti, L, Kuwabara, S, Van den Bergh, P, Monges, S, Marfia, G, Shahrizaila, N, Galassi, G, Péréon, Y, Bürmann, J, Kuitwaard, K, Kleyweg, R, Marchesoni, C, Sedano Tous, M, Querol, L, Illa, I, Wang, Y, Nobile-Orazio, E, Rinaldi, S, Schenone, A, Pardo, J, Vermeij, F, Lehmann, H, Granit, V, Cavaletti, G, Gutiérrez-Gutiérrez, G, Barroso, F, Visser, L, Katzberg, H, Dardiotis, E, Attarian, S, van der Kooi, A, Eftimov, F, Wirtz, P, Samijn, J, Gilhuis, H, Hadden, R, Holt, J, Sheikh, K, Karafiath, S, Vytopil, M, Antonini, G, Feasby, T, Faber, C, Gijsbers, C, Busby, M, Roberts, R, Silvestri, N, Fazio, R, van Dijk, G, Garssen, M, Straathof, C, Gorson, K, Jacobs, B, Public Health, and Immunology

Subjects

Guillain-Barrè, predicting, outcome, IGOS, MODELS, Guillain-Barre Syndrome, Prognosis, Settore MED/26, Cohort Studies, POOR-PROGNOSIS, Outcome Assessment, Health Care, Humans, INTRAVENOUS IMMUNOGLOBULIN, Neurology (clinical), Prospective Studies, Child, Research Article

Abstract

Background and ObjectivesThe clinical course and outcome of the Guillain-Barré syndrome (GBS) are diverse and vary among regions. The modified Erasmus GBS Outcome Score (mEGOS), developed with data from Dutch patients, is a clinical model that predicts the risk of walking inability in patients with GBS. The study objective was to validate the mEGOS in the International GBS Outcome Study (IGOS) cohort and to improve its performance and region specificity.MethodsWe used prospective data from the first 1,500 patients included in IGOS, aged ≥6 years and unable to walk independently. We evaluated whether the mEGOS at entry and week 1 could predict the inability to walk unaided at 4 and 26 weeks in the full cohort and in regional subgroups, using 2 measures for model performance: (1) discrimination: area under the receiver operating characteristic curve (AUC) and (2) calibration: observed vs predicted probability of being unable to walk independently. To improve the model predictions, we recalibrated the model containing the overall mEGOS score, without changing the individual predictive factors. Finally, we assessed the predictive ability of the individual factors.ResultsFor validation of mEGOS at entry, 809 patients were eligible (Europe/North America [n = 677], Asia [n = 76], other [n = 56]), and 671 for validation of mEGOS at week 1 (Europe/North America [n = 563], Asia [n = 65], other [n = 43]). AUC values were >0.7 in all regional subgroups. In the Europe/North America subgroup, observed outcomes were worse than predicted; in Asia, observed outcomes were better than predicted. Recalibration improved model accuracy and enabled the development of a region-specific version for Europe/North America (mEGOS-Eu/NA). Similar to the original mEGOS, severe limb weakness and higher age were the predominant predictors of poor outcome in the IGOS cohort.DiscussionmEGOS is a validated tool to predict the inability to walk unaided at 4 and 26 weeks in patients with GBS, also in countries outside the Netherlands. We developed a region-specific version of mEGOS for patients from Europe/North America.Classification of EvidenceThis study provides Class II evidence that the mEGOS accurately predicts the inability to walk unaided at 4 and 26 weeks in patients with GBS.Trial Registration InformationNCT01582763.

Published

2022

3. Guillain-Barré syndrome during the Zika virus outbreak in Northeast Brazil: An observational cohort study

Author

Leonhard, S.E. (Sonja E.), Halstead, S.K. (Susan), Lant, S.B. (Suzannah B.), Militão de Albuquerque, M.D.F.P. (Maria de Fatima Pessoa), de Brito, C.A.A. (Carlos Alexandre Antunes), de Albuquerque, L.B.B. (Lívia Brito Bezerra), Ellul, M.A. (Mark A.), de Oliveira França, R.F. (Rafael Freitas), Gourlay, D. (Dawn), Griffiths, M.J. (Michael J.), de Miranda Henriques-Souza, A.M. (Adélia Maria), de Morais Machado, M.Í. (Maria Í.), Medialdea-Carrera, R. (Raquel), Mehta, R. (Ravi), da Paz Melo, R. (Roberta), Mesquita, S.D. (Solange D.), Moreira, Á.J.P. (Álvaro J.P.), Pena, L.J. (Lindomar J.), Santos, M.L. (Marcela Lopes), Turtle, L. (Lance), Solomon, T. (Tom), Willison, H.J. (Hugh), Jacobs, B.C. (Bart), Brito Ferreira, M.L. (Maria L.), Leonhard, S.E. (Sonja E.), Halstead, S.K. (Susan), Lant, S.B. (Suzannah B.), Militão de Albuquerque, M.D.F.P. (Maria de Fatima Pessoa), de Brito, C.A.A. (Carlos Alexandre Antunes), de Albuquerque, L.B.B. (Lívia Brito Bezerra), Ellul, M.A. (Mark A.), de Oliveira França, R.F. (Rafael Freitas), Gourlay, D. (Dawn), Griffiths, M.J. (Michael J.), de Miranda Henriques-Souza, A.M. (Adélia Maria), de Morais Machado, M.Í. (Maria Í.), Medialdea-Carrera, R. (Raquel), Mehta, R. (Ravi), da Paz Melo, R. (Roberta), Mesquita, S.D. (Solange D.), Moreira, Á.J.P. (Álvaro J.P.), Pena, L.J. (Lindomar J.), Santos, M.L. (Marcela Lopes), Turtle, L. (Lance), Solomon, T. (Tom), Willison, H.J. (Hugh), Jacobs, B.C. (Bart), and Brito Ferreira, M.L. (Maria L.)

Abstract

Objective: To determine the clinical phenotype of Guillain-Barré syndrome (GBS) after Zika virus (ZIKV) infection, the anti-glycolipid antibody signature, and the role of other circulating arthropod-borne viruses, we describe a cohort of GBS patients identified during ZIKV and chikungunya virus (CHIKV) outbreaks in Northeast Brazil. Methods: We prospectively recruited GBS patients from a regional neurology center in Northeast Brazil between December 2014 and February 2017. Serum and CSF were tested for ZIKV, CHIKV, and dengue virus (DENV), by RT-PCR and antibodies, and serum was tested for GBS-associated antibodies to glycolipids. Results: Seventy-one patients were identified. Forty-eight (68%) had laboratory evidence of a recent arbovirus infection; 25 (52%) ZIKV, 8 (17%) CHIKV, 1 (2%) DENV, and 14 (29%) ZIKV and CHIKV. Most patients with a recent arbovirus infection had motor and sensory symptoms (72%), a demyelinating electrophysiological subtype (67%) and a facial palsy (58%). Patients with a recent infection with ZIKV and CHIKV had a longer hospital admission and more frequent mechanical ventilation compared to the other patients. No specific anti-glycolipid antibody signature was identified in association with arbovirus infection, although significant antibody titres to GM1, GalC, LM1, and GalNAc-GD1a were found infrequently. Conclusion: A large proportion of cases had laboratory evidence of a recent infection with ZIKV or CHIKV, and recent infection with both viruses was found in almost one third of patients. Most patients with a recent arbovirus infection had a sensorimotor, demyelinating GBS. We did not find a specific anti-glycolipid antibody signature in association with arbovirus-related GBS.

Published

2021

4. Guillain-Barré Syndrome Outbreak in Peru 2019 Associated With Campylobacter jejuni Infection

Author

Ramos, A.P. (Ana P.), Leonhard, S.E. (Sonja E.), Halstead, S.K. (Susan), Cuba, M.A. (Mireya A.), Castañeda, C.C. (Carlos C.), Dioses, J.A. (Jose A.), Tipismana, M.A. (Martin A.), Abanto, J.T. (Jesus T.), Llanos, A. (Alejandro), Gourlay, D. (Dawn), Grogl, M. (Max), Ramos, M. (Mariana), Rojas, J.D. (Jesus D.), Meza, R. (Rina), Puiu, D. (Daniela), Sherman, R.M. (Rachel M.), Salzberg, S.L. (Steven L.), Simner, P.J. (Patricia J.), Willison, H.J. (Hugh), Jacobs, B.C. (Bart), Cornblath, D.R. (David), Umeres, H.F. (Hugo F.), Pardo, C. (Carlos), Ramos, A.P. (Ana P.), Leonhard, S.E. (Sonja E.), Halstead, S.K. (Susan), Cuba, M.A. (Mireya A.), Castañeda, C.C. (Carlos C.), Dioses, J.A. (Jose A.), Tipismana, M.A. (Martin A.), Abanto, J.T. (Jesus T.), Llanos, A. (Alejandro), Gourlay, D. (Dawn), Grogl, M. (Max), Ramos, M. (Mariana), Rojas, J.D. (Jesus D.), Meza, R. (Rina), Puiu, D. (Daniela), Sherman, R.M. (Rachel M.), Salzberg, S.L. (Steven L.), Simner, P.J. (Patricia J.), Willison, H.J. (Hugh), Jacobs, B.C. (Bart), Cornblath, D.R. (David), Umeres, H.F. (Hugo F.), and Pardo, C. (Carlos)

Abstract

OBJECTIVE: To identify the clinical phenotypes and infectious triggers in the 2019 Peruvian Guillain-Barré syndrome (GBS) outbreak. METHODS: We prospectively collected clinical and neurophysiologic data of patients with GBS admitted to a tertiary hospital in Lima, Peru, between May and August 2019. Molecular, immunologic, and microbiological methods were used to identify causative infectious agents. Sera from 41 controls were compared with cases for antibodies to Campylobacter jejuni and gangliosides. Genomic analysis was performed on 4 C jejuni isolates. RESULTS: The 49 included patients had a median age of 44 years (interquartile range [IQR] 30-54 years), and 28 (57%) were male. Thirty-two (65%) had symptoms of a preceding infection: 24 (49%) diarrhea and 13 (27%) upper respiratory tract infection. The median time between infectious to neurologic symptoms was 3 days (IQR 2-9 days). Eighty percent had a pure motor form of GBS, 21 (43%) had the axonal electrophysiologic subtype, and 18% the demyelinating subtype. Evidence of recent C jejuni infection was found in 28/43 (65%). No evidence of recent arbovirus infection was found. Twenty-three cases vs 11 controls (OR 3.3, confidence interval [CI] 95% 1.2-9.2, p < 0.01) had IgM and/or IgA antibodies against C jejuni. Anti-GM1:phosphatidylserine and/or anti-GT1a:GM1 heteromeric complex antibodies were strongly positive in cases (92.9% sensitivity and 68.3% specificity). Genomic analysis showed that the C jejuni strains were closely related and had the Asn51 polymorphism at cstII gene. CONCLUSIONS: Our study indicates that the 2019 Peruvian GBS outbreak was associated with C jejuni infection and that the C jejuni strains linked to GBS circulate widely in different parts of the world.

Published

2021

5. Second intravenous immunoglobulin dose in patients with Guillain-Barré syndrome with poor prognosis (SID-GBS): a double-blind, randomised, placebo-controlled trial

Author

Walgaard, C., Walgaard, C., Jacobs, B.C., Lingsma, H.F., Steyerberg, E.W., van den Berg, B., Doets, A.Y., Leonhard, S.E., Verboon, C., Huizinga, R., Drenthen, J., Arends, S., Budde, I.K., Kleyweg, R.P., Kuitwaard, K., van der Meulen, M.F.G., Samijn, J.P.A., Vermeij, F.H., Kuks, J.B.M., van Dijk, G.W., Wirtz, P.W., Eftimov, F., van der Kooi, A.J., Garssen, M.P.J., Gijsbers, C.J., de Rijk, M.C., Visser, L.H., Blom, R.J., Linssen, W.H.J.P., van der Kooi, E.L., Verschuuren, J.J.G.M., van Koningsveld, R., Dieks, R.J.G., Gilhuis, H.J., Jellema, K., van der Ree, T.C., Bienfait, H.M.E., Faber, C.G., Lovenich, H., van Engelen, B.G.M., Groen, R.J., Merkies, I.S.J., van Oosten, B.W., van der Pol, W.L., van der Meulen, W.D.M., Badrising, U.A., Stevens, M., Breukelman, A.J.J., Zwetsloot, C.P., van der Graaff, M.M., Wohlgemuth, M., Dutch GBS Study Grp, van Doorn, Pieter Antoon, Walgaard, C., Walgaard, C., Jacobs, B.C., Lingsma, H.F., Steyerberg, E.W., van den Berg, B., Doets, A.Y., Leonhard, S.E., Verboon, C., Huizinga, R., Drenthen, J., Arends, S., Budde, I.K., Kleyweg, R.P., Kuitwaard, K., van der Meulen, M.F.G., Samijn, J.P.A., Vermeij, F.H., Kuks, J.B.M., van Dijk, G.W., Wirtz, P.W., Eftimov, F., van der Kooi, A.J., Garssen, M.P.J., Gijsbers, C.J., de Rijk, M.C., Visser, L.H., Blom, R.J., Linssen, W.H.J.P., van der Kooi, E.L., Verschuuren, J.J.G.M., van Koningsveld, R., Dieks, R.J.G., Gilhuis, H.J., Jellema, K., van der Ree, T.C., Bienfait, H.M.E., Faber, C.G., Lovenich, H., van Engelen, B.G.M., Groen, R.J., Merkies, I.S.J., van Oosten, B.W., van der Pol, W.L., van der Meulen, W.D.M., Badrising, U.A., Stevens, M., Breukelman, A.J.J., Zwetsloot, C.P., van der Graaff, M.M., Wohlgemuth, M., Dutch GBS Study Grp, and van Doorn, Pieter Antoon

Abstract

Background Treatment with one standard dose (2 g/kg) of intravenous immunoglobulin is insufficient in a proportion of patients with severe Guillain-Barre syndrome. Worldwide, around 25% of patients severely affected with the syndrome are given a second intravenous immunoglobulin dose (SID), although it has not been proven effective. We aimed to investigate whether a SID is effective in patients with Guillain-Barre syndrome with a predicted poor outcome.Methods In this randomised, double-blind, placebo-controlled trial (SID-GBS), we included patients (>= 12 years) with Guillain-Barre syndrome admitted to one of 59 participating hospitals in the Netherlands. Patients were included on the first day of standard intravenous immunoglobulin treatment (2 g/kg over 5 days). Only patients with a poor prognosis (score of >= 6) according to the modified Erasmus Guillain-Barre syndrome Outcome Score were randomly assigned, via block randomisation stratified by centre, to SID (2 g/kg over 5 days) or to placebo, 7-9 days after inclusion. Patients, outcome adjudicators, monitors, and the steering committee were masked to treatment allocation. The primary outcome measure was the Guillain-Barre syndrome disability score 4 weeks after inclusion. All patients in whom allocated trial medication was started were included in the modified intention-to-treat analysis.Findings Between Feb 16, 2010, and June 5, 2018, 327 of 339 patients assessed for eligibility were included. 112 had a poor prognosis. Of those, 93 patients with a poor prognosis were included in the modified intention-to-treat analysis: 49 (53%) received SID and 44 (47%) received placebo. The adjusted common odds ratio for improvement on the Guillain-Barre syndrome disability score at 4 weeks was 1.4 (95% CI 0.6-3.3; p=0.45). Patients given SID had more serious adverse events (35% vs 16% in the first 30 days), including thromboembolic events, than those in the placebo group. Four patients died in the intervention group (

Published

2021

6. Guillain-Barré syndrome in times of pandemics

Author

Leonhard, S.E., Cornblath, D.R. (David), Endtz, H.P. (Hubert), Sejvar, J.J., Jacobs, B.C. (Bart), Leonhard, S.E., Cornblath, D.R. (David), Endtz, H.P. (Hubert), Sejvar, J.J., and Jacobs, B.C. (Bart)

Published

2020

7. Guillain-Barré syndrome related to Zika virus infection: A systematic review and meta-analysis of the clinical and electrophysiological phenotype

Author

Leonhard, S.E. (Sonja E.), Bresani-Salvi, C.C. (Cristiane C.), Lyra Batista, J.D. (Joanna D.), Cunha, S. (Sergio), Jacobs, B.C. (Bart), Brito Ferreira, M.L. (Maria Lucia), P Militão de Albuquerque, M.F. (Maria de Fatima), Leonhard, S.E. (Sonja E.), Bresani-Salvi, C.C. (Cristiane C.), Lyra Batista, J.D. (Joanna D.), Cunha, S. (Sergio), Jacobs, B.C. (Bart), Brito Ferreira, M.L. (Maria Lucia), and P Militão de Albuquerque, M.F. (Maria de Fatima)

Abstract

BACKGROUND: The Zika virus (ZIKV) has been associated with Guillain-Barré syndrome (GBS) in epidemiological studies. Whether ZIKV-associated GBS is related to a specific clinical or electrophysiological phenotype has not been established. To this end, we performed a systematic review and meta-analysis of all published st

Published

2020

8. Diagnosis and management of Guillain–Barré syndrome in ten steps

Author

Leonhard, S.E. (Sonja E.), Mandarakas, M.R. (Melissa R.), Gondim, F.A.A. (Francisco A. A.), Bateman, K. (Kathleen), Ferreira, M.L.B. (Maria L. B.), Cornblath, D.R. (David), Doorn, P.A. (Pieter) van, Dourado, M.E. (Mario E.), Hughes, R.A.C. (Richard), Islam, B. (Badrul), Kusunoki, S. (Susumu), Pardo, C. (Carlos), Reisin, R. (Ricardo), Sejvar, J.J. (James J.), Shahrizaila, N. (Nortina), Soares, C. (Cristiane), Umapathi, T. (Thirugnanam), Wang, Y. (Yuzhong), Yiu, E.M. (Eppie M.), Willison, H.J. (Hugh), Jacobs, B.C. (Bart), Leonhard, S.E. (Sonja E.), Mandarakas, M.R. (Melissa R.), Gondim, F.A.A. (Francisco A. A.), Bateman, K. (Kathleen), Ferreira, M.L.B. (Maria L. B.), Cornblath, D.R. (David), Doorn, P.A. (Pieter) van, Dourado, M.E. (Mario E.), Hughes, R.A.C. (Richard), Islam, B. (Badrul), Kusunoki, S. (Susumu), Pardo, C. (Carlos), Reisin, R. (Ricardo), Sejvar, J.J. (James J.), Shahrizaila, N. (Nortina), Soares, C. (Cristiane), Umapathi, T. (Thirugnanam), Wang, Y. (Yuzhong), Yiu, E.M. (Eppie M.), Willison, H.J. (Hugh), and Jacobs, B.C. (Bart)

Abstract

Guillain–Barré syndrome (GBS) is a rare, but potentially fatal, immune-mediated disease of the peripheral nerves and nerve roots that is usually triggered by infections. The incidence of GBS can therefore increase during outbreaks of infectious diseases, as was seen during the Zika virus epidemics in 2013 in French Polynesia and 2015 in Latin America. Diagnosis and management of GBS can be complicated as its clinical presentation and disease course are heterogeneous, and no international clinical guidelines are currently available. To support clinicians, especially in the context of an outbreak, we have developed a globally applicable guideline for the diagnosis and management of GBS. The guideline is based on current literature and expert consensus, and has a ten-step structure to facilitate its use in clinical practice. We first provide an introduction to the diagnostic criteria, clinical variants and differential diagnoses of GBS. The ten steps then cover early recognition and diagnosis of GBS, admission to the intensive care unit, treatment indication and selection, monitoring and treatment of disease progression, prediction of clinical course and outcome, and management of complications and sequelae.

Published

2019

9. Diagnosis and treatment of Guillain-Barré syndrome during the Zika virus epidemic in Brazil: A national survey study

Author

Leonhard, S.E. (Sonja E.), Conde, R.M. (Rodrigo M.), de Assis Aquino Gondim, F. (Francisco), Jacobs, B.C. (Bart), Leonhard, S.E. (Sonja E.), Conde, R.M. (Rodrigo M.), de Assis Aquino Gondim, F. (Francisco), and Jacobs, B.C. (Bart)

Abstract

The Zika virus (ZIKV) epidemic in Brazil in 2015-2016 was followed by an increase in the incidence of patients with Guillain-Barré syndrome (GBS). With this national survey study, we aimed to gain a better understanding of how neurologists in Brazil are currently diagnosing and treating patients with GBS, and how this increase in incidence has impacted the management of the disease. The questionnaire consisted of 52 questions covering: personal profile of the neurologist, practice of managing GBS during and outside of the ZIKV epidemic, and limitations in managing GBS. All 3264 neurologists that were member of the Brazilian Academy of Neurology at the time of the study were invited to participate. The questionnaire was fully answered by 171 (5%) neurologists. Sixty-one percent of neurologists noticed an increase in patients with GBS during the ZIKV epidemic, and 30% experienced an increase in problems in managing GBS during this time. The most important limitations in the diagnosis and management of GBS included the availability of nerve conduction studies (NCS), beds in the Intensive Care Unit (ICU) and referral to rehabilitation centers. Most neurologists did not use a protocol for treating patients with GBS and the treatment practice varied. Increasing availability of NCS and beds in the ICU and rehabilitation centers, and the implementation of (inter)national guidelines, are critical in supporting Brazilian neurologist in their management of GBS, and

Published

2019

10. Zika virus infection in the returning traveller: What every neurologist should know

Author

Leonhard, S.E. (Sonja), Lant, S. (Suzannah), Jacobs, B.C. (Bart), Wilder-Smith, A. (Annelies), Ferreira, M.L.B. (Maria Lucia Brito), Solomon, T. (Tom), Willison, H.J. (Hugh), Leonhard, S.E. (Sonja), Lant, S. (Suzannah), Jacobs, B.C. (Bart), Wilder-Smith, A. (Annelies), Ferreira, M.L.B. (Maria Lucia Brito), Solomon, T. (Tom), and Willison, H.J. (Hugh)

Abstract

Zika virus has been associated with a wide range of neurological complications. Neurologists in areas without current active transmission of the virus may be confronted with Zika-associated neurological disease, as a large number of returning travellers with Zika virus infection have been reported and the virus continues to spread to previously unaffected regions. This review provides an overview of Zika virus-associated neurological disease and aims to support neurologists who may encounter patients returning from endemic areas.

Published

2018

11. Second IVIg course in Guillain‐Barré syndrome patients with poor prognosis (SID‐GBS trial): Protocol for a double‐blind randomized, placebo‐controlled clinical trial.

Author

Walgaard, Christa, Jacobs, Bart C., Lingsma, Hester F., Steyerberg, Ewout W., Cornblath, David R., van Doorn, Pieter A., van Doorn, P.A., Jacobs, B.C., Walgaard, C., de Wit, M.C.Y., Steyerberg, E.W., Cornblath, D.R., van den Berg, B., Doets, A.Y., Leonhard, S.E., Verboon, J.C., van Woerkom, M., Tio‐Gillen, A.P., van Rijs, W., and Huizinga, H.

Subjects

THERAPEUTIC use of immunoglobulins, FUNCTIONAL assessment, LENGTH of stay in hospitals, HOSPITAL admission & discharge, IMMUNOGLOBULINS, INTENSIVE care units, MEDICAL societies, PATIENTS, GUILLAIN-Barre syndrome, RANDOMIZED controlled trials, TREATMENT effectiveness, BLIND experiment, PROGNOSIS

Abstract

One course of intravenous immunoglobulins (IVIg) of 2 g/kg is standard treatment in Guillain‐Barré syndrome (GBS) patients unable to walk independently. Despite treatment some patients recover poorly, in part related to rapid consumption of IVIg, indicating that they may benefit from a second course of IVIg. The aim of the study is to determine whether a second course of IVIg, administered 1 week after start of the first course in patients with GBS and predicted poor outcome improves functional outcome on the GBS disability scale after 4 weeks. Secondary outcome measures include adverse events (AEs), Medical Research Council sumscore and GBS disability score after 8, 12, and 26 weeks, length of hospital and ICU admission, mortality, and changes in serum IgG levels. GBS patients of 12 years and older with a poor prognosis, based on the modified Erasmus GBS outcome score (mEGOS) at 1 week after start of the first IVIg course are eligible for randomization in this double‐blind, placebo‐controlled (IVIg or albumin) clinical trial. This study will determine if a second course of IVIg administered in the acute phase of the disease is safe, feasible, and effective in patients with GBS and a poor prognosis. This Dutch trial is registered prospectively as NTR 2224 in the Netherlands National Trial Register (NTR) which is the Primary Registry in the WHO Registry Network for the Netherlands. [ABSTRACT FROM AUTHOR]

Published

2018