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Switching Natalizumab to Biosimilar

Posted on March 28, 2026 by
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Høgestøl EA, Brustad ÅW, Celius EG, Meling M, Berg-Hansen P, Kro GB, König M, Schanke Y, Halvorsen B, Warren DJ, Gehin JE, Bolstad N, Nygaard GO. Serum drug levels and JCV assay discrepancies after switching from originator to biosimilar natalizumab. BMJ Neurol Open. 2026 Mar 18;8(1):e001477. doi: 10.1136/bmjno-2025-001477. 

Background: In January 2024, all people with multiple sclerosis (pwMS) treated with natalizumab (NTZ) at Oslo University Hospital were switched from originator to biosimilar NTZ. We prospectively evaluated disease activity, safety, serum drug levels, immunogenicity and biomarkers.

Methods: This observational study included 39 pwMS switching to biosimilar NTZ. Clinical relapses, MRI activity and side effects were recorded. NTZ levels and anti-drug antibodies (ADAb) by in-house assays; anti-John Cunningham virus (JCV) antibodies by Stratify (Biogen) and Immunowell (Sandoz) platforms; leucocytes and serum levels of neurofilament light chain (NfL) and glial fibrillar acidic protein (GFAP) were measured by Mesoscale platform.

Results: Eleven pwMS (28%) reported new side effects, most commonly fatigue, headache and muscle pain. Mean NTZ levels were 15.1 mg/L before and 14.9 mg/L after switching (difference -0.3, 95% CI -1.4 to 0.8). ADAb was detected in one pwMS, unchanged after switch. The proportion of JCV-positive cases increased from 13% (Stratify) to 52% (Immunowell), leading four pwMS to discontinue NTZ. Leukocytes were stable after switch. Median NfL remained stable (45.3 vs 44.0 pg/mL; median difference -1.3, 95% CI -6.0 to 3.5), whereas GFAP decreased (23.0 vs 20.5 pg/mL; difference -2.5, 95% CI -4.7 to -0.3).

Conclusions: Switching from originator to biosimilar NTZ was associated with stable disease activity. Drug levels, ADAb, leukocytes and NfL remained similar before and after switching, and GFAP decreased, of uncertain relevance. The marked rise in JCV-positivity on the Immunowell assay underscores the need for harmonisation of anti-JCV antibody testing.

So they dont find a big difference between natalizumab and biosimilar natalizumab, but if you had the Tryruko, you were more likely to have JC virus positivity. They say “The lack of harmonisation of the current companion diagnostic tests for NTZ reduces the applicability of biosimilar NTZ.

Source: multiple-sclerosis-research.org

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