Switching from natalizumab to antiCD20 monoclonal antibodies: Short transition interval is associated with improved outcome

Gabriel Bsteh; Robert Hoepner; Jonathan A Gernert; Klaus Berek; Christiane Gradl; Dariia Kliushnikova; Anna Damulina; Gerhard Traxler; Fabian Föttinger; Sebastian Habernig; Nik Krajnc; Alejandro Xavier León Betancourt; Markus Ponleitner; Tobias Zrzavy; Florian Deisenhammer; Franziska Di Pauli; Joachim Havla; Michael Khalil; Tania Kümpfel; Peter Wipfler; Andrew Chan; Thomas Berger; Helly Hammer; Harald Hegen

doi:10.1111/ene.16587

Switching from natalizumab to antiCD20 monoclonal antibodies: Short transition interval is associated with improved outcome

Gabriel Bsteh
, Robert Hoepner
, Jonathan A Gernert
, Klaus Berek
, Christiane Gradl
, Dariia Kliushnikova
, Anna Damulina
, Gerhard Traxler
, Fabian Föttinger
, Sebastian Habernig
, Nik Krajnc
, Alejandro Xavier León Betancourt
, Markus Ponleitner
, Tobias Zrzavy
, Florian Deisenhammer
, Franziska Di Pauli
, Joachim Havla
, Michael Khalil
, Tania Kümpfel
, Peter Wipfler

Andrew Chan, Thomas Berger, Helly Hammer, Harald Hegen

Division of Neurology (University Hospital St. Pölten)

Research output: Journal article (peer-reviewed) › Journal article

2 Citations (Scopus)

Abstract

OBJECTIVE: To investigate the impact of transition interval length when switching from natalizumab (NTZ) to anti-CD20 monoclonal antibodies (antiCD20) on recurrent disease activity and safety in relapsing multiple sclerosis (RMS).

METHODS: Aggregating data from 8 MS centres in Austria, Switzerland, and Germany, we included RMS patients who (i) continuously received NTZ for ≥3 months, (ii) were switched to antiCD20, and (iii) had ≥12 months follow-up after switch. The primary endpoint was occurrence of relapse after switch, secondary endpoints included severe infections (CTCAE grade ≥3).

RESULTS: Overall, 139 RMS patients were included (70.5% females, mean age at switch 38.8 years [SD 9.7], mean disease duration at switch 11.3 years [SD 6.2], median duration on NTZ 4.4 years [range: 0.3-16.4], median transition interval 58 days [0-180]). Relapse occurred in 18 patients (12.9%) after NTZ discontinuation. Of those, 11 (61.1%) patients relapsed during the transition interval. No patient with a transition interval below 30 days experienced a relapse, compared to 11.1% and 16.1% with transition intervals of 30-44 days and ≥ 45 days, respectively. In multivariable Cox regression, a transition interval ≥ 45 days predicted a 4.73-fold increased risk of relapse. Over approximately 4 years of follow-up, six severe infections were reported without any noticeable effect of transition interval length. No PML occurred.

CONCLUSIONS: Switching from NTZ to antiCD20 is generally both effective and safe. Keeping the transition interval below 30 days provides the optimal balance between preventing recurrent disease activity and ensuring safety.

Original language	English
Article number	e16587
Pages (from-to)	e16587
Journal	European Journal of Neurology
Volume	32
Issue number	1
DOIs	https://doi.org/10.1111/ene.16587
Publication status	Published - Jan 2025

Keywords

Adult
Female
Humans
Male
Middle Aged
Drug Substitution
Immunologic Factors/therapeutic use
Multiple Sclerosis, Relapsing-Remitting/drug therapy
Natalizumab/therapeutic use
Recurrence
Treatment Outcome

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10.1111/ene.16587

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Bsteh, G., Hoepner, R., Gernert, J. A., Berek, K., Gradl, C., Kliushnikova, D., Damulina, A., Traxler, G., Föttinger, F., Habernig, S., Krajnc, N., Betancourt, A. X. L., Ponleitner, M., Zrzavy, T., Deisenhammer, F., Di Pauli, F., Havla, J., Khalil, M., Kümpfel, T., ... Hegen, H. (2025). Switching from natalizumab to antiCD20 monoclonal antibodies: Short transition interval is associated with improved outcome. European Journal of Neurology, 32(1), e16587. Article e16587. https://doi.org/10.1111/ene.16587

@article{28492732dbdf4850b10a277aa16b326a,

title = "Switching from natalizumab to antiCD20 monoclonal antibodies: Short transition interval is associated with improved outcome",

abstract = "OBJECTIVE: To investigate the impact of transition interval length when switching from natalizumab (NTZ) to anti-CD20 monoclonal antibodies (antiCD20) on recurrent disease activity and safety in relapsing multiple sclerosis (RMS).METHODS: Aggregating data from 8 MS centres in Austria, Switzerland, and Germany, we included RMS patients who (i) continuously received NTZ for ≥3 months, (ii) were switched to antiCD20, and (iii) had ≥12 months follow-up after switch. The primary endpoint was occurrence of relapse after switch, secondary endpoints included severe infections (CTCAE grade ≥3).RESULTS: Overall, 139 RMS patients were included (70.5\% females, mean age at switch 38.8 years [SD 9.7], mean disease duration at switch 11.3 years [SD 6.2], median duration on NTZ 4.4 years [range: 0.3-16.4], median transition interval 58 days [0-180]). Relapse occurred in 18 patients (12.9\%) after NTZ discontinuation. Of those, 11 (61.1\%) patients relapsed during the transition interval. No patient with a transition interval below 30 days experienced a relapse, compared to 11.1\% and 16.1\% with transition intervals of 30-44 days and ≥ 45 days, respectively. In multivariable Cox regression, a transition interval ≥ 45 days predicted a 4.73-fold increased risk of relapse. Over approximately 4 years of follow-up, six severe infections were reported without any noticeable effect of transition interval length. No PML occurred.CONCLUSIONS: Switching from NTZ to antiCD20 is generally both effective and safe. Keeping the transition interval below 30 days provides the optimal balance between preventing recurrent disease activity and ensuring safety.",

keywords = "Adult, Female, Humans, Male, Middle Aged, Drug Substitution, Immunologic Factors/therapeutic use, Multiple Sclerosis, Relapsing-Remitting/drug therapy, Natalizumab/therapeutic use, Recurrence, Treatment Outcome",

author = "Gabriel Bsteh and Robert Hoepner and Gernert, \{Jonathan A\} and Klaus Berek and Christiane Gradl and Dariia Kliushnikova and Anna Damulina and Gerhard Traxler and Fabian F{\"o}ttinger and Sebastian Habernig and Nik Krajnc and Betancourt, \{Alejandro Xavier Le{\'o}n\} and Markus Ponleitner and Tobias Zrzavy and Florian Deisenhammer and \{Di Pauli\}, Franziska and Joachim Havla and Michael Khalil and Tania K{\"u}mpfel and Peter Wipfler and Andrew Chan and Thomas Berger and Helly Hammer and Harald Hegen",

note = "Publisher Copyright: {\textcopyright} 2024 The Author(s). European Journal of Neurology published by John Wiley \& Sons Ltd on behalf of European Academy of Neurology.",

year = "2025",

month = jan,

doi = "10.1111/ene.16587",

language = "English",

volume = "32",

pages = "e16587",

journal = "European Journal of Neurology",

issn = "1351-5101",

publisher = "Wiley-Blackwell Publishing Ltd",

number = "1",

}

Bsteh, G, Hoepner, R, Gernert, JA, Berek, K, Gradl, C, Kliushnikova, D, Damulina, A, Traxler, G, Föttinger, F, Habernig, S, Krajnc, N, Betancourt, AXL, Ponleitner, M, Zrzavy, T, Deisenhammer, F, Di Pauli, F, Havla, J, Khalil, M, Kümpfel, T, Wipfler, P, Chan, A, Berger, T, Hammer, H & Hegen, H 2025, 'Switching from natalizumab to antiCD20 monoclonal antibodies: Short transition interval is associated with improved outcome', European Journal of Neurology, vol. 32, no. 1, e16587, pp. e16587. https://doi.org/10.1111/ene.16587

TY - JOUR

T1 - Switching from natalizumab to antiCD20 monoclonal antibodies

T2 - Short transition interval is associated with improved outcome

AU - Bsteh, Gabriel

AU - Hoepner, Robert

AU - Gernert, Jonathan A

AU - Berek, Klaus

AU - Gradl, Christiane

AU - Kliushnikova, Dariia

AU - Damulina, Anna

AU - Traxler, Gerhard

AU - Föttinger, Fabian

AU - Habernig, Sebastian

AU - Krajnc, Nik

AU - Betancourt, Alejandro Xavier León

AU - Ponleitner, Markus

AU - Zrzavy, Tobias

AU - Deisenhammer, Florian

AU - Di Pauli, Franziska

AU - Havla, Joachim

AU - Khalil, Michael

AU - Kümpfel, Tania

AU - Wipfler, Peter

AU - Chan, Andrew

AU - Berger, Thomas

AU - Hammer, Helly

AU - Hegen, Harald

PY - 2025/1

Y1 - 2025/1

N2 - OBJECTIVE: To investigate the impact of transition interval length when switching from natalizumab (NTZ) to anti-CD20 monoclonal antibodies (antiCD20) on recurrent disease activity and safety in relapsing multiple sclerosis (RMS).METHODS: Aggregating data from 8 MS centres in Austria, Switzerland, and Germany, we included RMS patients who (i) continuously received NTZ for ≥3 months, (ii) were switched to antiCD20, and (iii) had ≥12 months follow-up after switch. The primary endpoint was occurrence of relapse after switch, secondary endpoints included severe infections (CTCAE grade ≥3).RESULTS: Overall, 139 RMS patients were included (70.5% females, mean age at switch 38.8 years [SD 9.7], mean disease duration at switch 11.3 years [SD 6.2], median duration on NTZ 4.4 years [range: 0.3-16.4], median transition interval 58 days [0-180]). Relapse occurred in 18 patients (12.9%) after NTZ discontinuation. Of those, 11 (61.1%) patients relapsed during the transition interval. No patient with a transition interval below 30 days experienced a relapse, compared to 11.1% and 16.1% with transition intervals of 30-44 days and ≥ 45 days, respectively. In multivariable Cox regression, a transition interval ≥ 45 days predicted a 4.73-fold increased risk of relapse. Over approximately 4 years of follow-up, six severe infections were reported without any noticeable effect of transition interval length. No PML occurred.CONCLUSIONS: Switching from NTZ to antiCD20 is generally both effective and safe. Keeping the transition interval below 30 days provides the optimal balance between preventing recurrent disease activity and ensuring safety.

AB - OBJECTIVE: To investigate the impact of transition interval length when switching from natalizumab (NTZ) to anti-CD20 monoclonal antibodies (antiCD20) on recurrent disease activity and safety in relapsing multiple sclerosis (RMS).METHODS: Aggregating data from 8 MS centres in Austria, Switzerland, and Germany, we included RMS patients who (i) continuously received NTZ for ≥3 months, (ii) were switched to antiCD20, and (iii) had ≥12 months follow-up after switch. The primary endpoint was occurrence of relapse after switch, secondary endpoints included severe infections (CTCAE grade ≥3).RESULTS: Overall, 139 RMS patients were included (70.5% females, mean age at switch 38.8 years [SD 9.7], mean disease duration at switch 11.3 years [SD 6.2], median duration on NTZ 4.4 years [range: 0.3-16.4], median transition interval 58 days [0-180]). Relapse occurred in 18 patients (12.9%) after NTZ discontinuation. Of those, 11 (61.1%) patients relapsed during the transition interval. No patient with a transition interval below 30 days experienced a relapse, compared to 11.1% and 16.1% with transition intervals of 30-44 days and ≥ 45 days, respectively. In multivariable Cox regression, a transition interval ≥ 45 days predicted a 4.73-fold increased risk of relapse. Over approximately 4 years of follow-up, six severe infections were reported without any noticeable effect of transition interval length. No PML occurred.CONCLUSIONS: Switching from NTZ to antiCD20 is generally both effective and safe. Keeping the transition interval below 30 days provides the optimal balance between preventing recurrent disease activity and ensuring safety.

KW - Adult

KW - Female

KW - Humans

KW - Male

KW - Middle Aged

KW - Drug Substitution

KW - Immunologic Factors/therapeutic use

KW - Multiple Sclerosis, Relapsing-Remitting/drug therapy

KW - Natalizumab/therapeutic use

KW - Recurrence

KW - Treatment Outcome

UR - https://www.scopus.com/pages/publications/85212278727

U2 - 10.1111/ene.16587

DO - 10.1111/ene.16587

M3 - Journal article

C2 - 39686558

SN - 1351-5101

VL - 32

SP - e16587

JO - European Journal of Neurology

JF - European Journal of Neurology

IS - 1

M1 - e16587

ER -

Switching from natalizumab to antiCD20 monoclonal antibodies: Short transition interval is associated with improved outcome

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