Memory B Cells are Major Targets for Effective Immunotherapy in Relapsing Multiple Sclerosis

Baker, David; Marta, Mónica; Pryce, Gareth; Giovannoni, Gavin; Schmierer, Klaus

doi:10.1016/j.ebiom.2017.01.042

Cited by 229 publications

(273 citation statements)

References 97 publications

(217 reference statements)

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“…Disease-driving lymphocytes, including B-cells, are believed to migrate to the CSF and CNS from peripheral stores during phases of MS disease activity (8,11,12). Due to their immunological properties and functionality, SM B-cells are generally believed to be highly relevant to the immune pathology of MS (35). Indeed, when persistent PB SM cells were clonally related to second time-point CSF B-cells, these T2-CSF cells were nearly always SM and PC.…”

Section: Discussionmentioning

confidence: 99%

Longitudinally persistent cerebrospinal fluid B-cells resist treatment in multiple sclerosis

Greenfield

Dandekar

Ramesh

et al. 2018

Preprint

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B-cells are key contributors to chronic autoimmune pathology in multiple sclerosis (MS). Clonally related B-cells exist in the cerebrospinal fluid (CSF), meninges, and central nervous system (CNS) parenchyma of MS patients. Longitudinally stable CSF oligoclonal band (OCB) antibody patterns suggest some local CNS B-cell persistence; however, the longitudinal B-cell dynamics within and between the CSF and blood remain unknown. We sought to address this by performing immunoglobulin heavy chain variable region repertoire sequencing on B-cells from longitudinally collected blood and CSF samples of MS patients (n=10). All patients were untreated at the time of the initial sampling; the majority (n=7) were treated with immune modulating therapies 1.2 (+/-0.3 SD) years later during the second sampling. We found clonal persistence of B-cells in the CSF of five patients; these B-cells were frequently immunoglobulin (Ig) classswitched and CD27+. We identified specific blood B-cell subsets that appear to provide input into CNS repertoires over time. We demonstrate complex patterns of clonal B-cell persistence in CSF and blood, even in patients on high-efficacy immune modulating therapy. Our findings support the concept that peripheral B-cell activation and CNS-compartmentalized immune mechanisms are in part therapy-resistant.

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Section: Discussionmentioning

confidence: 99%

Longitudinally persistent cerebrospinal fluid B-cells resist treatment in multiple sclerosis

Greenfield

Dandekar

Ramesh

et al. 2018

Preprint

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“…We selected Cladribine for the following reasons: (1) class I evidence of efficacy of the active compound in people with relapsing MS10, 15, 22; (2) selective lymphocyte mechanism of action not requiring cell‐proliferation and notably B cell targeting potential that appears to be associated with effective control of active MS23, 24; (3) CNS penetration for peripheral and CNS immune cell inactivation and modulation16, 23; (4) safety comparable or better than similarly effective, current treatments12; (5) known relative safety in people with advanced MS15; (6) induction therapy potential requiring only short courses of treatment10 with rapid elimination from the body potentially allowing additional use of neuroprotection and symptomatic treatments without complications due to drug‐drug interactions23; and importantly, (7) convenience for the patient with easy and rapid administration during brief hospital visits to our day case unit, and few monitoring needs compared to some of the current DMT. This will limit travel requirements for someone restricted to a wheelchair.…”

Section: Discussionmentioning

confidence: 99%

Cladribine to treat disease exacerbation after fingolimod discontinuation in progressive multiple sclerosis

Alvarez-Gonzalez

Adams

Mathews

et al. 2017

Ann Clin Transl Neurol

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Rebound disease following cessation of disease modifying treatment (DMT) has been reported in people with both relapsing and progressive multiple sclerosis (pwRMS, pwPMS) questioning strict separation between these two phenotypes. While licensed DMT is available for pwRMS to counter rebound disease, no such option exists for pwPMS. We report on a pwPMS who developed rebound disease, with 45 Gadolinium‐enhancing lesions on T1 weighted MRI brain, within 6 months after fingolimod 0.5 mg/day was stopped. Treatment with a short course of subcutaneous cladribine 60 mg led to effective suppression of inflammatory activity and partial recovery with no short‐term safety issues or adverse events.

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“…Decreased frequency of B cells following treatment with DMF has been reported by several investigators (Chaves et al, ; Claes et al, ; Diebold et al, ; Fleischer et al, ). It has been shown that DMF preferentially targets the B memory cells, which are worthy targets for MS immunotherapy (Baker et al, ; Smith et al, ). Although DMF reduced the incidence of CD27 + IgD memory B cells it increased the incidence of CD27 ‐ IgD + naıve B cells (Smith et al, ).…”

Section: Mechanism(s) Of Dmf Actionmentioning

confidence: 99%

Dimethyl fumarate: Regulatory effects on the immune system in the treatment of multiple sclerosis

Hosseini

Masjedi

Baradaran

et al. 2018

Journal Cellular Physiology

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Dimethyl fumarate (DMF) is an important oral treatment option for various autoimmune diseases, such as multiple sclerosis (MS) and psoriasis. DMF and its dynamic metabolite, monomethyl fumarate (MMF) are the major compounds that exert therapeutic effects on several pathologic conditions in part, through downregulation of immune responses. The exact mechanism of DMF is yet to be fully understood even though its beneficial effects on the immune system are extensively studied. It has been shown that DMF/MMF can affect various immune cells, which can get involved in both the naive and adaptive immune systems, such as T cells, B cells, dendritic cells, macrophages, neutrophils, and natural killer cells. It is suggested that DMF/MMF may exert their effect on immune cells through inhibition of nuclear factor‐κB translocation, upregulation of nuclear factor erythroid‐derived 2(E2)‐related factor antioxidant pathway, and activation of hydroxyl carboxylic acid receptor 2. In this review, the mechanisms underlying the modulatory functions of DMF or MMF on the main immune cell populations involved in the immunopathogenesis of MS are discussed.

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Memory B Cells are Major Targets for Effective Immunotherapy in Relapsing Multiple Sclerosis

Cited by 229 publications

References 97 publications

Longitudinally persistent cerebrospinal fluid B-cells resist treatment in multiple sclerosis

Longitudinally persistent cerebrospinal fluid B-cells resist treatment in multiple sclerosis

Cladribine to treat disease exacerbation after fingolimod discontinuation in progressive multiple sclerosis

Dimethyl fumarate: Regulatory effects on the immune system in the treatment of multiple sclerosis

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