Is It Safe To Switch Biosimilars?
DermatologyPlaque PsoriasisPsoriasis Deep Dive Series

Is It Safe To Switch Biosimilars?

RₓPodcast disclaimerThis podcast is produced for educational purposes only. The conversation between hosts represents a discussion of published clinical evidence and is not intended as clinical advice, a substitute for professional medical judgment, or a recommendation for any specific treatment.
Psoriasis Deep Dive SeriesEp 4 of 4
Is It Safe To Switch Biosimilars?

Hosted by Sarah Gellar & Marcus Webb

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Show Notes

The NOR-SWITCH trial established that switching from reference infliximab to a biosimilar is safe. Multiple subsequent studies have confirmed this across adalimumab and other biologics. Sarah Mitchell and James Carter examine the switching evidence, the nocebo effect, and how the biosimilar dividend is reshaping access to care.

Transcription
Sarah Gellar

Picture a patient for a second. Uh, he's 43 years old and he has plaque psoriasis.

Marcus Webb

Okay.

Sarah Gellar

And we aren't talking about like a mild rash on his elbow. Imagine 40% of his body covered in these painful, itchy, just severely inflamed plaques.

Marcus Webb

Oh, wow. Yeah, that is a really severe presentation.

Sarah Gellar

Right. And he's been through the wringer trying to find relief. He's failed two different conventional systemic treatments already.

Marcus Webb

Which is exhausting for a patient.

Sarah Gellar

Totally. But finally, his medical team prescribes this biologic drug called Adalimumab, and it works flawlessly. I mean, he achieves a PASI 90.

Marcus Webb

Oh, that's huge. Uh, for those listening in dermatology, PASI 90 translates to near total clearance of the disease. It is the absolute gold standard outcome.

Sarah Gellar

Right. So for 18 straight months, his body is perfectly stable. He essentially has his life back.

Marcus Webb

When you work in clinical practice, getting a patient to that level of sustained clearance is the ultimate goal. That's what you want.

Sarah Gellar

Exactly. But then a wrench gets thrown into the gears. His insurance coverage changes.

Marcus Webb

Oh, of course.

Sarah Gellar

Almost overnight, his doctor gets this notice from the pharmacy benefit manager saying, "Hey, you need to switch this perfectly stable patient off his current medication. You have to transition him to a cheaper alternative, uh, called a biosimilar."

Marcus Webb

Yeah, that's a classic scenario.

Sarah Gellar

And the doctor looks at this patient who is finally thriving after years of suffering, and she hesitates. She pushes back against the insurance company.

Marcus Webb

Naturally.

Sarah Gellar

Right. And that leaves her wrestling with a really serious professional dilemma. Is she being a good, fiercely protective clinician, or is she being, you know, overly cautious to the point of actively resisting evidence-based medicine?

Marcus Webb

It is a profound dilemma. And honestly, it highlights this massive tension we see between clinical instinct and the sort of economic realities of modern healthcare systems.

Sarah Gellar

Totally. So welcome to today's deep dive. We are exploring a really fascinating discussion we sourced between a consultant dermatologist and a clinical pharmacologist.

Marcus Webb

Yeah, it's a great exchange.

Sarah Gellar

It really is. They tackle the deep science, the complicated psychology, and the fundamental ethics of biosimilar drugs.

Marcus Webb

There's a lot to get into.

Sarah Gellar

There is. Our mission today is to unpack a really critical question for you. When your body is perfectly stable on a highly complex medication, is it ever truly safe to swap it out for a cheaper alternative? So, okay, let's unpack this.

Marcus Webb

Sounds good. To really understand why the doctor in that opening scenario hesitated, we kind of have to establish what a biosimilar actually is.

Sarah Gellar

Right, because there's a lot of confusion there.

Marcus Webb

There is a pervasive assumption, um, even among some practicing clinicians, honestly, that a biosimilar is essentially just a generic version of a biologic drug.

Sarah Gellar

Like it's the exact same thing, just a different brand name.

Marcus Webb

Exactly. But they are fundamentally different categories.

Sarah Gellar

I think a lot of us fall into that trap because we're just so used to how generic drugs work, you know? Like, you take a brand name medication like Aspirin, the patent expires, and another company starts manufacturing generic Aspirin. At the end of the day, you're dealing with a small molecule drug.

Marcus Webb

Yes, a very simple structure.

Sarah Gellar

Right. It's a relatively simple chemical structure that can be perfectly synthesized in really any well-equipped commercial lab.

Marcus Webb

And the output is chemically identical. You can analyze the generic Aspirin and the brand name Aspirin down to the literal atom, and there is zero structural difference.

Sarah Gellar

But biologics aren't like that.

Marcus Webb

Not at all. Biologics do not follow that rule. These are not simple chemicals synthesized in a beaker. They are massive, intensely complex proteins, and they're produced by living cells.

Sarah Gellar

Living cells. That's wild.

Marcus Webb

Yeah. Adalimumab, the drug our 43-year-old patient was taking, is a monoclonal antibody. It consists of roughly 1,300 amino acids folded into this highly specific three-dimensional shape.

Sarah Gellar

Which means the manufacturing process is an entirely different beast. You're dealing with what? Living cell lines, specific fermentation vats, highly proprietary purification steps.

Marcus Webb

Exactly. The industry mantra is literally, the process is the product.

Sarah Gellar

Wow. The process is the product.

Marcus Webb

Right. If a new manufacturer wants to make a biosimilar, they do not have access to the original company's exact cell line. They don't have their specific bioreactor conditions.

Sarah Gellar

So they have to guess.

Marcus Webb

Well, they have to reverse engineer the entire process.

Sarah Gellar

Okay, so it's sort of like trying to perfectly clone a prize-winning racehorse.

Marcus Webb

Ooh, I like that.

Sarah Gellar

Like, even if you manage to secure the exact same genetic blueprint, the environment matters.

Marcus Webb

Right.

Sarah Gellar

If your cloned horse is raised in a slightly different climate or fed a slightly different blend of oats, which I guess in our scenario is the biological fermentation vat.

Marcus Webb

That's exactly it.

Sarah Gellar

Its muscle development and its temperament will be subtly different. You are never going to get a 100% identical atomic clone of the original horse.

Marcus Webb

That captures the biological reality perfectly. Because it's grown in a living system, a biosimilar will naturally have minor structural variations.

Sarah Gellar

So it's not a perfect twin?

Marcus Webb

No, the goal of the manufacturer isn't to create an identical twin. It is to engineer a highly similar molecule that regulators agree has, quote, no clinically meaningful differences in safety, efficacy, or immunogenicity.

Sarah Gellar

Okay, wait. No clinically meaningful difference sounds a lot like lawyer speak to me.

Marcus Webb

It does sound like that, yeah.

Sarah Gellar

If the scientific community openly admits that a biosimilar is not a flawless 100% clone, how can a regulatory agency legally guarantee a patient's safety?

Marcus Webb

That's the big question.

Sarah Gellar

Like, what is stopping a seemingly subtle difference in that protein fold from triggering some massive clinical failure?

Marcus Webb

So regulatory agencies like the FDA in the US and the EMA in Europe rely on a framework called the totality of evidence approach.

Sarah Gellar

Okay, what does that mean?

Marcus Webb

It completely flips the traditional drug approval process on its head. With a brand new, novel drug, the ultimate proof of safety and efficacy comes at the very end of the pipeline.

Sarah Gellar

Right, during those massive phase three clinical trials involving thousands of human patients.

Marcus Webb

Exactly. Because you have no idea how this totally new chemical will behave in a complex human system until you test it at scale.

Sarah Gellar

But a biosimilar isn't a totally novel concept.

Marcus Webb

Right. The target and the mechanism are already well understood. So the regulatory heavy lifting happens at the very beginning of the pipeline in the laboratory.

Sarah Gellar

Before it ever touches a human.

Marcus Webb

Yes. Regulators demand exhaustive analytical characterization. We're talking mass spectrometry, advanced blinding assays, deep functional analysis.

Sarah Gellar

We really put it under the microscope.

Marcus Webb

Literally and figuratively. They map the molecular structure and test its biological activity down to the most microscopic detail possible.

Sarah Gellar

They're essentially playing the most rigorous game of spot the difference imaginable, just analyzing the protein fold by fold.

Marcus Webb

Yes. Long before a single human patient is involved. And once that structural and functional parity is definitively proven in the lab, then they run pharmacokinetic studies.

Sarah Gellar

Just to verify that the drug clears the human body at the same rate.

Marcus Webb

Exactly. By the time they actually run a clinical trial, the trial itself is usually quite small.

Sarah Gellar

Oh, really?

Marcus Webb

Yeah, it's not designed to prove if the drug works, the analytical data already proved that. It's merely a confirmatory step to catch any highly improbable residual issues.

Sarah Gellar

Wow. Okay, so because that extensive lab data does so much of the heavy lifting, it leads to a regulatory mechanism that, um, makes a lot of prescribers very uncomfortable.

Marcus Webb

You're talking about extrapolation.

Sarah Gellar

Yes, extrapolation. If the structural data is rock solid, regulators will approve a biosimilar for diseases it was never even tested on in human trials.

Marcus Webb

It is a major psychological hurdle for doctors.

Sarah Gellar

I can imagine.

Marcus Webb

If a biosimilar is rigorously tested in a clinical trial specifically for rheumatoid arthritis, the EMA or FDA might extrapolate that data and automatically approve the drug for plaque psoriasis as well.

Sarah Gellar

Without requiring a multimillion dollar dedicated psoriasis trial.

Marcus Webb

Exactly.

Sarah Gellar

Which invites a totally valid pushback, I think. I mean, psoriasis involves entirely different inflammatory pathways and completely distinct patient demographics compared to rheumatoid arthritis.

Marcus Webb

It's true. They are very different diseases.

Sarah Gellar

If a master key works flawlessly on the lock to a sprawling mansion, it is a massive leap of faith to assume it works on the lock to a tiny apartment just because they're both buildings, you know?

Marcus Webb

The analogy holds, but we have to shift our perspective on what the lock actually is here.

Sarah Gellar

Okay.

Marcus Webb

The key isn't fitting into the house of the broader disease. It is fitting into the specific molecular lock of the inflammation itself.

Sarah Gellar

Ah, I see.

Marcus Webb

Adalimumab works by seeking out and binding to a very specific inflammatory cytokine called TNF alpha.

Sarah Gellar

So if the lab data proves the biosimilar binds to TNF alpha with the exact same affinity as the original drug, the downstream clinical effect on the human body is going to be identical.

Marcus Webb

Exactly. Regardless of whether that TNF alpha is causing joint pain in arthritis or skin plaques in psoriasis.

Sarah Gellar

The mechanism of action is agnostic to the disease state.

Marcus Webb

Right. Now, regulators are not reckless about this.

Sarah Gellar

Okay, good to know.

Marcus Webb

When you look at a more complex biologic like Ustekinumab, which targets two different inflammatory pathways, IL-12 and IL-23.

Sarah Gellar

Which is used for vastly different conditions like psoriasis and Crohn's disease, right?

Marcus Webb

Yes. For those, the extrapolation bar is much higher. Regulators demand rigorous scientific justification to prove that the minor structural variations won't impact one disease state differently than the other.

Sarah Gellar

Okay, that makes sense. And we're not just relying on theoretical molecular models anymore either. We actually have extensive post-marketing registry data for the older biosimilars now.

Marcus Webb

We do. And registries are great because they capture the messy, real-world patients that controlled clinical trials usually exclude.

Sarah Gellar

Right. And the data from thousands of psoriasis patients in those registries confirms that the extrapolation was scientifically sound.

Marcus Webb

The clinical efficacy remains exactly as predicted.

Sarah Gellar

Okay, so let's pivot back to that 43-year-old patient from our introduction.

Marcus Webb

Right, the guy with the insurance switch.

Sarah Gellar

Yeah. The extrapolation data proves the biosimilar works for new patients starting therapy. But we are talking about swapping out the medication of a patient whose immune system is perfectly suppressed and highly stable on the original biologic.

Marcus Webb

That is the core clinical dilemma. Establishing efficacy in a naive patient is one thing. Disrupting a stabilized patient is another.

Sarah Gellar

Right.

Marcus Webb

To answer that, we really have to look at the landmark NOR-SWITCH trial. It was published in The Lancet back in 2017.

Sarah Gellar

This was a huge watershed moment in the medical community.

Marcus Webb

It truly was. The researchers took nearly 500 patients who were completely stable on an original biologic called Infliximab. Crucially, these patients represented six different indications.

Sarah Gellar

Mm-hmm.

Marcus Webb

So you had rheumatoid arthritis, psoriasis, inflammatory bowel disease, et cetera.

Sarah Gellar

And they randomized the group, right?

Marcus Webb

Yes. Half remained on their original medication and half were abruptly switched to a biosimilar.

Sarah Gellar

Wow. So they were actively testing the extrapolation theory and the switching theory simultaneously across multiple diseases.

Marcus Webb

Very ambitious trial.

Sarah Gellar

What was the outcome for the patients who were forced to switch?

Marcus Webb

The trial established non-inferiority.

Sarah Gellar

Okay.

Marcus Webb

Over a 52-week period, disease worsening occurred in 26% of the patients who switched to the biosimilar compared to 30% of the patients who remained on the original biologic.

Sarah Gellar

So it was statistically comparable, meaning the literal act of switching did not cause a catastrophic loss of stability.

Marcus Webb

Exactly.

Sarah Gellar

But NOR-SWITCH only looked at a single, isolated swap. What happens when insurance formularies force a patient to bounce back and forth between different biosimilars multiple times over a few years?

Marcus Webb

Yeah, that exact scenario was the focus of another study, the VOLTAIRE-X study.

Sarah Gellar

Oh, they actually studied that.

Marcus Webb

They did. They looked specifically at psoriasis patients taking Adalimumab who underwent multiple alternating switches between the reference product and the biosimilar.

Sarah Gellar

Yeah.

Marcus Webb

The results were highly reassuring. They showed no significant loss of efficacy and no spike in adverse events despite the repeated disruption.

Sarah Gellar

That's impressive. But we need to address the underlying biological fear here, which is immunogenicity.

Marcus Webb

Right. The immune response.

Sarah Gellar

Yeah. When you inject a massive, complex protein, like a monoclonal antibody into a human body, there is always a risk that the immune system will flag it as a foreign threat.

Marcus Webb

And start producing anti-drug antibodies to neutralize it.

Sarah Gellar

Which neutralizes the drug's efficacy entirely.

Marcus Webb

Exactly. The clinical fear is that the subtle structural differences in a biosimilar, you know, those minor variations from the fermentation process, could be just enough to trigger an immune response in a patient who was previously perfectly tolerant to the original drug.

Sarah Gellar

Okay, but the clinical trial data for single switches does not show any signal for increased immunogenicity.

Marcus Webb

That's true.

Sarah Gellar

However, the source material notes a pretty glaring structural flaw in how we measure that risk. Immunogenicity testing is not universally standardized across these various studies.

Marcus Webb

It's really not. The assays used to detect these antibodies vary significantly from trial to trial.

Sarah Gellar

They use different testing methods, different sensitivities, and even different baseline definitions of what constitutes a positive antibody result.

Marcus Webb

Right. It's kind of the wild west.

Sarah Gellar

So, if one laboratory test is only sensitive enough to detect a massive systemic immune response, it might report zero antibodies.

Marcus Webb

Yep.

Sarah Gellar

Meanwhile, a highly sensitive test run on the exact same blood sample might find micro-reactions. So without a universal standard, an absence of signal in a trial might just mean the researchers were looking through a blurry microscope.

Marcus Webb

That is a vital caveat. The data we have is incredibly reassuring, but the lack of assay standardization means we cannot offer a titanium-clad guarantee based on trials alone.

Sarah Gellar

Right.

Marcus Webb

That is why pharmacovigilance, the mandatory ongoing safety tracking required by the FDA and EMA after a drug hits the market, is the true safety net here.

Sarah Gellar

We are constantly monitoring those real-world registries for any unexpected spikes in immune reactions.

Marcus Webb

Exactly. And while single switches are heavily supported by this data, multiple sequential switches still make clinical pharmacologists quite cautious.

Sarah Gellar

Because of that cumulative risk.

Marcus Webb

Yeah. Every time you swap a patient to a different biosimilar to chase a cheaper pharmacy contract, you are introducing a new micro-exposure.

Sarah Gellar

A new variable.

Marcus Webb

Right. There are theoretical concerns that this formulary ping-pong could eventually provoke cumulative immunogenicity over time. The current data doesn't prove multiple switches are harmful, but it certainly doesn't endorse the practice as harmless either.

Sarah Gellar

Okay, so if the molecular data for a single switch is so robust and the clinical trials show non-inferiority, why do so many clinics report that patients genuinely feel worse after being transitioned to a biosimilar?

Marcus Webb

That's a fascinating phenomenon.

Sarah Gellar

A patient walks in and says their joints are aching, their skin is flaring up, and the new drug is clearly failing them. If the mechanism of action is identical, what is causing the physical decline?

Marcus Webb

We are looking at a classic nocebo effect here.

Sarah Gellar

The nocebo effect.

Marcus Webb

Yeah, the negative psychosocial context of the prescription swap is actually triggering somatic symptoms.

Sarah Gellar

So it's basically the psychological inverse of the placebo effect.

Marcus Webb

Precisely.

Sarah Gellar

With a placebo, the expectation of healing physically reduces pain. With a nocebo effect, a patient's deep anxiety and negative expectations about a drug actually manifest as physical side effects and decreased efficacy.

Marcus Webb

The anxiety itself can trigger stress responses that exacerbate the very inflammatory pathways the biologic is attempting to suppress.

Sarah Gellar

That's incredible.

Marcus Webb

The TRACE study provided brilliant insight into this phenomenon. Researchers monitored patients who were being transitioned to biosimilars. They found that patients who were thoroughly educated about the switch, patients who understood the totality of evidence approach and the rigorous safety data, were significantly less likely to report nocebo-related symptoms.

Sarah Gellar

Which exposes a massive vulnerability in modern clinical practice, frankly.

Marcus Webb

Oh, totally. Doctors are operating under immense time pressure.

Sarah Gellar

Right. For many prescribers, transitioning a patient to a biosimilar is viewed as a tedious administrative mandate from an insurance company.

Marcus Webb

Just a box to check.

Sarah Gellar

Yeah, they click a button in the electronic health record, hand over the new prescription, and rush to the next room.

Marcus Webb

The communication gap is profound.

Sarah Gellar

I mean, think about your last visit to the pharmacy. If the pharmacist suddenly swapped your life-saving, highly specialized medication without any prior warning just to satisfy a new insurance contract, your heart rate would spike.

Marcus Webb

You'd panic.

Sarah Gellar

You would instantly assume you're receiving an inferior generic knockoff. You would go home hypervigilant, scanning your body for every minor ache or skin blemish, convinced the drug was failing you.

Marcus Webb

It's completely understandable.

Sarah Gellar

So a purely administrative headache is translating into a biological inflammatory flare-up that completely changes the definition of what a side effect can be.

Marcus Webb

It really does, and it highlights why clinical communication is as vital as the molecule itself.

Sarah Gellar

Absolutely.

Marcus Webb

The blueprint for mitigating this nocebo effect is entirely manageable, though. First, never let the patient discover the switch at the pharmacy counter.

Sarah Gellar

Have a dedicated conversation in the clinic first.

Marcus Webb

Yes. Second, be transparent about the minor non-clinical differences.

Sarah Gellar

Like acknowledging that the injection pen might be a different color.

Marcus Webb

Or that the injection might sting a little more because the manufacturer uses a different citrate preservative.

Sarah Gellar

Oh, that's a good point.

Marcus Webb

If you proactively warn them about those sensory changes, they process them as expected variations rather than terrifying evidence that the drug is toxic.

Sarah Gellar

Right.

Marcus Webb

Finally, schedule a dedicated follow-up appointment for 8 to 12 weeks post-switch. Establishing that safety net dramatically lowers patient anxiety.

Sarah Gellar

So we have addressed the psychological component. But clinical confidence is not a static metric. How confident should a doctor actually be today when looking across the entire landscape of biosimilars?

Marcus Webb

Well, confidence is heavily dependent on the specific timeline and vintage of the drug in question.

Sarah Gellar

Meaning how long it's been around.

Marcus Webb

Right. For older biologics like Adalimumab and Etanercept, the biosimilars have been circulating in European markets since 2016 and 2018.

Sarah Gellar

So we have a lot of data on those.

Marcus Webb

Mountains of it. We have access to massive, multi-year, real-world tracking systems like the DANBIO registry in Scandinavia.

Sarah Gellar

Okay.

Marcus Webb

For those specific drugs, clinical confidence is absolute. Single switches are unequivocally supported by the data.

Sarah Gellar

But what about the newer biosimilars hitting the market right now?

Marcus Webb

Like biosimilars for Ustekinumab, which are just receiving approvals around 2024 and 2025. The analytical and structural data is incredibly strong, but the real-world longitudinal switching data is still accumulating. So the clinical posture there is moderate to high confidence.

Sarah Gellar

Meaning you proceed with the switch, but you maintain robust monitoring.

Marcus Webb

Exactly.

Sarah Gellar

And there are drugs where the medical community still needs to proceed with extreme caution, right?

Marcus Webb

Oh, certainly. We are looking at the upcoming pipeline of IL-17 inhibitors, like Secukinumab, which are currently navigating phase three trials, or the IL-23 inhibitors that are still three to five years away from biosimilar approval.

Sarah Gellar

So when those eventually launch, you can't blindly apply the soaring confidence of an eight-year-old Adalimumab biosimilar to a brand new product.

Marcus Webb

No, absolutely not. And we must always account for the clinical unknowns, which are the special populations.

Sarah Gellar

Right, because clinical trials are inherently designed to study relatively stable, predictable adults.

Marcus Webb

They systematically exclude pediatric patients, elderly patients managing complex polypharmacy, and individuals with profound immunosuppression.

Sarah Gellar

So, when you are extrapolating a biosimilar's efficacy into those highly vulnerable demographics, the standard of caution must be significantly higher.

Marcus Webb

It has to be.

Sarah Gellar

So, zooming all the way out, it becomes clear that responsible medicine kind of rejects extremes here. It is not about blindly demanding that every patient switch immediately to save the healthcare system money.

Sarah Gellar

Nor is it about stubbornly refusing to switch anyone because the concept of biological variance feels a bit uncomfortable.

Marcus Webb

Right. It's about actively matching the established vintage and data profile of the drug to the specific clinical reality of the patient sitting in the exam room.

Sarah Gellar

That is the definition of evidence-based pragmatism, really.

Marcus Webb

Exactly.

Sarah Gellar

Which brings us back to our opening scenario. The 43-year-old patient who achieved near total clearance on his original biologic.

Marcus Webb

Oh, yes.

Sarah Gellar

His doctor was agonizing over whether to fight the insurance mandate or proceed with the biosimilar swap. Based on the totality of the evidence today, what is the correct clinical verdict?

Marcus Webb

The verdict is clear. You transition him to the biosimilar.

Sarah Gellar

You do.

Marcus Webb

You do. You sit down, you invest five minutes in an empathetic, scientifically grounded conversation about why the drug is safe. You warn him about the different injection pen, and you schedule a 12-week follow-up.

Sarah Gellar

Because the data overwhelmingly indicates he will maintain his clearance.

Marcus Webb

It does. In fact, withholding that transition out of an abundance of undocumented caution ultimately does a disservice to the broader sustainability of the healthcare system.

Sarah Gellar

The source text highlighted a really fascinating psychological barrier here, actually. The dermatologist in the discussion realized her hesitation wasn't genuinely rooted in the molecular science.

Marcus Webb

Right, she knew the trial data was solid.

Sarah Gellar

Exactly. Her hesitation stemmed from the deep psychological discomfort of disrupting a patient who was finally stable. Medical professionals are human, you know? They fall victim to the status quo bias just like anyone else.

Marcus Webb

When things are quiet, the instinct is to avoid rocking the boat at all costs.

Sarah Gellar

But the clinical pharmacologist offered a brilliant reframing of that mindset. They said, "Stability is not the same as optimal."

Marcus Webb

It is a crucial distinction for any practitioner to make.

Sarah Gellar

I agree.

Marcus Webb

If clinicians prioritize the sheer comfort of a quiet status quo over integrating new evidence, medicine would just stagnate.

Sarah Gellar

Right. Dosages would never be optimized, outdated treatments would never be retired, and the systemic costs of healthcare would become completely unmanageable. That perfectly sets up a final thought for you to mull over as we wrap up this deep dive. We can clearly see how a doctor's instinct to cling to a comfortable status quo can inadvertently prevent a patient from receiving sustainable, optimized care. But step outside the walls of the medical clinic for a moment. Where else in your life are you letting the sheer comfort of a stable status quo prevent you from adopting a change? A change that might require a slightly uncomfortable transition at first, but is ultimately much more sustainable for you and for the larger systems you participate in. Something to think about.

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Sarah Gellar
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Cite This Article

Gellar S. Is it safe to switch biosimilars?. The Life Science Feed. Published May 28, 2026. Updated July 9, 2026. Accessed July 13, 2026. https://thelifesciencefeed.com/podcast/2026-05-28/is-it-safe-to-switch-biosimilars.

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