EBV is considered a risk factor in triggering MS. Mounting evidence suggests that EBV-infected immune cells, in particular memory B cells, play an important role in propagating both relapsing and progressive forms of MS. ATA188 offers a novel treatment approach selectively targeting and eliminating EBV-infected B cells and plasma cells in the circulation and central nervous system.
A phase 1a multicentre study assessed safety and efficacy of ATA188 in patients with progressive forms of MS. Patients were treated across 4 dose-escalating cohorts, with 6 patients each in cohorts 1-3 and 7 patients in cohort 4. Across the 4 dose cohorts, ATA188 was well tolerated, with no dose-limiting toxicities or fatal adverse events. Additionally, ATA188 infusion showed no clinically meaningful effect on cytokine levels post-infusion.
Two methods to assess clinical outcomes were used. The first scale was based on Sustained Disability Improvement (SDI), a composite of improvement in Expanded Disability Status Scale (EDSS) or Timed 25-Foot Walk at consecutive time points (3 and 6 months, 6 and 12 months). All patients in cohorts 1-3 showing SDI at 6 months maintained improvement through 12 months (see Table). Additionally, there was a dose-related increase in the number of patients with SDI. The second composite scale (designed to detect early signals of efficacy) was an a priori classification of patient outcomes, incorporating 7 scales for MS symptoms, function, and disability. This scale also showed a dose-related trend of a higher proportion of patients showing favourable clinical improvement. Based on these results, the cohort 3 dose was selected for the randomised, placebo-controlled phase 1b study.
Table. Clinical outcomes and composite scale of SDI in patients receiving ATA188 [1].
m, months; SDI, sustained disability improvement.
- Bar-Or A, et al. Abstract LB130, EAN 2020.
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Table of Contents: EAN 2020
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Alzheimer's Disease and Other Dementias
Non-Alzheimerâs disease pathophysiology in the elderly
Novel genetic association with resistance to ERC tau deposition
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How genetic testing can contribute to epilepsy management
Cenobamate effective in focal epilepsy
Sustained seizure reductions with cannabidiol for Lennox-Gastaut syndrome
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Sleep disorders mark PD progression
Directional DBS superior to omnidirectional DBS
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Migraine as a cyclical functional disorder
Reassuring real-world safety profile of 3 CGRP inhibitors
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Eptinezumab in chronic migraine and medication-overuse headache
Fremanezumab tolerability in cardiovascular patients with migraine
Effects of galcanezumab on health-related quality of life
Multiple Sclerosis
Imaging to evaluate remyelination and neuroprotection
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Epstein-Barr virus-targeted T-cell immunotherapy for progressive MS
High NEDA rates after 2 years of ocrelizumab
Switching from natalizumab to moderate- versus high-efficacy DMT
Results of compounds in late stages of development
Alemtuzumab efficacy and safety data of over 9 years
Fampridine treatment results in routine clinical practice
Air pollution is a possible risk factor for MS
Neuromyelitis Optica Spectrum Disorder
Genetic association studies in NMOSD needed
Eculizumab in NMOSD: the PREVENT study
Long-term safety of satralizumab consistent with double-blind periods
Neuromuscular Disorders
Biomarkers predicting motor function in SMA
Sustained benefits of avalglucosidase alfa in late-onset Pompe disease
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