Insufficient disease inhibition by intrathecal rituximab in progressive multiple sclerosis

Komori, Mika; Lin, Yen Chih; Cortese, Irene; Blake, Andrew; Ohayon, Joan; Cherup, Jamie; Marić, Dragan; Kósa, Péter; Wu, Tianxia; Bielekova, Bibiana

doi:10.1002/acn3.293

Cited by 132 publications

(143 citation statements)

References 34 publications

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“…The current study demonstrates that approximately 0.1% of systemically administered daclizumab reaches the intrathecal compartment, consistent with other monoclonal antibodies such as rituximab 17, 18. The observed rise in serum and CSF IL‐2 levels provides evidence for the ability of daclizumab to inhibit consumption of IL‐2 by activated T cells14 in both systemic and intrathecal compartments.…”

Section: Discussionsupporting

confidence: 83%

Pharmacodynamic effects of daclizumab in the intrathecal compartment

Komori

Kósa

Stein

et al. 2017

Ann Clin Transl Neurol

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ObjectiveIt was previously demonstrated that daclizumab therapy normalizes cellular cerebrospinal fluid (CSF) abnormalities typical of multiple sclerosis (MS) in the majority of treated patients. However, CSF cells represent only the mobile portion of intrathecal immune responses. Therefore, we asked whether daclizumab also reverses compartmentalized inflammation and if not, whether residual inflammation correlates with clinical response to the drug.MethodsForty MS patients treated with an intravenous or subcutaneous injection of daclizumab were followed for up to 16 years in two open‐label clinical trials. MRI contrast‐enhancing lesions (CELs), clinical scales, and CSF biomarkers quantified residual disease.ResultsRapid decreases in CELs, sustained throughout the observation period, were observed with daclizumab treatment. Daclizumab therapy induced modest but statistically significant (P < 0.0001) decreases in CSF levels of T‐cell activation marker CD27 and IgG index. Interleukin 2 (IL‐2) CSF levels increased from baseline levels during treatment, consistent with reduced IL‐2 consumption by T cells, as a consequence of daclizumab's saturation of high‐affinity IL‐2 receptors. CSF levels of IL‐12p40, chitinase‐3‐like protein‐1 (CHI3L1), chemokine C‐X‐C motif ligand 13, and neurofilament light chain (NFL) were also significantly reduced by daclizumab. Among them, inhibition of CHI3L1 correlated with inhibition of NFL and with lack of disease progression.InterpretationThese observations confirm daclizumab's direct pharmacodynamics effects on immune cells within central nervous system tissues and identify inhibition of CSF biomarkers of myeloid lineage as a stronger determinant of reduction in clinical MS activity than inhibition of biomarkers of adaptive immunity.

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Section: Discussionsupporting

confidence: 83%

Pharmacodynamic effects of daclizumab in the intrathecal compartment

Komori

Kósa

Stein

et al. 2017

Ann Clin Transl Neurol

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“…The authors demonstrated that higher rituximab concentrations paradoxically decreased the rituximab concentration on the surface of B cells, due to facilitated internalization of CD20/ rituximab complexes in vitro [Komori et al 2016]. Therefore, the 200 mg dose was considered sufficient to saturate CD20 leading to long-lasting depletion of B cells from peripheral circulation [Komori et al 2016]. However, greater surface binding does not mean more-efficient depletion and the study did not investigate B-cell depletion in vivo for the different rituximab dosages to allow definite conclusions.…”

Section: Dosing Of B-cell-depleting Therapies: Experiences From Rituxmentioning

confidence: 99%

“…rituximab on day 1 and day 15 with intrathecally administered rituximab. The authors demonstrated that higher rituximab concentrations paradoxically decreased the rituximab concentration on the surface of B cells, due to facilitated internalization of CD20/ rituximab complexes in vitro [Komori et al 2016]. Therefore, the 200 mg dose was considered sufficient to saturate CD20 leading to long-lasting depletion of B cells from peripheral circulation [Komori et al 2016].…”

Section: Dosing Of B-cell-depleting Therapies: Experiences From Rituxmentioning

confidence: 99%

“…Apart from the usage as monotherapy, rituximab was also tested as add-on therapy (4-weekly doses of 375 mg/m 2 , added on to IFNs or glatiramer acetate) in patients with RRMS demonstrating an additional reduction of Gd-enhanced brain lesions [Naismith et al 2010]. The RIVITALISE trial [ClinicalTrials.gov identifier: NCT01212094] evaluated the efficacy of intrathecally administered rituximab compared with placebo in SPMS following the hypothesis of compartmentalized inflammation in the progressive phase of MS. 2% of serum concentrations were measured in the CSF representing a 20-fold increase in bioavailability of serum values achievable without intrathecal dosing [Komori et al 2016]. However, the trial was prematurely terminated due to not meeting efficacy endpoints during the interim analysis.…”

Section: Dosing Of B-cell-depleting Therapies: Experiences From Rituxmentioning

confidence: 99%

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Targeting B cells in relapsing–remitting multiple sclerosis: from pathophysiology to optimal clinical management

Bittner

Ruck

Wiendl

et al. 2016

Ther Adv Neurol Disord

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Multiple sclerosis (MS) is a chronic inflammatory demyelinating disease that is caused by an autoimmune response against central nervous system (CNS) structures. Traditionally considered a T-cell-mediated disorder, the contribution of B cells to the pathogenesis of MS has long been debated. Based on recent promising clinical results from CD20-depleting strategies by three therapeutic monoclonal antibodies in clinical phase II and III trials (rituximab, ocrelizumab and ofatumumab), targeting B cells in MS is currently attracting growing interest among basic researchers and clinicians. Many questions about the role of B and plasma cells in MS remain still unanswered, ranging from the role of specific B-cell subsets and functions to the optimal treatment regimen of B-cell depletion and monitoring thereafter. Here, we will assess our current knowledge of the mechanisms implicating B cells in multiple steps of disease pathology and examine current and future therapeutic approaches for the treatment of MS.

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“…In patients using rituximab for other indications, PML cases have rarely been reported [70]. Although rituximab rapidly and consistently decreases the numbers of peripheral CD20+ and CD19+ cells [71], a small phase II trial of intrathecal rituximab was terminated early because of low efficacy on the CSF biomarkers [72]. Rituximab induced an incomplete and transient depletion of B cells in the CSF, whilst the effects on peripheral B cells were complete and lasting.…”

Section: Agents In Trialmentioning

confidence: 99%