Last updated on November 18th, 2025 at 06:25 pm

Possible reasons to switch

• Natalizumab is a very high-efficacy DMT capable of achieving long-term NEIDA (no evident inflammatory disease activity) and limiting end-organ damage (brain volume loss) in most people with MS who receive it.
• Following rebaselining, the average annual brain volume loss for patients treated with natalizumab is within the expected range for age-matched people without MS.
• When natalizumab is used early in the disease course, many people with MS report a reduction in symptoms of disability, fatigue and brain fog.
• Studies in humans suggest natalizumab exposure has no adverse effect on pregnancy outcomes.

Reasons for caution

• Natalizumab is an immunosuppressive therapy and has been associated with opportunistic infections, of which the JC virus (JCV) is the commonest.
• Patients who are seropositive for JCV are at greatly increased risk of developing progressive multifocal leukoencephalopathy (PML), a serious, potentially fatal complication of natalizumab treatment.
• If you have a central nervous infection, care is needed when switching from an S1P modulator or fumarate to natalizumab because it will blunt the immune response towards the infectious agent.
• If switching from teriflunomide to natalizumab to increase disease control or to attempt pregnancy, rapid teriflunomide elimination is needed because of its long half-life and potentially toxic effects on the foetus.
• Cladribine, anti-CD20s, alemtuzumab, mitoxantrone and HSCT are all immunosuppressive therapies; if you are JCV-seropositive, switching from any of these DMTs to natalizumab will increase your risk of developing PML.

Natalizumab

Recent data have shown that increasing the dosing interval between natalizumab infusions (extended interval dosing, EID) will lower the risk of developing PML.

Restarting natalizumab

Before restarting natalizumab it is important to do routine blood tests, a baseline MRI and check for anti-natalizumab antibodies. The presence of anti-natalizumab antibodies increases the risk of developing infusion reactions and is a contraindication to restarting natalizumab. It is not uncommon for someone with MS to want to switch back to natalizumab after trying another DMT. Natalizumab is known to reduce MS-related fatigue and brain fog, and this often returns when it washes out. The ability to reduce PML risk with EID will increase the number of patients requesting to go back onto natalizumab to help manage such cognitive symptoms.

Other DMTs

In general, natalizumab can be used after any of the DMTs provided the baseline screening bloods are satisfactory and there are no contraindications to the specific DMT. Some important caveats are highlighted below.

Interferon-beta and glatiramer acetate

I have no concerns and would not recommend any specific washout period after stopping either IFN-beta or glatiramer acetate.

Alemtuzumab and HSCT (non-selective cell depleting DMTs)

If you wish to start natalizumab after alemtuzumab or HSCT because of recurrent disease activity, I suggest doing so as soon as possible. Alemtuzumab and HSCT are immunosuppressive therapies, however, so if you are JCV-seropositive they will greatly increase your risk of developing PML and will render the so-called anti-JCV index unreliable. If your MS is not active post-alemtuzumab or HSCT, I would question the need for natalizumab because both these DMTs can induce long-term remission.

Cladribine and anti-CD20 therapies (selective cell depleting DMTs)

If you wish to start natalizumab after cladribine or an anti-CD20 therapy because of recurrent disease activity, then I would suggest doing so as soon as possible. Cladribine and anti-CD20s are immunosuppressive therapies, however, so if you are JCV-seropositive they will increase your risk of developing PML and will render the so-called anti-JCV index unreliable. If your MS is not active post-cladribine or an anti-CD20, I would question the need for natalizumab because these DMTs can induce long-term remission.

S1P modulators (fingolimod, siponimod, ozanimod and ponesimod)

No washout period is required when switching from an S1P modulator to natalizumab. However, if you have an infectious complication, particularly a CNS infection, then you would be ill-advised to start natalizumab until the CNS infection has been cleared. Natalizumab will prevent lymphocyte trafficking into the CNS and hence will blunt the immune response to the infectious agent. 

Fumarates (dimethyl fumarate and diroximel fumarate)

No washout period is required when switching from a fumarate to natalizumab. The same warning about CNS infections applies to fumarates as to S1P modulators mentioned above.

Teriflunomide

No teriflunomide washout period is required when switching to natalizumab. However, if your reason for switching to natalizumab is to control MS disease or fall pregnant, then you will need to undergo rapid teriflunomide elimination because of its long half-life and potential for teratogenicity.

Mitoxantrone

Mitoxantrone is an immunosuppressive therapy. Therefore, if you are JCV-seropositive it will increase your risk of developing PML and will render the so-called anti-JCV index unreliable.

Special circumstances

The presence of specific comorbidities and adverse events may make it difficult to start natalizumab after certain DMTs. These are, however, uncommon in routine clinical practice.

What about switching from natalizumab to another DMT?

A switch is relatively straightforward if you are JC virus-seronegative and are switching because of lack of efficacy or for a lifestyle choice, for example:

• you are tired of monthly infusions (please note, however, there is now a subcutaneous formulation that is given as two injections)
• you want an immune reconstitution therapy (IRT) that offers the freedom to fall pregnant without worrying about rebound activity
• you simply prefer the long-term potential of an IRT.

In this situation, switching from natalizumab without a washout period, to prevent rebound disease activity after natalizumab, makes sense and should be a relatively safe option.

The situation if you are JC virus-seropositive is much more problematic because of the risk of carry-over PML. With a maintenance agent, such as an S1P modulator, we simply exclude asymptomatic PML by doing an MRI and, if you want to be extra vigilant, a lumbar puncture to look for JCV DNA in the spinal fluid. If these tests are clear, we start the S1P modulator as soon as possible after the last natalizumab infusion, knowing that if PML should develop we can stop the S1P modulator and it will be cleared from the body within 4 ̶ 6 weeks or less (depending which S1P modulator you are taking). This early switching strategy also prevents rebound activity when natalizumab wears off after approximately 3 ̶ 4 months.

With an IRT, such as alemtuzumab, things are more complicated because we can’t reverse its action. Hence, we must be confident that there is no carry-over PML. Why am I so concerned? Simple: if you develop carry-over PML post-alemtuzumab, before reconstitution of your immune system, you are likely to succumb to PML – which is potentially fatal. We rely on a functioning immune system, in particular a population of cells called CD8+ cytotoxic T lymphocytes, to clear the JC virus from the brain. CD8+ lymphocytes take many months to reconstitute post-alemtuzumab and other IRTs, during which time the PML is unchecked.

You might argue that by treating MS, a disabling disease, with immunosuppressive therapies we simply create another ticking time bomb and swap one disease, MS, for another disease, immunosuppression. The difference between these two diseases is that MS-related disability is in general irreversible and associated with loss of quality of life. Immunosuppression, on the other hand, can be derisked to some extent and its consequences – in particular, opportunistic infections – can be treated. For more information, please read the sections on each DMT.

We now know that people with MS who are JCV-seropositive either need to come off natalizumab or switch to EID, because of the risk of PML. For high-risk subjects who decide to stay on natalizumab we offer 3-monthly MRI studies to detect asymptomatic PML, which has a better prognosis than symptomatic PML.