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Abstract

Background:

Rituximab and ocrelizumab are anti-CD20 monoclonal antibodies that have shown a marked reduction in multiple sclerosis (MS) inflammatory activity. However, their real-world safety profile has not been adequately compared.

Objective:

To investigate the adverse event (AE) profile of rituximab and ocrelizumab reported to the Food and Drug Administration Adverse Event Reporting System (FAERS) database.

Methods:

The FAERS database was filtered by indication (MS) and drug (rituximab or ocrelizumab). Disproportionality analyses including but not limited to reporting odds ratio (ROR) were conducted to identify drug–AE associations. A signal was detected if the lower limit of the 95% confidence interval of ROR (ROR₀₂₅) exceeded 1.

Results:

There were 623 and 7948 reports for rituximab and ocrelizumab, respectively. The most frequent AEs with rituximab and ocrelizumab were infusion-related reaction (4.82%) and urinary tract infection (10.52%), respectively. The strongest drug–AE association for rituximab and ocrelizumab were ear pruritus (ROR₀₂₅: 47.53) and oral herpes (ROR₀₂₅: 38.99), respectively. Ocrelizumab was associated with an almost two times higher frequency of infections than rituximab (21.93% vs 11.05%, respectively).

Conclusion:

This study revealed differences in reporting AEs between rituximab and ocrelizumab. Infections were reported more frequently with ocrelizumab. Although speculative, a potentially different or more extensive B-cell depletion by ocrelizumab might explain these findings. Additional pharmacovigilance studies need to be performed to better characterize differences in the AE profile in B-cell-depleting therapies.

Keywords

Rituximab ocrelizumab CD20 adverse event profile FAERS multiple sclerosis

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References

Compston

Coles

Multiple sclerosis. Lancet 2008; 372: 1502–1517.

Ghasemi

Razavi

Nikzad

Multiple Sclerosis: Pathogenesis, symptoms, diagnoses and cell-based therapy. Cell J 2017; 19(1): 1–10.

Greenfield

Hauser

SL.

B Cell therapy for multiple sclerosis: Entering an era. Ann Neurol 2018; 83(1): 13–26.

Loma

Heyman

Multiple sclerosis: Pathogenesis and treatment. Curr Neuropharmacol 2011; 9: 409–416.

Stashenko

Nadler

Hardy

, et al. Characterization of a human B lymphocyte-specific antigen. J Immunol 1980; 125: 1678–1685.

Holley

Bremer

Kendall

, et al. CD20+inflammatory T-cells are present in blood and brain of multiple sclerosis patients and can be selectively targeted for apoptotic elimination. Mult Scler Relat Disord 2014; 3(5): 650–658.

Palanichamy

Jahn

Nickles

, et al. Rituximab efficiently depletes increased CD20-expressing T cells in multiple sclerosis patients. J Immunol 2014; 193: 580–586.

Beers

Chan

CHT

French

, et al. CD20 as a target for therapeutic type I and II monoclonal antibodies. Semin Hematol 2010; 47(2): 107–114.

Pieper

Grimbacher

Eibel

B-cell biology and development. J Allergy Clin Immunol 2013; 131: 959–971.

10.

Hauser

Waubant

Arnold

, et al. B-cell depletion with rituximab in relapsing-remitting multiple sclerosis. N Engl J Med 2008; 358: 676–688.

11.

Hawker

O’Connor

Freedman

, et al. Rituximab in patients with primary progressive multiple sclerosis: Results of a randomized double-blind placebo-controlled multicenter trial. Ann Neurol 2009; 66(4): 460–471.

12.

Hauser

Bar-Or

Comi

, et al. Ocrelizumab versus interferon beta-1a in relapsing multiple sclerosis. N Engl J Med 2017; 376: 221–234.

13.

Montalban

Hauser

Kappos

, et al. Ocrelizumab versus placebo in primary progressive multiple sclerosis. N Engl J Med 2017; 376: 209–220.

14.

Scotti

Disanto

Sacco

, et al. Effectiveness and safety of rituximab in multiple sclerosis: An observational study from Southern Switzerland. PLoS ONE 2018; 13(5): e0197415.

15.

FDA and Adverse Event Reporting System (FAERS) Public Dashboard. FDA, www.fda.gov (accessed 2 April 2020).

16.

MedDRA . Version 22.1, www.meddra.org (accessed 26 March 2020).

17.

Sakaeda

Tamon

Kadoyama

, et al. Data mining of the public version of the FDA adverse event reporting system. Int J Med Sci 2013; 10: 796–803.

18.

Yoshimura

Kadoyama

Sakaeda

, et al. A Survey of the FAERS database concerning the adverse event profiles of α1-adrenoreceptor blockers for lower urinary tract symptoms. Int J Med Sci 2013; 10(7): 864–869.

19.

Bate

Lindquist

Edwards

, et al. A Bayesian neural network method for adverse drug reaction signal generation. Eur J Clin Pharmacol 1998; 54(4): 315–321.

20.

van Puijenbroek

Bate

Leufkens

, et al. A comparison of measures of disproportionality for signal detection in spontaneous reporting systems for adverse drug reactions. Pharmacoepidemiol Drug Saf 2002; 11(1): 3–10.

21.

Szarfman

Machado

O’Neill

RT.

Use of screening algorithms and computer systems to efficiently signal higher-than-expected combinations of drugs and events in the US FDA’s spontaneous reports database. Drug Saf 2002; 25(6): 381–392.

22.

Mills

Mao-Draayer

Next-generation anti-CD20 monoclonal antibodies in autoimmune disease treatment. Auto Immun Highlights 2017; 8: 12.

23.

Klein

Lammens

SchÃ¤fer

, et al. Epitope interactions of monoclonal antibodies targeting CD20 and their relationship to functional properties. Mabs 2013; 5(1): 22–33.

24.

Mössner

Brünker

Moser

, et al. Increasing the efficacy of CD20 antibody therapy through the engineering of a new type II anti-CD20 antibody with enhanced direct and immune effector cell-mediated B-cell cytotoxicity. Blood 2010; 115: 4393–4402.

25.

Kappos

Calabresi

, et al. Ocrelizumab in relapsing-remitting multiple sclerosis: A phase 2, randomised, placebo-controlled, multicentre trial. Lancet 2011; 378: 1779–1787.

26.

Sorensen

Lisby

Grove

, et al. Safety and efficacy of ofatumumab in relapsing-remitting multiple sclerosis: A phase 2 study. Neurology 2014; 82: 573–581.

27.

Baker

Pryce

James

, et al. The ocrelizumab phase II extension trial suggests the potential to improve the risk: benefit balance in multiple sclerosis. medrxiv 2020; 2020.01.09.20016774.

28.

Hallberg

Boremalm

Evertsson

, et al. Risk of hypogammaglobulinemia in long-term treatment with rituximab. ECTRIMS 2019, abstract 65, https://onlinelibrary.ectrims-congress.eu/ (accessed 13 July 2020).

29.

Ancau

Berthele

Hemmer

CD20 monoclonal antibodies for the treatment of multiple sclerosis: Up-to-date. Expert Opin Biol Ther 2019; 19(8): 829–843.

30.

Derfuss

Serum immunoglobulin levels and risk of serious infections in the pivotal Phase III trials of ocrelizumab in multiple sclerosis and their open-label extensions. ECTRIMS 2019, abstract 65. https://onlinelibrary.ectrims-congress.eu/ (accessed 13 July 2020).

31.

Varghese

Standaert

Olivieri

, et al. The temporal impact of aging on the burden of herpes zoster. BMC Geriatr 2017; 17: 30.

32.

Arvin

AM.

Humoral and cellular immunity to varicella-zoster virus: An overview. J Infect Dis 2008; 197: S58–S60.

33.

Deshpande

Kumaraguru

Rouse

BT.

Dual role of B cells in mediating innate and acquired immunity to herpes simplex virus infections. Cell Immunol 2000; 202: 79–87.

34.

Pandya

Murray

Pollok

, et al. The immune system in cancer pathogenesis: Potential therapeutic approaches. J Immunol Res 2016; 2016: 4273943.

35.

Alping

Askling

Burman

, et al. Cancer risk for fingolimod, natalizumab, and rituximab in multiple sclerosis patients. Ann Neurol 2020; 87(5): 688–699.

36.

Velter

Pagès

Schneider

, et al. Four cases of rituximab-associated melanoma. Melanoma Res 2014; 24(4): 401–403.

37.

Monaco

Jones

Rigby

WFC

. Rituximab associated late-onset neutropenia-a rheumatology case series and review of the literature. Clin Rheumatol 2016; 35: 2457–2462.

38.

Zanetta

Robotti

Nozzolillo

, et al. Late onset absolute neutropenia associated with ocrelizumab treatment in multiple sclerosis: A case report and review of the literature. J Neurol Sci 2020; 409: 116603.

39.

Futosi

Fodor

Mócsai

Neutrophil cell surface receptors and their intracellular signal transduction pathways. Int Immunopharmacol 2013; 17: 638–650.

40.

Cohen

BA.

Late-onset neutropenia following ocrelizumab therapy for multiple sclerosis. Neurology 2019; 92: 435–436.

41.

Montastruc

J-L

Sommet

Bagheri

, et al. Benefits and strengths of the disproportionality analysis for identification of adverse drug reactions in a pharmacovigilance database. Br J Clin Pharmacol 2011; 72(6): 905–908.

42.

Hazell

Shakir

SAW

. Under-reporting of adverse drug reactions: A systematic review. Drug Saf 2006; 29: 385–396.

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Adverse event profile differences between rituximab and ocrelizumab: Findings from the FDA Adverse Event Reporting Database

Abstract

Background:

Objective:

Methods:

Results:

Conclusion:

Keywords

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References

Supplementary Material