2012
DOI: 10.1001/archneurol.2012.1316
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Is It Too Early to Predict the Failure of Natalizumab in NMO?—Reply

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Cited by 7 publications
(6 citation statements)
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“…3 However, relapse prevention remains a challenging issue in NMO because established multiple sclerosis therapies such as interferons, natalizumab, and fingolimod have been reported to show little efficacy or even to be detrimental. [4][5][6] According to smaller case series or retrospective cohort studies, long-term immunosuppression with azathioprine 7 or mycophenolate mofetil 8 is recommended for mild NMO cases, with methotrexate being an alternative treatment option. 3,9 In patients with more severe NMO courses, rituximab 10 and mitoxantrone hydrochoride 11 have been reported to diminish the relapse frequency.…”
mentioning
confidence: 99%
“…3 However, relapse prevention remains a challenging issue in NMO because established multiple sclerosis therapies such as interferons, natalizumab, and fingolimod have been reported to show little efficacy or even to be detrimental. [4][5][6] According to smaller case series or retrospective cohort studies, long-term immunosuppression with azathioprine 7 or mycophenolate mofetil 8 is recommended for mild NMO cases, with methotrexate being an alternative treatment option. 3,9 In patients with more severe NMO courses, rituximab 10 and mitoxantrone hydrochoride 11 have been reported to diminish the relapse frequency.…”
mentioning
confidence: 99%
“…Taking also the previous literature into account, it is apparent that NAT is not beneficial for most patients with NMOSD. 6 8 , 19 24 A review of 19 patients published so far revealed that the majority of patients with NMOSD treated with NAT for at least 3 months deteriorated (table e-2). Moreover, early appearance of severe attacks with atypical cerebral manifestation was noted in a subset of NMO NAT patients.…”
Section: Discussionmentioning
confidence: 99%
“…The first study investigated the initial cohort of 175 NMO patients as to their demographic, clinical and imaging findings with regard to AQP4 serostatus [8]. In parallel, a subgroup of patients in this cohort was identified that was initially misdiagnosed as relapsing-remitting MS and were routinely put on a high-dose MS therapy with natalizumab [14]; despite this, the patients continued to exhibit persistent related disease activity [15,16]. This difficult diagnosis following a somewhat circuitous route was documented in an article on patients who initially underwent a spinal biopsy (which was in some cases not acceptably tolerated) for a suspect-ed malignant spinal tumor, but who in the end had apparent tumefactive longitudinal extensive transverse myelitis (LETM) [17].…”
Section: Scientific Activity and Original Workmentioning
confidence: 99%