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Tytuł:
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Status of the neuromyelitis optica spectrum disorder in Latin America.
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Autorzy:
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Rivera VM; Department of Neurology, Baylor College of Medicine, Houston, Texas, USA.
Hamuy F; Centro Nacional de Esclerosis Multiple, Asuncion, Paraguay.
Rivas V; Instituto Nacional de Neurologia y Neurocirugia 'Manuel Velasco Suarez' (INNN), Mexico City, Mexico.
Gracia F; Hospital Santo Tomas, Panama, Panama.
Rojas JI; Centro de Esclerosis Múltiple de Buenos Aires, Buenos Aires, Argentina.
Bichuetti DB; Universidade Federal de Sao Paulo, Sao Paulo, Brazil.
Villa AM; Hospital Ramos Mejía, Universidad de Buenos Aires, Argentina.
Marques VD; Hospital das Clinicas da Faculdade de Medicina de Ribeirao Preto - USP, Ribeirao Preto, Sao Paulo, Brazil.
Soto A; Centro Medico Docente La Trinidad, Caracas, Venezuela.
Bertado B; lnstituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
Frenk IT; Departamento de Neurología, lnstituto Nacional de Ciencias Médicas y Nutrición 'Salvador Zubirán' (INCMNSZ), Mexico City, Mexico.
Galleguillos L; Clínica Alemana de Santiago, Santiago, Chile.
Quiñones J; Fundación Valle del Lili, Cali, Colombia.
Ramirez DA; Hospital Docente Padre Bellini, Santo Domingo, Dominican Republic.
Caparó-Zamalloa C; Centro Básico de investigación en Demencia y Enfermedades Desmielinizantes del SNC, lnstituto Nacional de Ciencias Neurológicas, Lima, Peru.
Ciampi E; Pontificia Universidad Catolica de Chile y Hospital Dr. Sotero del Rio, Santiago, Chile.
Lana-Peixoto MA; Universidade Federal de Minas Gerais, Belo Horizonte, Brazil.
Rodríguez E; Centro Médico Nacional 'La Raza', IMSS, Mexico City, Mexico.
Zarco L; Pontificia Universidad Javeriana - Hospital Universitario San Ignacio, Bogota, Colombia.
Sinay V; Fundacón Favaloro, Buenos Aires, Argentina.
Armas E; Centro Médico Docente La Trinidad, Caracas, Venezuela.
Becker J; Pontificia Universidade Catolica, Rio Grande do Sul, Porto Alegre, Brazil.
Benzadón A; Caja de Seguro Social, Panama, Panama.
Lopez E; Hospital Rosales, San Salvador, San Salvador.
Carnero Contentti E; Neuroimmunology Unit, Department of Neuroscience, Hospital Aleman, Buenos Aires, Argentina.
Correa-Diaz EP; Hospital Carlos Andrade Marín, Quito, Ecuador.
Diaz A; lnstituto Guatemalteco de Seguridad Social, Guatemala, Guatemala.
Fleitas CV; lnstituto de Previsión Social, Asuncion, Paraguay.
Playas G; Hospital General de Mexico, Mexico City, Mexico.
Molina O; Hospital Universitario de Maracaibo y Policlínica Maracaibo, Maracaibo, Venezuela.
Rojas E; Hospital Nacional EsSalud Guillermo Almenara Irigoyen, Lima, Peru.
Sato D; Pontificia Universidade Catolica do Rio Grande do Sul, Porto Alegre, Brazil.
Soto I; Hospital Clínico de Maracaibo, Maracaibo, Venezuela.
Céspedes JV; Hospital San Juan de Dios, San Jose, Costa Rica.
Correale J; lnstituto Fleni, Buenos Aires, Argentina.
Barboza A; Hospital Central de Mendoza, Mendoza, Argentina.
Monterrey P; Caja Costarricense de Seguro Social, Alajuela, Costa Rica.
Candelario A; Grupo Medico San Martin, Santo Domingo, Dominican Republic.
Tavolini DR; lnstituto de Neurociencias Cognitivas, Neurociencias Orono, Rosario, Argentina.
Parajeles A; Hospital Clínica Bíblica, San Jose, Costa Rica.
Pujol BS; Hospital Regional Universitario Jose María Cabral y Báez, Santiago de los Caballeros, Dominican Republic.
Diaz de la Fe A; Centro Internacional de Restauración Neurológica, CIREN, Habana, Cuba.
Alonso R; Centro Universitario de Esclerosis Multiple, Hospital Ramos Mejía, Buenos Aires, Argentina.
Bolaña C; Hospital Pasteur, Montevideo, Paraguay.
Guzman MK; Clínica Dávila, Santiago, Chile.
Carrá A; Hospital Británico Buenos Aires, Buenos Aires, Argentina.
Gamarra OG; Clínicas Privadas, Lima, Peru.
Raggio JV; Hospital Nacional EsSalud Guillermo Almenara Irigoyen, Lima, Peru.
Rodriguez LC; lnstituto Hondureño De Seguridad Social, Tegucigalpa, Honduras.
Ramirez NE; Hospital Dr. Mario Catarino Rivas, San Pedro Sula, Honduras.
Ordoñez L; Hospital Español de México, Mexico City, Mexico.
Skromne E; lnstituto Mexicano De Neurociencias, State of Mexico, Mexico.
Portillo LL; lnstituto Guatemalteco de Seguridad Social, Guatemala, Guatemala.
Canabal AP; Private Practice, Mayaguez, Puerto Rico.
Weiser R; Hospital Horacio Oduber, Oranjestad, Aruba.
Sirias V; Hospital San Felipe, Tegucigalpa, Honduras.
Calderón RF; Hospital Clinico Magallanes, Punta Arenas, Chile.
Cornejo EA; lnstituto Salvadoreño del Seguro Social, San Salvador, El Salvador.
Hernández M; Clínica Alemana de Santiago, Santiago, Chile.
Quiroz JCD; Neurocentro, La Paz, Bolivia.
Garcia LA; Hospital Militar, Managua, Nicaragua.
Cedeño CO; Caja Costarricense de Seguro Social, Alajuela, Costa Rica.
Martínez J; Hospital Vivian Pellas, Managua, Nicaragua.
Abad-Herrera P; Hospital Metropolitano, Quito, Ecuador.
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Źródło:
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Multiple sclerosis and related disorders [Mult Scler Relat Disord] 2021 Aug; Vol. 53, pp. 103083. Date of Electronic Publication: 2021 Jun 15.
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Typ publikacji:
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Journal Article
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Język:
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English
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Imprint Name(s):
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Original Publication: [Amsterdam] : Elsevier B. V.
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MeSH Terms:
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Neuromyelitis Optica*/epidemiology
Neuromyelitis Optica*/therapy
Aquaporin 4 ; Autoantibodies ; Humans ; Latin America/epidemiology ; Myelin-Oligodendrocyte Glycoprotein ; Neoplasm Recurrence, Local
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Contributed Indexing:
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Keywords: Diagnosis; Latin America; Neuromyelitis optica; Socioeconomic aspects; Therapy
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Substance Nomenclature:
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0 (Aquaporin 4)
0 (Autoantibodies)
0 (Myelin-Oligodendrocyte Glycoprotein)
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Entry Date(s):
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Date Created: 20210625 Date Completed: 20210824 Latest Revision: 20210824
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Update Code:
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20240105
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DOI:
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10.1016/j.msard.2021.103083
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PMID:
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34171682
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Background: Neuromyelitis optica spectrum disorders (NMOSD) is an increasing diagnostic and therapeutic challenge in Latin America (LATAM). Despite the heterogeneity of this population, ethnic and socioeconomic commonalities exist, and epidemiologic studies from the region have had a limited geographic and population outreach. Identification of some aspects from the entire region are lacking.
Objectives: To determine ethnic, clinical characteristics, and utilization of diagnostic tools and types of therapy for patients with NMOSD in the entire Latin American region.
Methods: The Latin American Committee for Treatment and Research in MS (LACTRIMS) created an exploratory investigational survey addressed by Invitation to NMOSD Latin American experts identified through diverse sources. Data input closed after 30 days from the initial invitation. The questionnaire allowed use of absolute numbers or percentages. Multiple option responses covering 25 themes included definition of type of practice; number of NMOSD cases; ethnicity; utilization of the 2015 International Panel criteria for the diagnosis of Neuromyelitis optica (IPDN); clinical phenotypes; methodology utilized for determination of anti-Aquaporin-4 (anti- AQP4) antibodies serological testing, and if this was performed locally or processed abroad; treatment of relapses, and long-term management were surveyed.
Results: We identified 62 investigators from 21 countries reporting information from 2154 patients (utilizing the IPDN criteria in 93.9% of cases), which were categorized in two geographical regions: North-Central, including the Caribbean (NCC), and South America (SA). Ethnic identification disclosed Mestizos 61.4% as the main group. The most common presenting symptoms were concomitant presence of optic neuritis and transverse myelitis in 31.8% (p=0.95); only optic neuritis in 31.4% (more common in SA), p<0.001); involvement of the area postrema occurred in 21.5% and brain stem in 8.3%, both were more frequent in the South American cases (p<0.001). Anti-AQP4 antibodies were positive in 63.9% and anti-Myelin Oligodendrocyte Glycoprotein (MOG) antibodies in 4.8% of total cases. The specific laboratorial method employed was not known by 23.8% of the investigators. Acute relapses were identified in 81.6% of cases, and were treated in 93.9% of them with intravenous steroids (IVS); 62.1% with plasma exchange (PE), and 40.9% with intravenous immunoglobulin-G (IVIG). Therapy was escalated in some cases due to suboptimal initial response. Respondents favored Rituximab as long-term therapy (86.3%), whereas azathioprine was also utilized on 81.8% of the cases, either agent used indistinctly by the investigators according to treatment accessibility or clinical judgement. There were no differences among the geographic regions.
Conclusions: This is the first study including all countries of LATAM and the largest cohort reported from a multinational specific world area. Ethnic distributions and phenotypic features of the disease in the region, challenges in access to diagnostic tools and therapy were identified. The Latin American neurological community should play a determinant role encouraging and advising local institutions and health officials in the availability of more sensitive and modern diagnostic methodology, in facilitating the the access to licensed medications for NMOSD, and addressing concerns on education, diagnosis and management of the disease in the community.
(Copyright © 2021. Published by Elsevier B.V.)
