Your search keyword '"Willison, H.J. (Hugh)"' showing total 14 results

1. 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

2. 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

3. International Guillain-Barré Syndrome Outcome Study: protocol of a prospective observational cohort study on clinical and biological predictors of disease course and outcome in Guillain-Barré syndrome

Author

Jacobs, B.C. (Bart C.), Berg, B. (Bianca) van den, Verboon, C. (Christine), Chavada, G. (Govindsinh), Cornblath, D.R. (David), Gorson, K.C. (Kenneth), Harbo, T. (Thomas), Hartung, H.P., Hughes, R.A.C. (Richard A. C.), Kusunoki, S. (Susumu), Doorn, P.A. (Pieter) van, Willison, H.J. (Hugh J.), Jacobs, B.C. (Bart), Hughes, R.A.C. (Richard), Cornblath, D.R., Gorson, K.C., Kusunoki, S., Willison, H.J. (Hugh), van Woerkom, M., van den Berg, B., Verboon, C., Roodbol, J. (J.), Reisin, R. (R.), Reddel, S.W., Islam, Z. (Zhahirul), Islam, B., Mohammad, Q.D. (Quazi), Bergh, P.Y.K. (Paul) van den, Feasby, T.E., Wang, Y.Z., Harbo, T., Péréon, Y., Lehmann, H.C., Dardiotis, E., Nobile-Orazio, E. (Eduarde), Shahrizaila, N., Jacobs, B.C., Bateman, K., Illa, I. (Isabel), Querol, L. (Luis), Hsieh, S.T., Willison, H.J., Chavada, G., Davidson, A., Addington, J.M., Ajroud-Driss, S., Andersen, H., Antonini, G., Attarian, S., Badrising, U.A. (Umesh), Barroso, F.A., Benedetti, L., Beronio, A., Bianco, M., Binda, D., Briani, C., Bürmann, J., Bella, I.R., Bertorini, T.E., Bhavaraju-Sanka, R., Brannagan, T.H., Busby, M., Butterworth, S., Campagnolo, M., Casasnovas, C., Cavaletti, G., Chao, C.S., Chen, S., Chetty, S., Claeys, T. (Tine), Cohen, J.A., Conti, M.E., Cosgrove, J.S., Dalakas, M.C. (Marinos), Dimachkie, M.M., Dillmann, U., Domínguez González, C., Doppler, K., Dornonville de la Cour, C., Echaniz-Laguna, A., Eftimov, F. (Filip), Faber, C.G., Fazio, R. (R.), Fokke, M. (Maureen), Fujioka, T., Fulgenzi, E. (E.), Galassi, G., Garcia, T., Garnero, M., Garssen, M.P.J. (Marcel), Gijsbers, C.J., Gilchrist, J.M., Gilhuis, J. (Job), Goldstein, J.M., Goyal, N., Granit, V., Grapperon, A., Gutiérrez Gutiérrez, G., Gutmann, L., Hadden, R.D.M. (Rob), Holbech, J.V., Holt, J.K.L., Homedes Pedret, C., Htut, M., Jellema, K., Jericó Pascual, I., Kaida, K.I. (Ken Ichi), Karafiath, S., Katzberg, H. (Hans), Kiers, H.A.L. (Henk), Kieseier, B.C. (Bernd), Kimpinski, K., Kleyweg, R.P., Kokubun, N., Kolb, N.A., Kuitwaard, K. (Krista), Kuwabara, S., Kwan, J.Y., Ladha, S.S., Landschoff Lassen, L., Lawson, V., Ledingham, D., Léon Cejas, L., Luciano, C.A., Lucy, S.T., Lunn, M.P.T. (Michael P. T.), Magot, A., Manji, H., Marchesoni, A., Marfia, G.A.M., Márquez Infante, C., Martinez Hernandez, E., Mataluni, G., Mattiazi, M., McDermott, C.J., Meekins, G.D., Miller, J., Monges, M.S., Montero, M.C.J., Morís de la Tassa, G., Nascimbene, C., Neumann, C., Nowak, R.J., Orizaola Balaguer, P., Osei-Bonsu, M., Pan, E.B.L., Pardo Fernandez, J., Pasnoor, M., Pulley, M.T., Rajabally, Y.A., Rinaldi, S. (Sabina), Ritter, C., Roberts, R.C., Rojas-Marcos, I., Rudnicki, S.A., Sachs, G.M., Samijn, J.P. (Johnny), Santoro, L., Saperstein, D.S., Savransky, A., Schneider, H., Schenone, A. (Andrea), Sedano Tous, M.J., Sekiguchi, Y., Sheikh, K.A., Silvestri, N.J., Sindrup, S.H., Sommer, C., Stein, B., Stino, A.M., Spyropoulos, A., Srinivasan, J., Suzuki, H., Taylor, S.W., Tankisi, H., Tigner, D., Twydell, P.T., Valzania, F., van Damme, P., Kooj, A.J. (Anneke), Dijk, G.W. (Gert) van, van der Ree, T., Koningsveld, R. (Rinske) van, Varrato, J.D., Vermeij, F.H. (Frederique), Verschuuren, J.J. (Jan), Visser, L.H. (Leendert), Vytopil, M.V., Waheed, W., Wilken, M., Wilkerson, C., Wirtz, P.W., Yamagishi, Y., Yiu, E.M., Zhou, L., Zivkovic, S.A. (Sasa), Jacobs, B.C. (Bart C.), Berg, B. (Bianca) van den, Verboon, C. (Christine), Chavada, G. (Govindsinh), Cornblath, D.R. (David), Gorson, K.C. (Kenneth), Harbo, T. (Thomas), Hartung, H.P., Hughes, R.A.C. (Richard A. C.), Kusunoki, S. (Susumu), Doorn, P.A. (Pieter) van, Willison, H.J. (Hugh J.), Jacobs, B.C. (Bart), Hughes, R.A.C. (Richard), Cornblath, D.R., Gorson, K.C., Kusunoki, S., Willison, H.J. (Hugh), van Woerkom, M., van den Berg, B., Verboon, C., Roodbol, J. (J.), Reisin, R. (R.), Reddel, S.W., Islam, Z. (Zhahirul), Islam, B., Mohammad, Q.D. (Quazi), Bergh, P.Y.K. (Paul) van den, Feasby, T.E., Wang, Y.Z., Harbo, T., Péréon, Y., Lehmann, H.C., Dardiotis, E., Nobile-Orazio, E. (Eduarde), Shahrizaila, N., Jacobs, B.C., Bateman, K., Illa, I. (Isabel), Querol, L. (Luis), Hsieh, S.T., Willison, H.J., Chavada, G., Davidson, A., Addington, J.M., Ajroud-Driss, S., Andersen, H., Antonini, G., Attarian, S., Badrising, U.A. (Umesh), Barroso, F.A., Benedetti, L., Beronio, A., Bianco, M., Binda, D., Briani, C., Bürmann, J., Bella, I.R., Bertorini, T.E., Bhavaraju-Sanka, R., Brannagan, T.H., Busby, M., Butterworth, S., Campagnolo, M., Casasnovas, C., Cavaletti, G., Chao, C.S., Chen, S., Chetty, S., Claeys, T. (Tine), Cohen, J.A., Conti, M.E., Cosgrove, J.S., Dalakas, M.C. (Marinos), Dimachkie, M.M., Dillmann, U., Domínguez González, C., Doppler, K., Dornonville de la Cour, C., Echaniz-Laguna, A., Eftimov, F. (Filip), Faber, C.G., Fazio, R. (R.), Fokke, M. (Maureen), Fujioka, T., Fulgenzi, E. (E.), Galassi, G., Garcia, T., Garnero, M., Garssen, M.P.J. (Marcel), Gijsbers, C.J., Gilchrist, J.M., Gilhuis, J. (Job), Goldstein, J.M., Goyal, N., Granit, V., Grapperon, A., Gutiérrez Gutiérrez, G., Gutmann, L., Hadden, R.D.M. (Rob), Holbech, J.V., Holt, J.K.L., Homedes Pedret, C., Htut, M., Jellema, K., Jericó Pascual, I., Kaida, K.I. (Ken Ichi), Karafiath, S., Katzberg, H. (Hans), Kiers, H.A.L. (Henk), Kieseier, B.C. (Bernd), Kimpinski, K., Kleyweg, R.P., Kokubun, N., Kolb, N.A., Kuitwaard, K. (Krista), Kuwabara, S., Kwan, J.Y., Ladha, S.S., Landschoff Lassen, L., Lawson, V., Ledingham, D., Léon Cejas, L., Luciano, C.A., Lucy, S.T., Lunn, M.P.T. (Michael P. T.), Magot, A., Manji, H., Marchesoni, A., Marfia, G.A.M., Márquez Infante, C., Martinez Hernandez, E., Mataluni, G., Mattiazi, M., McDermott, C.J., Meekins, G.D., Miller, J., Monges, M.S., Montero, M.C.J., Morís de la Tassa, G., Nascimbene, C., Neumann, C., Nowak, R.J., Orizaola Balaguer, P., Osei-Bonsu, M., Pan, E.B.L., Pardo Fernandez, J., Pasnoor, M., Pulley, M.T., Rajabally, Y.A., Rinaldi, S. (Sabina), Ritter, C., Roberts, R.C., Rojas-Marcos, I., Rudnicki, S.A., Sachs, G.M., Samijn, J.P. (Johnny), Santoro, L., Saperstein, D.S., Savransky, A., Schneider, H., Schenone, A. (Andrea), Sedano Tous, M.J., Sekiguchi, Y., Sheikh, K.A., Silvestri, N.J., Sindrup, S.H., Sommer, C., Stein, B., Stino, A.M., Spyropoulos, A., Srinivasan, J., Suzuki, H., Taylor, S.W., Tankisi, H., Tigner, D., Twydell, P.T., Valzania, F., van Damme, P., Kooj, A.J. (Anneke), Dijk, G.W. (Gert) van, van der Ree, T., Koningsveld, R. (Rinske) van, Varrato, J.D., Vermeij, F.H. (Frederique), Verschuuren, J.J. (Jan), Visser, L.H. (Leendert), Vytopil, M.V., Waheed, W., Wilken, M., Wilkerson, C., Wirtz, P.W., Yamagishi, Y., Yiu, E.M., Zhou, L., and Zivkovic, S.A. (Sasa)

Abstract

Guillain-Barré syndrome (GBS) is an acute polyradiculoneuropathy with a highly variable clinical presentation, course, and outcome. The factors that determine the clinical variation of GBS are poorly understood which complicates the care and treatment of individual patients. The protocol of the ongoing International GBS Outcome Study (IGOS), a prospective, observational, multicenter cohort study that aims to identify the clinical and biological determinants and predictors of disease onset, subtype, course and outcome of GBS is presented here. Patients fulfilling the diagnostic criteria for GBS, regardless of age, disease severity, variant forms, or treatment, can participate if included within 2 weeks after onset of weakness. Information about demography, preceding infections, clinical features, diagnostic findings, treatment, course, and outcome is collected. In addition, cerebrospinal fluid and serial blood samples for serum and DNA is collected at standard time points. The original aim was to include at least 1,000 patients with a follow-up of 1–3 years. Data are collected via a web-based data entry system and stored anonymously. IGOS started in May 2012 and by January 2017 included more than 1,400 participants from 143 active centers in 19 countries across 5 continents. The IGOS data/biobank is available for research projects conducted by expertise groups focusing on specific topics including epidemiology, diagnostic criteria, clinimetrics, electrophysiology, antecedent events, antibodies, genetics, prognostic modeling, treatment effects, and long-term outcome of GBS. The IGOS will help to standardize the international collection of data and biosamples for future research of GBS.

Published

2017

4. 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

5. ZikaPLAN: addressing the knowledge gaps and working towards a research preparedness network in the Americas

Author

Wilder-Smith, A. (Annelies), Preet, R. (Raman), Brickley, E.B. (Elizabeth B.), Ximenes, R.A.A. (Ricardo Arraes de Alencar), Miranda-Filho, D.B. (Demócrito de Barros), Turchi Martelli, C.M. (Celina Maria), Araújo, T.V.B. (Thália Velho Barreto de), Montarroyos, U.R. (Ulisses Ramos), Moreira, M.E. (Maria Elisabeth), Turchi, M.D. (Marília Dalva), Solomon, T. (Tom), Jacobs, B.C. (Bart), Villamizar, C.P. (Carlos Pardo), Osorio, L. (Lyda), de Filipps, A.M.B. (Ana Maria Bispo), Neyts, J., Kaptein, S.J.F. (Suzanne), Huits, R.M.H.G. (Ralph M. H. G.), Ariën, K.K. (Kevin K.), Willison, H.J. (Hugh), Edgar, J. (Julia), Barnett, S.C. (Susan C.), Peeling, R. (Rosanna), Boeras, D. (Debi), Guzman, M.G. (Maria G.), de Silva, A.M. (Aravinda M.), Falconar, A., Romero-Vivas, C. (Claudia), Gaunt, M.W. (Michael W.), Sette, A. (Alessandro), Weiskopf, D. (Daniela), Lambrechts, L. (Louis), Dolk, H. (Helen), Morris, J.K. (Joan K.), Orioli, I.M. (Ieda M.), O'Reilly, K.M. (Kathleen M.), Yakob, L. (Laith), Rocklöv, J. (Joacim), Soares, C. (Cristiane), Ferreira, M.L.B. (Maria Lúcia Brito), Franca, R.F.O. (Rafael Freitas de Oliveira), Precioso, A.R. (Alexander R.), Logan, J. (James), Lang, T. (Trudie), Jamieson, N. (Nina), Massad, E. (Eduardo), Wilder-Smith, A. (Annelies), Preet, R. (Raman), Brickley, E.B. (Elizabeth B.), Ximenes, R.A.A. (Ricardo Arraes de Alencar), Miranda-Filho, D.B. (Demócrito de Barros), Turchi Martelli, C.M. (Celina Maria), Araújo, T.V.B. (Thália Velho Barreto de), Montarroyos, U.R. (Ulisses Ramos), Moreira, M.E. (Maria Elisabeth), Turchi, M.D. (Marília Dalva), Solomon, T. (Tom), Jacobs, B.C. (Bart), Villamizar, C.P. (Carlos Pardo), Osorio, L. (Lyda), de Filipps, A.M.B. (Ana Maria Bispo), Neyts, J., Kaptein, S.J.F. (Suzanne), Huits, R.M.H.G. (Ralph M. H. G.), Ariën, K.K. (Kevin K.), Willison, H.J. (Hugh), Edgar, J. (Julia), Barnett, S.C. (Susan C.), Peeling, R. (Rosanna), Boeras, D. (Debi), Guzman, M.G. (Maria G.), de Silva, A.M. (Aravinda M.), Falconar, A., Romero-Vivas, C. (Claudia), Gaunt, M.W. (Michael W.), Sette, A. (Alessandro), Weiskopf, D. (Daniela), Lambrechts, L. (Louis), Dolk, H. (Helen), Morris, J.K. (Joan K.), Orioli, I.M. (Ieda M.), O'Reilly, K.M. (Kathleen M.), Yakob, L. (Laith), Rocklöv, J. (Joacim), Soares, C. (Cristiane), Ferreira, M.L.B. (Maria Lúcia Brito), Franca, R.F.O. (Rafael Freitas de Oliveira), Precioso, A.R. (Alexander R.), Logan, J. (James), Lang, T. (Trudie), Jamieson, N. (Nina), and Massad, E. (Eduardo)

Abstract

Zika Preparedness Latin American Network (ZikaPLAN) is a research consortium funded by the European Commission to address the research gaps in combating Zika and to establish a sustainable network with research capacity building in the Americas. Here we present a report on ZikaPLAN`s mid-term achievements since its initiation in October 2016 to June 2019, illustrating the research objectives of the 15 work packages ranging from virology, diagnostics, entomology and vector control, modelling to clinical cohort studies in pregnant women and neonates, as well as studies on the neurological complications of Zika infections in adolescents and adults. For example, the Neuroviruses Emerging in the Americas Study (NEAS) has set up more than 10 clinical sites in Colombia. Through the Butantan Phase 3 dengue vaccine trial, we have access to samples of 17,000 subjects in 14 different geographic locations in Brazil. To address the lack of access to clinical samples for diagnostic evaluation, ZikaPLAN set up a network of quality sites with access to well-characterized clinical specimens and capacity for independent evaluations. The International Committee for Congenital Anomaly Surveillance Tools was formed with global representation from regional networks conducting birth defects surveillance. We have collated a comprehensive inventory of resources and tools for birth defects surveillance, and developed an App for low resource regions facilitating the coding and description of all major externally visible congenital anomalies including congenital Zika syndrome. Research Capacity Network (REDe) is a shared and open resource centre where researchers and health workers can access tools, resources and support, enabling better and more research in the region. Addressing the gap in research capacity in LMICs is pivotal in ensuring broad-based systems to be prepared for the next outbreak. Our shared and open research space through REDe will be used to maximize the transfer of research

Published

2019

6. 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

7. Inhibition of complement in Guillain-Barré syndrome: the ICA-GBS study

Author

Davidson, A.I. (Amy I.), Halstead, S.K. (Susan), Goodfellow, J.A. (John A.), Chavada, G. (Govind), Mallik, A. (Arup), Overell, J. (James), Lunn, M.P.T. (Michael P. T.), McConnachie, A. (Alex), Doorn, P.A. (Pieter) van, Willison, H.J. (Hugh), Davidson, A.I. (Amy I.), Halstead, S.K. (Susan), Goodfellow, J.A. (John A.), Chavada, G. (Govind), Mallik, A. (Arup), Overell, J. (James), Lunn, M.P.T. (Michael P. T.), McConnachie, A. (Alex), Doorn, P.A. (Pieter) van, and Willison, H.J. (Hugh)

Abstract

The outcome of Guillain-Barré syndrome (GBS) remains unchanged since plasma exchange and intravenous immunoglobulin (IVIg) were introduced over 20 years ago. Pathogenesis studies on GBS have identified the terminal component of complement cascade as a key disease mediator and therapeutic target. We report the first use of terminal complement pathway inhibition with eculizumab in humans with GBS. In a randomised, double-blind, placebo-controlled trial, 28 subjects eligible on the basis of GBS disability grade of at least 3 were screened, of whom 8 (29%) were randomised. Five received eculizumab for 4 weeks, alongside standard IVIg treatment. The safety outcomes, monitored via adverse events capture, showed eculizumab to be well-tolerated and safe when administered in conjunction with IVIg. Primary and secondary efficacy outcomes in the form of GBS disability scores (GBS DS), MRC sum scores, Rasch overall disability scores, and overall neuropathy limitation scores are reported descriptively. For the primary efficacy outcome at 4 weeks after recruitment, two of two placebo- and two of five eculizumab-treated subjects had improved by one or more grades on the GBS DS. Although the small sample size precludes a statistically meaningful analysis, these pilot data indicate further studies on complement inhibition in GBS are warranted.

Published

2017

8. Microarray screening of Guillain-Barré syndrome sera for antibodies to glycolipid complexes

Author

Halstead, S.K. (Susan), Kalna, G. (Gabriela), Islam, M.B. (Mohammad B.), Jahan, I. (Israt), Mohammad, Q.D. (Quazi), Jacobs, B.C. (Bart), Endtz, H.P. (Hubert), Islam, Z. (Zhahirul), Willison, H.J. (Hugh), Halstead, S.K. (Susan), Kalna, G. (Gabriela), Islam, M.B. (Mohammad B.), Jahan, I. (Israt), Mohammad, Q.D. (Quazi), Jacobs, B.C. (Bart), Endtz, H.P. (Hubert), Islam, Z. (Zhahirul), and Willison, H.J. (Hugh)

Abstract

__Objective:__ To characterize the patterns of autoantibodies to glycolipid complexes in a large cohort of Guillain-Barré syndrome (GBS) and control samples collected in Bangladesh using a newly developed microarray technique. __Methods:__ Twelve commonly studied glycolipids and lipids, plus their 66 possible heteromeric complexes, totaling 78 antigens, were applied to polyvinylidene fluoride-coated slides using a microarray printer. Arrays were probed with 266 GBS and 579 control sera (2 mL per serum, diluted 1/50) and bound immunoglobulin G detected with secondary antibody. Scanned arrays were subjected to statistical analyses. __Results:__ Measuring antibodies to single targets was 9% less sensitive than to heteromeric complex targets (49.2% vs 58.3%) without significantly affecting specificity (83.9% 85.0%). The optimal screening protocol for GBS sera comprised a panel of 10 glycolipids (4 single glycolipids GM1, GA1, GD1a, GQ1b, and their 6 heteromeric complexes), resulting in an overall assay sensitivity of 64.3% and specificity of 77.1%. Notable heteromeric targets were GM1:GD1a, GM1:GQ1b, and GA1:GD1a, in which exclusive binding to the complex was observed. __Conclusions:__ Rationalizing the screening protocol to capture the enormous diversity of glycolipid complexes can be achieved by miniaturizing the screening platform to a microarray platform, and applying simple bioinformatics to determine optimal sensitivity and specificity of the targets. Glycolipid complexes are an important category of glycolipid antigens in autoimmune neuropathy cases that require specific analytical and bioinformatics methods for optimal detection.

Published

2016

9. Antibodies to heteromeric glycolipid complexes in guillain-barré syndrome

Author

Rinaldi, S. (Simon), Brennan, K.M. (Kathryn), Kalna, G. (Gabriela), Walgaard, C. (Christa), Doorn, P.A. (Pieter) van, Jacobs, B.C. (Bart), Yu, R.K. (Robert), Mansson, J.-E. (Jan-Eric), Goodyear, C.S. (Carl), Willison, H.J. (Hugh), Rinaldi, S. (Simon), Brennan, K.M. (Kathryn), Kalna, G. (Gabriela), Walgaard, C. (Christa), Doorn, P.A. (Pieter) van, Jacobs, B.C. (Bart), Yu, R.K. (Robert), Mansson, J.-E. (Jan-Eric), Goodyear, C.S. (Carl), and Willison, H.J. (Hugh)

Abstract

Autoantibodies are infrequently detected in the sera of patients with the demyelinating form of Guillain-Barré syndrome most commonly encountered in the Western world, despite abundant circumstantial evidence suggesting their existence. We hypothesised that antibody specificities reliant on the cis interactions of neighbouring membrane glycolipids could explain this discrepancy, and would not have been detected by traditional serological assays using highly purified preparations of single gangliosides. To assess the frequency of glycolipid complex antibodies in a Western European cohort of patients GBS we used a newly developed combinatorial glycoarray methodology to screen against large range of antigens (11 gangliosides, 8 other single glycolipids and 162 heterodimeric glycolipid complexes). Serum samples of 181 patients from a geographically defined, Western European cohort of GBS cases were analysed, along with 161 control sera. Serum IgG binding to single gangliosides was observed in 80.0% of axonal GBS cases, but in only 11.8% of cases with demyelinating electrophysiology. The inclusion of glycolipid complexes increased the positivity rate in demyelinating disease to 62.4%. There were 40 antigens with statistically significantly increased binding intensities in GBS as compared to healthy control sera. Of these, 7 complex antigens and 1 single ganglioside also produced statistically significantly increased binding intensities in GBS versus neurological disease controls. The detection of antibodies against specific complexes was associated with particular clinical features including disease severity, requirement for mechanical ventilation, and axonal electrophysiology. This study demonstrates that while antibodies against single gangliosides are often found in cases with axonal-type electrophysiology, antibodies against glycolipid complexes predominate in cases with demyelinating electrophysiology, providing a more robust serum biomarker than has ever been previ

Published

2013

10. Sialylation of campylobacter jejuni lipo-oligosaccharides: Impact on phagocytosis and cytokine production in mice

Author

Huizinga, R. (Ruth), Easton, A.S. (Alistair), Donachie, A.M. (Anne), Guthrie, J. (Jim), Rijs, W. (Wouter) van, Heikema, A.P. (Astrid), Boon, L. (Louis), Samsom, J.N. (Janneke), Jacobs, B.C. (Bart), Willison, H.J. (Hugh), Goodyear, C.S. (Carl), Huizinga, R. (Ruth), Easton, A.S. (Alistair), Donachie, A.M. (Anne), Guthrie, J. (Jim), Rijs, W. (Wouter) van, Heikema, A.P. (Astrid), Boon, L. (Louis), Samsom, J.N. (Janneke), Jacobs, B.C. (Bart), Willison, H.J. (Hugh), and Goodyear, C.S. (Carl)

Abstract

Background: Guillain-Barré syndrome (GBS) is a post-infectious polyradiculoneuropathy, frequently associated with antecedent Campylobacter jejuni (C. jejuni) infection. The presence of sialic acid on C. jejuni lipo-oligosaccharide (LOS) is considered a risk factor for development of GBS as it crucially determines the structural homology between LOS and gangliosides, explaining the induction of cross-reactive neurotoxic antibodies. Sialylated C. jejuni are recognised by TLR4 and sialoadhesin; however, the functional implications of these interactions in vivo are unknown. Methodology/Principal Findings: In this study we investigated the effects of bacterial sialylation on phagocytosis and cytokine secretion by mouse myeloid cells in vitro and in vivo. Using fluorescently labelled GM1a/GD1a ganglioside-mimicking C. jejuni strains and corresponding (Cst-II-mutant) control strains lacking sialic acid, we show that sialylated C. jejuni was more efficiently phagocytosed in vitro by BM-MΦ, but not by BM-DC. In addition, LOS sialylation increased the production of IL-10, IL-6 and IFN-β

Published

2012

11. Eculizumab prevents anti-ganglioside antibody-mediated neuropathy in a murine model

Author

Halstead, S.K. (Susan), Zitman, F.M.P. (Femke), Humphreys, P.D. (Peter), Greenshields, K. (Kay), Verschuuren, J.J. (Jan), Jacobs, B.C. (Bart), Rother, R.P. (Russell), Plomp, J.J. (Jaap), Willison, H.J. (Hugh), Halstead, S.K. (Susan), Zitman, F.M.P. (Femke), Humphreys, P.D. (Peter), Greenshields, K. (Kay), Verschuuren, J.J. (Jan), Jacobs, B.C. (Bart), Rother, R.P. (Russell), Plomp, J.J. (Jaap), and Willison, H.J. (Hugh)

Abstract

Anti-GQ1b ganglioside antibodies are the serological hallmark of the Miller Fisher syndrome (MFS) variant of the paralytic neuropathy, Guillain- Barré syndrome, and are believed to be the principal pathogenic mediators of the disease. In support of this, we previously showed in an in vitro mouse model of MFS that anti-GQ1b antibodies were able to bind and disrupt presynaptic motor nerve terminals at the neuromuscular junction (NMJ) as one of their target sites, thereby causing muscle paralysis. This injury only occurred through activation of complement, culminating in the formation and deposition of membrane attack complex (MAC, C5b-9) in nerve membranes. Since this step is crucial to the neuropathic process and an important convergence point for antibody and complement mediated membrane injury in general, it forms an attractive pharmacotherapeutic target. Here, we assessed the efficacy of the humanized monoclonal antibody eculizumab, which blocks the formation of human C5a and C5b-9, in preventing the immune-mediated motor neuropathy exemplified in this model. Eculizumab completely prevented electrophysiological and structural lesions at anti-GQ1b antibody pre-incubated NMJs in vitro when using normal human serum (NHS) as a complement source. In a novel in vivo mouse model of MFS generated through intraperitoneal injection of anti-GQ1b antibody and NHS, mice developed respiratory paralysis due to transmission block at diaphragm NMJs, resulting from anti-GQ1b antibody binding and complement activation. Intravenous injection of eculizumab effectively prevented respiratory paralysis and associated functional and morphological hallmarks of terminal motor neuropathy. We show that eculizumab protects against complement-mediated damage in murine MFS, providing the rationale for undertaking clinical trials in this disease and other antibody-mediated neuropathies in which complement activation is believed to be involved.

Published

2008

12. Immunoglobulins inhibit pathophysiological effects of anti-GQ1b-positive sera at motor nerve terminals through inhibition of antibody binding.

Author

Jacobs, B.C. (Bart), O' Hanlon, G.M. (Graham), Bullens, R.W. (Roland), Veitch, J. (Jean), Plomp, J.J. (Jaap), Willison, H.J. (Hugh), Jacobs, B.C. (Bart), O' Hanlon, G.M. (Graham), Bullens, R.W. (Roland), Veitch, J. (Jean), Plomp, J.J. (Jaap), and Willison, H.J. (Hugh)

Abstract

High-dose intravenous immunoglobulin (IVIg) is an effective treatment for many antibody-mediated neuromuscular diseases, suggesting that IVIg directly interferes with the pathways through which the pathogenic antibodies exert their effects. However, the precise mechanisms of action are unclear. Serum anti-GQ1b antibodies are stron

Published

2003

13. Structure of Campylobacter jejuni lipopolysaccharides determines antiganglioside specificity and clinical features of Guillain-Barré and Miller Fisher patients

Author

Ang, C.W. (Wim), Laman, J.D. (Jon), Willison, H.J. (Hugh), Wagner, E.R., Endtz, H.P. (Hubert), Klerk, M.A. de, Tio-Gillen, A.P. (Anne), Braak, N.P.W.C.J. (Nicole) van den, Jacobs, B.C. (Bart), Doorn, P.A. (Pieter) van, Ang, C.W. (Wim), Laman, J.D. (Jon), Willison, H.J. (Hugh), Wagner, E.R., Endtz, H.P. (Hubert), Klerk, M.A. de, Tio-Gillen, A.P. (Anne), Braak, N.P.W.C.J. (Nicole) van den, Jacobs, B.C. (Bart), and Doorn, P.A. (Pieter) van

Abstract

Ganglioside mimicry in the lipopolysaccharide (LPS) fraction of Campylobacter jejuni isolated from Guillain-Barre syndrome (GBS) and Miller Fisher syndrome (MFS) patients was compared with isolates from patients with an uncomplicated enteritis. The antibody response to C. jejuni LPS and gangliosides in neuropathy patients and controls was compared as well. LPS from GBS and MFS-associated isolates more frequently contained ganglioside-like epitopes compared to control isolates. Almost all neuropathy patients showed a strong antibody response against LPS and multiple gangliosides in contrast to enteritis patients. Isolates from GBS patients more frequently had a GM1-like epitope than isolates from MFS patients. GQ1b-like epitopes were present in all MFS-associated isolates and was associated with anti-GQ1b antibody reactivity and the presence of oculomotor symptoms. These results demonstrate that the expression of ganglioside mimics is a risk factor for the development of post-Campylobacter neuropathy. This study provides additional evidence for the hypothesis that the LPS fraction determines the antiganglioside specificity and clinical features in post-Campylobacter neuropathy patients.

Published

2002

14. Human IgM paraproteins demonstrate shared reactivity between Campylobacter jejuni lipopolysaccharides and human peripheral nerve disialylated gangliosides

Author

Jacobs, B.C. (Bart), O'Hanlon, S. (Simon), Breedland, E.G. (Elvera), Veitch, J. (Jean), Doorn, P.A. (Pieter) van, Willison, H.J. (Hugh), Jacobs, B.C. (Bart), O'Hanlon, S. (Simon), Breedland, E.G. (Elvera), Veitch, J. (Jean), Doorn, P.A. (Pieter) van, and Willison, H.J. (Hugh)

Published

1997