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10.1177/2055217318787829

http://scihub22266oqcxt.onion/10.1177/2055217318787829
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C6050870!6050870!30038790
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suck abstract from ncbi


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pmid30038790      Mult+Scler+J+Exp+Transl+Clin 2018 ; 4 (3): ä
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  • MOG-IgG-associated disease has a stereotypical clinical course, asymptomatic visual impairment and good treatment response #MMPMID30038790
  • Pandit L; Mustafa S; Nakashima I; Takahashi T; Kaneko K
  • Mult Scler J Exp Transl Clin 2018[Jul]; 4 (3): ä PMID30038790show ga
  • Objectives: We investigated the clinical characteristics and treatment response in myelin oligodendrocyte glycoprotein antibody (MOG-IgG)-associated disease and looked for evidence of subclinical disease. Methods: We prospectively evaluated the frequency and pattern of relapse, tested afferent visual function and monitored treatment response in 42 south Asian patients from a single centre. Results: Eighteen patients (42.9%) had monophasic and 24 (57.1%) a relapsing course. Disease duration was longer (P<0.02) in those with a relapsing course. Median time to the second attack was prolonged (P<0.04) in patients with recurrent transverse myelitis when compared with neuromyelitis optica spectrum disorder and recurrent optic neuritis. Thirteen out of 17 patients (76.5%) initially presenting with optic neuritis developed recurrent optic neuritis later. After the first attack of transverse myelitis, 17 out of 22 (77.3%) had disease confined to the spinal cord. Optical coherence tomography detected peripapillary retinal nerve fibre layer thickness (P<0.05) and macular ganglion cell complex volume (P<0.005) abnormalities in seven out of 10 (70.0%) patients without clinical optic neuritis. Immunosuppressants induced remission in 17 out of 22 (77.3%) patients during a median follow-up of 48 months and the median Expanded Disability Status Score was 1 (range 1?10). Conclusion: Our study highlighted the tendency for stereotypical attacks in MOG-IgG-associated disease, heterogeneity in clinical course among subtypes, subclinical visual impairment and the need for early and sustained immunosuppressive therapy.
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