Transcript Document
חידושים במעקב וטיפול בחולים עם ניוירומיליטיס אופטיקה כנס עידכון בנוירולוגיה 17ביוני 2014 ד"ר עדי וקנין דמבינסקי המרכז לטרשת נפוצה ,המחלקה לנוירולוגיה במרכז הרפואי הדסה עין-כרם ,ירושלים May 19, 2010 Eugene Devic, 1858-1930 Devic described a monophasic illness of bilateral ON and myelitis in quick succession (1873-1936), published in 1894. Patient description: Caucasian female Age 29: Severe visual loss with normal brain and c-spine MRIs Age 30: Para paresis and recurrent ON Exam: no light perception, sheetwhite optic atrophy in one eye, No motor disability Anti AQP4 Abs: positive Neuromyelitis optica Idiopathic, severe, autoimmune demyelinating disease of the CNS that preferentially affects the optic nerve and spinal cord. • Devic’s disease •Common in Africa, east Asia and Latin America More common in women than men a female to male ratio ranging from 3:1 in France to 10:1 in Japan •Median age: 39 •Has been long considered as a variant of Multiple sclerosis. Misdiagnosed patients treated as “severe” MS Neuromyelitis opticaEpidemyology -There are very few epidemiological studies in NMO. -NMO prevalence is estimated between 1 to 4.4/100.000 in the Western world. - There are differences in the regional distribution of NMO worldwide. E.g. – among the cohort of idiopathic demyelinating diseases of the CNS in Thailand, there is a high proportion of AQP4-antibody-positive patients (39%) if compared with European and American cohorts (less than 10%). 2006 Diagnostic Criteria for Neuromyelitis Optica Absolute Criteria (All Required) 1. Optic neuritis 2. Acute myelitis supportive criteria (At least 2-3 ) 1. Negative brain MRI at onset 2. Spinal cord MRI with contiguous T2-weighted signal abnormality extending over 3 or more vertebral segments 3. NMO IgG seropositivity Wingerchuk, D. M. et al. Neurology 2006;66:1485-1489 Neuromyelitis optica – clinical course • NMO is clinically characterized by acute, severe episodes of ON and TM. • The majority of patients have a relapsing disease course. • NMO-IgG seropositivity, in particular, is predictive of a relapsing course • NMO has usually a worse course than that of MS • 50% of untreated will be: • blind in one or both eyes • ambulatory disabled (requiring a wheelchair) within 5 years of disease onset • Morbidity in NMO patients is more directly linked to attacks In NMO, a secondary progressive phase, as seen in MS patients, is uncommon Neuromyelitis optica and other autoimmune diseases Coexisting autoimmune diseases and autoantibodies are frequent in patients with NMO Non organ specific - SLE, Sjogren syndrome Organ specific - thyroid disease, type 1 diabetes, celiac disease and myasthenia gravis. Antinuclear antibodies Autoantibody markers of Sjogren’s syndrome or SLE are found in ~47% of patients with NMOSD. NMO-IgG was not found in patients with Sjogren’s syndrome, or SLE, in the absence of clinical features of NMO Neuromyelitis optica -Imaging Although Negative brain MRI at onset is one of the supporting NMO criteria , About 60%-90 % of the patients will have brain lesions: 10% have “MS-like” brain abnormalities fulfilling Barkof criteria for MS Five (8%). Unique brain involvement: • thalamic or hypothalamic lesions • Medullery lesions Pittock et al, Arch Neurol 2006 Neuromyelitis optica -Imaging NMO LETM lesions often ‘fragment’ into multiple shorter lesions Tackley G et al. Mult Scler 2014;1352458514531087 T1-weighted MRI hypointensities within a LETM in NMO patient. Tackley G et al. Mult Scler 2014; Neuromyelitis optica -Imaging •Currently, MRI monitoring during clinical remission does not appear to be as useful as it is in MS •LETM remains the archetypal MRI lesion of NMO – it is the most specific non-clinical marker for NMO •There is no brain MRI abnormality of comparable specificity for NMO however the absence of Dawson’s fingers and cortical lesions are more typical to MS. •Single longitudinal lesion sometime evolve into multiple shorter spinal lesions. Brain stem lesion sometime resolve •Some patients fulfil MS imaging criteria Pathological and immunopathological findings in neuromyelitis optica (NMO). Jacob A et al. J Neurol Neurosurg Psychiatry Current concept of NMO spectrum disorders (NMOSD) The spectrum of NMO is wider than patients with both ON and TM. The term, NMO spectrum disorders (NMOSD), corresponds to restricted and typical forms of the disorder including : •recurrent optic neuritis •relapsing transverse myelitis •encephalitic presentations, which are common in children. •brainstem disorders (including intractable hiccup and nausea, or vomiting,and hypothalamic disorders (SIADH)) Current concept of NMO spectrum disorders (NMOSD) In NMOSD, especially in patients with brainstem or hypothalamic presentations (in the absence of the opticospinal phenotype) NMO-IgG seropositivity is crucial Characteristics of seronegative NMO SERONEGATIVE SEROPOSITIVE Gender M:F 1:1 1:9 Simultaneous ON&Myelitis ~36% ~3% Other AIs + +++ severity + +++ Mostly monophasic Mostly relapsing Incomplete definitions – over diagnosis of NMO Optic neuritis and partial, short spinal lesions, are usually not NMO even with normal brain MRI ! Criteria should therefore include: • LETM, Sever ON • Unique clinical syndrome – intractable hiccups and nausea. • hypothalamic dysfunction - symptomatic hypersomnia, narcolepsy, and endocrinopathies. • blood pressure fluctuations, vasogenic edema and posterior reversible encephalopathy syndrome. NMO – Hadassah clinical experience Since 1.2013 we tested 489 samples 37 were ANTI AQP4 Abs seropositive 30 CDNMO 3 were with recurrent ON 2 with LETM only 2 were pediatric NMO Out of 280 patients (with available clinical data) 6 CDNMO were Seronegative to AQP4 Treatments of NMO-spectrum disorders • Due to the low disease incidence, so far no clinical study provided evidence for the efficacy of therapeutic regimes. • Therapeutic outcomes of some immunological treatments are different between NMO and MS, making early differential diagnosis of these two disorders crucial • IFNs, Natalizumab and M/P Fingolimod exacerbate NMO Treatments of NMOSD treating the acute relapse Treating ASAP is crucial ! • IV high dose Steroids • Plasmapheresis • IVIG Treatments of NMO/NMOSDpreventive therapy Steroids (monthly courses or oral) Immunosuppressants (Azathioprine mainly; also MTX, Celcept, and cyclophosphamide) Rituximab Monthly Plasmapheresis ? Treatments of NMO/NMOSDpreventive therapy Targeting B-cells B-cell targeting therapies: Rituximab Ocrelizumab Ofatumumab Rituximab: Anti-CD20 Target CD-20 receptor Other names Mabthera Rituxan, and Zytux Rationale B cells involvement in autoimmune diseases – antibody mediated , B cells role as APCs and cytokine production Mode of action The antibody binds to CD20 expressed on B cells, from early pre-B cells to later in differentiation, but absent on terminally differentiated plasma cells. eliminates nearly all CD20-expressing B cells by complement-dependent cytotoxicity (CDC) and ADCC as well as induction of apoptosis Safety and tolerability 28 Severe infusion reaction, cardiac arrest, Infections – PML. resistance development, most likely due to less efficient antibodydependent cytotoxicity or to generation of human antichimeric antibodies (HACA). In the last years, newer generations of “humanized” anti-CD20 antibodies have been generated in order to reduce infusion-related side effects and the risk of HACA development humanized anti-CD20 antibodies Ocrelizumab Ocrelizumab (Roche) is a second-generation humanized anti-CD20 antibody that binds to a different but overlapping epitope compared to rituximab. As it depletes B cells predo- minantly via ADCC, it is considered to exhibit an improved efficacy profile combined with reduced infusionrelated reactions . Ofatumumab Ofatumumab (HuMax-CD20, Arzerra! [Genmab A/S and GlaxoSmithKline]) is a fully humanized anti-CD20 antibody binding to a completely distinct epitope, which results in pro- nounced complement-mediated cytotoxicity Therapy that targets complement Complement mediated damage has been demonstrated both in the brain and spinal cord of NMO patients. Complement bind to the NMOantibody complex inducing membrane-attackcomplex damage and reducing the numbers of aqp4 channels. Therapy that targets complement • A study in 14 NMO patients performed at the Mayo Clinic. A total of 40 attacks in all patients in the last year before study. During treatment, only two patients had slight relapses, 12 patients were completely relapse-free. • The median EDSS score declined from 4.3 to 3.5. • Despite immunization of all participants with tetravalent meningococcal vaccine, one patient developed meningococcal sepsis, from which he completely recovered and resumed treatment with eculizumab. • Eculizumab might be a very effective therapy for patients with highly active NMO. • Currently, there is an ongoing 12 months Phase I/II study in NMO-Ig-positive patients (NCT00904826). The role of B-cell activating factor (BAFF) in myasthenia gravis •B-cell activating factor (BAFF) is important in the differentiation and maturation of B cells and plasma cells. •BAFF may play a significant role in the immune process involved in NMO. •CSF BAFF levels were found to be significantly higher in NMO patients Vaknin-Dembinsky MSJ 2010 Belimumab : Anti-BAFF Target BAFF Other names Anti-BAFF Rationale BAFF- is important in the differentiation and maturation of B cells and plasma cells Mode of action inhibits BAFF action via binding circulating BAFF and reducing the number of circulating B-cells but not to the extent as rituximab Safety and tolerability approved in the US, Canada and Europe for the treatment of systemic lupus erythematosis 34 Monoclonal antibodies targeting cytokines Anti IL-6 antibodies Anti IL-17 antibodies Future directions: anti-IL-6 antibodies • The rationale for employing an IL-6 targeting strategy in NMO is based on the observations that i) NMO patients exhibit significantly elevated IL-6 levels in serum and CSF ii) IL-6 signaling promotes AQP4-autoantibody production in NMO • Recently, one group reported that three rituximabrefractory patients with NMO responded to a therapy with tocilizumab (Actemra®), a mAb against IL-6, which is FDA-approved for treatment of refractory RA Anti IL-17 antibodies • The rationale for employing an IL-17 targeting strategy in NMO is based on the observations that i) T cells derived from NMO patients exhibit Th-17 phenotype (Vaknin-Dembinsky et al Neurology 2012) ii) IL-17 is increased in animal models with NMO pathology • a mAb against IL-17, is currently tested for treatment of refractory RA, psoriasis. Anti IL-17 antibodies Anti IL-17 antibodies Secukinumab - a human antibody that neutralizes IL-17A. TH17 cells are highly involved in the pathogenesis of T-cell-mediated autoimmunity, This antibody already demonstrated promising results in a Phase II trial of psoriasis patients but failed in RA patients. Ixekizumab- humanized IL-17A-neutralizing antibody has recently proven effective in a Phase II trial for treatment of psoriasis. Currently being tested in RA and ankylosing spondylitis. Future and NMO specific strategies Recent experimental strategies, which showed some beneficial effect in animal models in vitro and in vivo •Aquaporumab – a competitive, non-pathogenic AQP4specific antibodies •Sivelestat -Neutrophil elastase inhibitors •Antihistamines with eosinophil-stabilizing actions • Enzymatic AQP4-IgG deglycosylation or cleavage Neuromyelitis optica (NMO) Take home massages : 1. NMO is a devastating disease that cause demyelination, necrosis of optic nerves and spinal cord 2. Associated with systemic and organ specific autoimmune disease (Lupus , Sjögren's syndrome, MG, Celiac etc). 3. Significant residua common 4. Anti AQP4 Abs should be tested in all patients presenting with NMO symptoms (optic neuritis and/or myelitis) as well in malignant MS (With or without other autoimmune diseases,with neoplasia,with atypical ADEM, with unique symptoms - intractable hiccups or vomiting, symptomatic narcolepsy, olfactory dysfunction and neuroendocrine dysfunctions) Neuromyelitis optica (NMO) Take home massages : • • • • • Treatment in the acute relapse should be stated immediately! Preventive therapy in the majority of patients is with steroids and other immunosuppressant medications (AZA,MTX) There is sufficient data to include RITUXIMAB to prevent disease relapse in NMO patients with moderate or severe disease. Other monoclonal antibodies that might have beneficial effect: humanized anti CD20, anti complement, anti BAFF, ant-IL-6,17 Newer approaches: Aquaporumab, enzymatic AQP4IgG deglycosylation or cleavage, Neutrophil elastase inhibitors, Antihistamines with eosinophil-stabilizing actions Neuromyelitis optica (NMO) Unanswered questions : • • • • • • What is the pathogenesis of NMO seronegative? What causing AQP-4 Abs to enter the brain? When and if we can stop therapy with RITUXIMAB Do AQP-4 Abs causing damage in peripheral organs? What is the role of astrocytes in the pathogenesis of NMO? What is the role of AQP4 specific T cells in the pathogenesis of NMO? Thank you!