Clinical presentation and prognosis in MOG-antibody disease: a UK study

Clinical presentation and prognosis in MOG-antibody disease: a UK study

See de Seze (doi:10.1093/brain/awx292) for a scientific commentary on this article. A condition associated with an autoantibody against MOG has been recently recognized as a new inflammatory disease of the central nervous system, but the disease course and disability outcomes are largely unknown. In...

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Veröffentlicht in:Brain (London, England : 1878) England : 1878), 2017-12, Vol.140 (12), p.3128-3138
Hauptverfasser: Jurynczyk, Maciej, Messina, Silvia, Woodhall, Mark R, Raza, Naheed, Everett, Rosie, Roca-Fernandez, Adriana, Tackley, George, Hamid, Shahd, Sheard, Angela, Reynolds, Gavin, Chandratre, Saleel, Hemingway, Cheryl, Jacob, Anu, Vincent, Angela, Leite, M Isabel, Waters, Patrick, Palace, Jacqueline
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Adolescent
Adult
Aged
Aged, 80 and over
Autoantibodies - blood
Child
Child, Preschool
Cohort Studies
Disabled Persons
Female
Humans
Infant
Male
Middle Aged
Myelin-Oligodendrocyte Glycoprotein - blood
Neuromyelitis Optica - blood
Neuromyelitis Optica - diagnosis
Neuromyelitis Optica - epidemiology
Prognosis
United Kingdom - epidemiology
Young Adult
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container_end_page 3138
container_issue 12
container_start_page 3128
container_title Brain (London, England : 1878)
container_volume 140
creator Jurynczyk, Maciej
Messina, Silvia
Woodhall, Mark R
Raza, Naheed
Everett, Rosie
Roca-Fernandez, Adriana
Tackley, George
Hamid, Shahd
Sheard, Angela
Reynolds, Gavin
Chandratre, Saleel
Hemingway, Cheryl
Jacob, Anu
Vincent, Angela
Leite, M Isabel
Waters, Patrick
Palace, Jacqueline
description See de Seze (doi:10.1093/brain/awx292) for a scientific commentary on this article. A condition associated with an autoantibody against MOG has been recently recognized as a new inflammatory disease of the central nervous system, but the disease course and disability outcomes are largely unknown. In this study we investigated clinical characteristics of MOG-antibody disease on a large cohort of patients from the UK. We obtained demographic and clinical data on 252 UK patients positive for serum immunoglobulin G1 MOG antibodies as tested by the Autoimmune Neurology Group in Oxford. Disability outcomes and disease course were analysed in more detail in a cohort followed in the Neuromyelitis Optica Oxford Service (n = 75), and this included an incident cohort who were diagnosed at disease onset (n = 44). MOG-antibody disease affects females (57%) slightly more often than males, shows no ethnic bias and typically presents with isolated optic neuritis (55%, bilateral in almost half), transverse myelitis (18%) or acute disseminated encephalomyelitis-like presentations (18%). In the total Oxford cohort after a median disease duration of 28 months, 47% of patients were left with permanent disability in at least one of the following: 16% patients had visual acuity ≤6/36 in at least one eye, mobility was limited in 7% (i.e. Expanded Disability Status Scale ≥ 4.0), 5% had Expanded Disability Status Scale ≥ 6.0, 28% had permanent bladder issues, 20% had bowel dysfunction, and 21% of males had erectile dysfunction. Transverse myelitis at onset was a significant predictor of long-term disability. In the incident cohort 36% relapsed after median disease duration of 16 months. The annualized relapse rate was 0.2. Immunosuppression longer than 3 months following the onset attack was associated with a lower risk of a second relapse. MOG-antibody disease has a moderate relapse risk, which might be mitigated by medium term immunosuppression at onset. Permanent disability occurs in about half of patients and more often involves sphincter and erectile functions than vision or mobility.
doi_str_mv 10.1093/brain/awx276
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A condition associated with an autoantibody against MOG has been recently recognized as a new inflammatory disease of the central nervous system, but the disease course and disability outcomes are largely unknown. In this study we investigated clinical characteristics of MOG-antibody disease on a large cohort of patients from the UK. We obtained demographic and clinical data on 252 UK patients positive for serum immunoglobulin G1 MOG antibodies as tested by the Autoimmune Neurology Group in Oxford. Disability outcomes and disease course were analysed in more detail in a cohort followed in the Neuromyelitis Optica Oxford Service (n = 75), and this included an incident cohort who were diagnosed at disease onset (n = 44). MOG-antibody disease affects females (57%) slightly more often than males, shows no ethnic bias and typically presents with isolated optic neuritis (55%, bilateral in almost half), transverse myelitis (18%) or acute disseminated encephalomyelitis-like presentations (18%). In the total Oxford cohort after a median disease duration of 28 months, 47% of patients were left with permanent disability in at least one of the following: 16% patients had visual acuity ≤6/36 in at least one eye, mobility was limited in 7% (i.e. Expanded Disability Status Scale ≥ 4.0), 5% had Expanded Disability Status Scale ≥ 6.0, 28% had permanent bladder issues, 20% had bowel dysfunction, and 21% of males had erectile dysfunction. Transverse myelitis at onset was a significant predictor of long-term disability. In the incident cohort 36% relapsed after median disease duration of 16 months. The annualized relapse rate was 0.2. Immunosuppression longer than 3 months following the onset attack was associated with a lower risk of a second relapse. MOG-antibody disease has a moderate relapse risk, which might be mitigated by medium term immunosuppression at onset. 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MOG-antibody disease affects females (57%) slightly more often than males, shows no ethnic bias and typically presents with isolated optic neuritis (55%, bilateral in almost half), transverse myelitis (18%) or acute disseminated encephalomyelitis-like presentations (18%). In the total Oxford cohort after a median disease duration of 28 months, 47% of patients were left with permanent disability in at least one of the following: 16% patients had visual acuity ≤6/36 in at least one eye, mobility was limited in 7% (i.e. Expanded Disability Status Scale ≥ 4.0), 5% had Expanded Disability Status Scale ≥ 6.0, 28% had permanent bladder issues, 20% had bowel dysfunction, and 21% of males had erectile dysfunction. Transverse myelitis at onset was a significant predictor of long-term disability. In the incident cohort 36% relapsed after median disease duration of 16 months. The annualized relapse rate was 0.2. Immunosuppression longer than 3 months following the onset attack was associated with a lower risk of a second relapse. MOG-antibody disease has a moderate relapse risk, which might be mitigated by medium term immunosuppression at onset. Permanent disability occurs in about half of patients and more often involves sphincter and erectile functions than vision or mobility.</description><subject>Adolescent</subject><subject>Adult</subject><subject>Aged</subject><subject>Aged, 80 and over</subject><subject>Autoantibodies - blood</subject><subject>Child</subject><subject>Child, Preschool</subject><subject>Cohort Studies</subject><subject>Disabled Persons</subject><subject>Female</subject><subject>Humans</subject><subject>Infant</subject><subject>Male</subject><subject>Middle Aged</subject><subject>Myelin-Oligodendrocyte Glycoprotein - blood</subject><subject>Neuromyelitis Optica - blood</subject><subject>Neuromyelitis Optica - diagnosis</subject><subject>Neuromyelitis Optica - epidemiology</subject><subject>Prognosis</subject><subject>United Kingdom - epidemiology</subject><subject>Young Adult</subject><issn>0006-8950</issn><issn>1460-2156</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2017</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNo9kDFPwzAQhS0EoqWwMSOPDISeY8ep2VAFBVHUhc7R1b4go9QpcSLaf0-ghemkp09P7z7GLgXcCjByvGrQhzF-bdNcH7GhUBqSVGT6mA0BQCcTk8GAncX4ASCUTPUpG6RGSA1GDNlsWvngLVZ801Ck0GLr68AxuD6o30MdfeQ-8NfFLMHQ-lXtdtz5SBjpjiNfvvDYdm53zk5KrCJdHO6ILR8f3qZPyXwxe57ezxMrTdYmZWpVaiGXFkph0TppZYlSk5rIDBw5tMY6sko4YSgvTWlF7lJFaBVkAHLErve9_brPjmJbrH20VFUYqO5iIYxWef_nJO_Rmz1qmzrGhspi0_g1NrtCQPGjrvhVV-zV9fjVoblbrcn9w3-u5De5_Wwh</recordid><startdate>20171201</startdate><enddate>20171201</enddate><creator>Jurynczyk, Maciej</creator><creator>Messina, Silvia</creator><creator>Woodhall, Mark R</creator><creator>Raza, Naheed</creator><creator>Everett, Rosie</creator><creator>Roca-Fernandez, Adriana</creator><creator>Tackley, George</creator><creator>Hamid, Shahd</creator><creator>Sheard, Angela</creator><creator>Reynolds, Gavin</creator><creator>Chandratre, Saleel</creator><creator>Hemingway, Cheryl</creator><creator>Jacob, Anu</creator><creator>Vincent, Angela</creator><creator>Leite, M Isabel</creator><creator>Waters, Patrick</creator><creator>Palace, Jacqueline</creator><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>20171201</creationdate><title>Clinical presentation and prognosis in MOG-antibody disease: a UK study</title><author>Jurynczyk, Maciej ; 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A condition associated with an autoantibody against MOG has been recently recognized as a new inflammatory disease of the central nervous system, but the disease course and disability outcomes are largely unknown. In this study we investigated clinical characteristics of MOG-antibody disease on a large cohort of patients from the UK. We obtained demographic and clinical data on 252 UK patients positive for serum immunoglobulin G1 MOG antibodies as tested by the Autoimmune Neurology Group in Oxford. Disability outcomes and disease course were analysed in more detail in a cohort followed in the Neuromyelitis Optica Oxford Service (n = 75), and this included an incident cohort who were diagnosed at disease onset (n = 44). MOG-antibody disease affects females (57%) slightly more often than males, shows no ethnic bias and typically presents with isolated optic neuritis (55%, bilateral in almost half), transverse myelitis (18%) or acute disseminated encephalomyelitis-like presentations (18%). In the total Oxford cohort after a median disease duration of 28 months, 47% of patients were left with permanent disability in at least one of the following: 16% patients had visual acuity ≤6/36 in at least one eye, mobility was limited in 7% (i.e. Expanded Disability Status Scale ≥ 4.0), 5% had Expanded Disability Status Scale ≥ 6.0, 28% had permanent bladder issues, 20% had bowel dysfunction, and 21% of males had erectile dysfunction. Transverse myelitis at onset was a significant predictor of long-term disability. In the incident cohort 36% relapsed after median disease duration of 16 months. The annualized relapse rate was 0.2. Immunosuppression longer than 3 months following the onset attack was associated with a lower risk of a second relapse. MOG-antibody disease has a moderate relapse risk, which might be mitigated by medium term immunosuppression at onset. Permanent disability occurs in about half of patients and more often involves sphincter and erectile functions than vision or mobility.</abstract><cop>England</cop><pmid>29136091</pmid><doi>10.1093/brain/awx276</doi><tpages>11</tpages><oa>free_for_read</oa></addata></record>
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source Oxford University Press Journals All Titles (1996-Current); MEDLINE; EZB-FREE-00999 freely available EZB journals; Alma/SFX Local Collection
subjects Adolescent
Adult
Aged
Aged, 80 and over
Autoantibodies - blood
Child
Child, Preschool
Cohort Studies
Disabled Persons
Female
Humans
Infant
Male
Middle Aged
Myelin-Oligodendrocyte Glycoprotein - blood
Neuromyelitis Optica - blood
Neuromyelitis Optica - diagnosis
Neuromyelitis Optica - epidemiology
Prognosis
United Kingdom - epidemiology
Young Adult
title Clinical presentation and prognosis in MOG-antibody disease: a UK study
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