Welcome to BioArctic Q4 Report 2024. For the first part of the conference call, the participants will be in listen-only mode. During the Q&A session, participants are able to ask questions by dialing #5 on their telephone keypad. Now, I will hand the conference over to CEO Gunilla Osswald and CFO Anders Martin-Löf. Please go ahead.
Good morning, and welcome to BioArctic's presentation for Q4 2024. Next slide, please. I'm Gunilla Osswald, I'm the CEO of BioArctic, and I will share today's presentation with our CFO Anders Martin-Löf. Our Chief Commercial Officer, Anna-Kaija Grönblad, is also here for the Q&A session after the presentation. Next slide, please. BioArctic is listed at Nasdaq Stockholm Large Cap, and this is our disclaimer. Next slide, please. Today, I would like to start with this slide, which I believe says a lot about the current status of BioArctic. First of all, I continue to be very excited about our BrainTransporter technology. We had a very important event in December with the first license agreement that was signed, including the BT technology, and that was with Bristol Myers Squibb. It's now pending the HSR clearance process.
I think this is very important also since it gives an external validation of our platform, as well as it opens up for further partnerships. The second part I want to mention is exidavnemab, which started phase IIa during Q4 last year, and it's progressing really well. All patients have already completed their screening phase for the low-dose part of the study. Thirdly, Leqembi sales continue to increase, and more and more patients are getting access to the treatment. We believe this is just the start, and continued development of more convenient dosing and more convenient diagnosis will continue to drive the growth going forward. Based on these achievements, BioArctic is now entering a new era, which I call BioArctic 2.0. That's based on that we now have continuous revenues with royalties. Quarter by quarter they are increasing. We're not anymore dependent on the very irregular milestones.
That leads to that we'll get more stable finances, and we expect to be profitable from this year and onwards. Our brain-transporter platform has been validated, and we have a strong partnering interest, which could potentially lead to several partnerships in the future. Our alpha-synuclein portfolio with exidavnemab and BT2238 is also receiving a lot of interest among external partners. Next slide, please. BioArctic is a global pioneer in neurodegenerative disorders. We are among world leaders as innovators in two different areas. The first one is in generating highly selective antibodies targeting aggregated forms of misfolded proteins for, for example, Alzheimer's disease, Parkinson's disease, and ALS. The second part is our brain-transporter technology, which helps biological treatments come better into the brain and coming closer to the target.
Our business model focuses on innovation of new treatments for neurodegenerative disorders and the blood-brain barrier technology, which also makes us now also be a platform company. An important part of our business model is partnering, and we see three types of partnering. The first one is for large indications like Alzheimer's disease and Parkinson's disease, where our aim is to license the project to a strategic partner before phase IIb, or at least before phase III. For orphan indications, BioArctic can drive our programs longer and potentially all the way to the market. For our BrainTransporter technology platform, we can also partner with companies that want their biologics to get increased brain penetration. Next slide, please. I will continue on that path and talk about the license agreement with BMS, which is a key event for BioArctic.
It's a global license for our PyroGlu-Aβ antibody program, which includes BAN1503 and BAN2803. BAN2803 is also utilizing the BrainTransporter technology, and the license was signed on the 19th of December. We had several interested parties, and BMS were fast and committed with a very good offer, and as I have said before, we are discussing with different potential partners, and if we find the right partner with the right proposal, we will partner, and in this case, it's a very good strategic fit for both parties. It came a little bit faster than I had expected. BMS is a great partner for the PyroGlu-Aβ program with patients in focus. We are now preparing for BMS to take over the projects, but we have to wait for the agreement to be cleared by the HSR process before the agreement can be concluded.
This is our largest agreement that has been signed so far, and one of the largest ones globally for such an early project. The agreement includes $100 million upfront and another $1.25 billion in milestones, plus tiered low-double-digit royalties on global sales. Importantly, BioArctic retains all other rights to the BrainTransporter technology outside of the pyroglutamate Aβ field. So I think that we can utilize this for several future potential partnering agreements. Next slide, please. The BrainTransporter platform continued to progress well and according to plan. We had in our plan that we were going to present validation data in the last quarter last year, Q4, and those data demonstrate rapid, broad, and deep brain distribution by utilizing the transferrin receptor. This could then lead to increased effect, decreased side effects, lower dose, and more convenient dosing.
I think that the next generation treatments for CNS will most likely include a blood-brain barrier technology. We continue to evolve our BT technology with different ways of engineering, depending on which the target is, if the target is extracellularly or intracellularly, or if we want to come into the lysosome in the cell or outside the lysosome, but still in the cell, so it's different ways of engineering the BrainTransporter . We have a versatile platform which can be utilized across modalities. We have started with antibodies and enzymes, and we are now also looking into other modalities, such as antisense oligos, etc. We experienced great interest at JPM in San Francisco in January and continue with several discussions regarding potential future partnerships, and we are excited about the discussions, but of course, we expect these discussions, as always, to take some time.
It's important for us to find the right partner with the right terms and the right commitment. Next slide, please. Another great achievement in Q4 last year was that exidavnemab, our alpha-synuclein program, started phase IIa in Parkinson's disease patients. And we are also now exploring the potential to include patients with multiple system atrophy, MSA. The study is progressing very well, and the low-dose part of the study is already fully recruited. And then there is three months' dosing and then follow-up. And we are now preparing for a safety interim review in the Q3 this year before progressing into the high-dose part. And we expect full study results the first half of next year. I think that our alpha-synuclein program is very exciting, especially based on two different things.
One is that we have a highly selective antibody, and to our knowledge, it's the most selective antibody which is binding strongly to the pathological forms of alpha-synuclein while sparing the physiological monomeric forms, and the second aspect is that we see several opportunities for indications going forward. For example, in Parkinson's disease, Parkinson's disease dementia, Lewy body dementia, prodromal Parkinson's disease, and multiple system atrophy, and all data that we have generated so far really support further progress, so really exciting about this program, next slide, please, then let's turn to Leqembi. The number of patients treated with Leqembi continues to grow, and it's more than 20,000 patients treated by now. And I think it's reassuring to hear that the clinical safety experience is on par with what was reported in the phase III program.
If we start on the regulatory side, Leqembi is now approved in 10 different geographies, with Mexico and Macau added now in January. Regulatory reviews are also ongoing in 17 additional markets and regions, including the European Union. In the EU, CHMP gave a positive opinion the 14th of November last year, and we were waiting for the European Commission decision in January. But the European Commission has asked the CHMP to consider two questions regarding information on the safety of Leqembi that became available after the adoption of the CHMP opinion in November, and whether this may require an update of the opinion, and to consider whether the wording of the risk minimization measures in the opinion is clear enough to ensure correct implementation. Our partner, Eisai, who are driving the regulatory process, they believe the existing information is clear and sufficient to address the questions.
We now expect the CHMP meeting the last week of February to address these questions. We are looking forward to the response from the European Union, and I really hope that European patients can get access to Leqembi soon. In January of this year, the FDA approved less frequent maintenance dosing intravenously every fourth week. This means that after 18 months' treatment, patients could reduce their dosing to once a month for the maintenance phase. I think this is a great step since it is important to continue dosing to get the most benefit for the patients, also after that the plaques have been cleared. In January, the FDA also accepted the new application, the new BLA for the subcutaneous autoinjector with maintenance dosing. The PDUFA date has been set to the 31st of August.
If we then look at the development side, the AHEAD 3-45, the phase III study, completed recruitment mid-October, and this study is for pre-symptomatic Alzheimer's disease, which means individuals with elevated levels of amyloid deposits in the brain, but they do not yet have any symptoms. They will receive treatment with Leqembi or placebo for four years. During the latest Alzheimer's Congress called CTAD, ASI presented new data from the phase III Clarity AD study, further supporting early and maintained treatment. Data presented at CTAD suggests that initiation of Leqembi in early stages of the disease can support clinical stability and even improvement in many patients if you start very early. I think this is positive news for the AHEAD 3-45 study, which will evaluate the possibility to prevent or delay onset of Alzheimer's disease.
Long-term data over 36 months from the open-label extension study were also presented at CTAD, suggesting continued benefit over time and the importance of continued treatment even after plaques have been cleared, and to maintain the suppression of the Alzheimer's pathology. This makes the less frequent maintenance dosing a benefit for the patient. I think it was also reassuring to hear that the clinical safety experience in clinical practice is on par with what has been reported in the phase III program, and if we look at the commercial side, as I said, we have more than 20,000 patients on Leqembi treatment globally, and the number of patients that are getting access is constantly increasing, and Anders will talk more about this. Next slide, please. I want to point out three major things that could broaden the use of Leqembi and accelerate the uptake of Leqembi.
The first one is subcutaneous autoinjector, which I think will make it much more convenient for the patient. And the first BLA has been submitted for maintenance dosing with the PDUFA date, as I said, late August. Thereafter, ASI planned to submit a supplementary BLA for subcutaneous autoinjector administration for the induction phase as well. The subcutaneous administration will make the treatment much more convenient for patients and caregivers with at-home administrations and with less requirements and lower costs for administration compared to intravenous administration. The second aspect is simplified diagnosis based on blood-based biomarkers. Today, blood-based biomarkers are being used for screening, and then they should be confirmed by PET or CSF. Within the next year, we believe that blood-based biomarkers will also be accepted as confirmatory. And this will be making the diagnosis considerably simplified and increasing the opportunities for primary care diagnosis.
The third aspect is to broaden the indication to even earlier stages of Alzheimer's disease, as I alluded to with the AHEAD 3-45 study in pre-symptomatic individuals, even before the symptoms appear, but the individuals have elevated levels of amyloid beta in the brain. So I think Leqembi has huge opportunities to help many patients, and we expect the uptake to be more rapid, especially from 2026 and onwards. Next slide, please. So in summary, our portfolio is progressing really well, all the way from very early innovative discovery and all the way to helping patients on the market with these devastating diseases. And today, I have highlighted Leqembi, exidavnemab, our PyroGlu-Aβ programs, and our BT platform. And I'm really pleased to note that BioArctic's innovations and research with high quality is being recognized externally. Next slide, please.
And then I will hand over to Anders Martin-Löf for the financial summary.
Thank you, Gunilla. I will then start to focus on the Leqembi sales. As you can see here on the slide, the global sales for the Q4 of 2024 were JPY 13.3 billion. That corresponds to $87 million, i.e., a 33% increase from the Q3 of 2024. So we now really see a solid development. And of course, if you compare year over year, it is more of a tenfold increase. So we are in a rapid growth phase. For us, this means that the royalties increased by 38% from the Q3 to SEK 96.7 million, or for the full year, we recorded roughly SEK 230 million in royalties. This is primarily then driven by the US expansion. It is now in line with the updated forecast that Eisai issued in their last quarterly report.
The US sales were JPY 7.7 billion, corresponding to $50 million, which means that the sales grew by 31% over the Q3 numbers. And we're now up to 13,500 patients. As you may recall, Eisai described the problem with an infusion capacity bottleneck in their last quarterly report. And now that problem is being resolved. The capacity has been increasing rapidly. So the 6,000 patients that Eisai hinted were waiting for treatment due to capacity issues are now being included at a very rapid pace. So now they're up to 3,500 patients. So they are really working hard to resolve that problem. Over time, the infusion capacity will also become less of a problem. Already now, maintenance therapy, as Gunilla mentioned, is approved in the U.S. with using infusions, so that reduces the number of infusions for patients that have been on treatment for a long time by 50%.
But also, even more importantly, the subcutaneous version removes the need for infusions entirely. And we expect that to be approved for maintenance therapy in the Q3 of this year. And Eisai has guided that they also expect induction therapy with the subcutaneous version to become approved in the first half of next year. So all in all, we believe that the growth will continue in the U.S. in 2025. And in 2026, there will be a much stronger focus on the primary care sector. And Eisai has started preparation for that already now in 2025. So we will see a shift moving over more to general practitioners in the primary care sector going from specialists only. In Japan, we saw a really strong development. Japan has been a really strong market from the very beginning. The sales were JPY 4.1 billion in the Q4, corresponding to $27 million.
Strong 49% growth over the Q3. And as you can see, the number of patients is more than half of the numbers in the US, even though Japan is a much smaller market and the drug has been on sale for two quarters less in Japan. So really, really strong development there. And there you can see that Eisai has already started promoting directly to consumers to raise awareness about mild cognitive impairment and to promote early diagnosis. And I think that is the way to go also in the US. And that's the development that we expect to start in the US as well. China is also very strong. It may seem that it's not growing since the sales in the Q4 were roughly the same as in the Q3, coming in at JPY 1.3 billion or $8 million.
However, the sales in the first quarter of sales in China, which was the Q3, were probably a little bit stronger than the underlying demand, as there was some inventory build-up. So all in all, I would say China is moving really well. The underlying demand is increasing, and we will continue to see solid growth there, even though ASI is only selling towards the private market. But that's still a significant market. To conclude, we believe that ASI is on track to reach their financial year forecast of JPY 45.5 billion. That is for the period that started in the Q2 of 2024 and that will end of March 2025. That then will correspond to $280 million.
As you can see from the accumulated sales in the first three quarters of that period, that were JPY 29.6 billion or $194 million, they need to generate roughly as much sales in the coming quarter as they did in the last quarter to reach the forecast. We believe that they will continue to grow. We believe there is a very high likelihood that we will actually beat their forecast. Going forward, as Gunilla mentioned, we believe that we will see continued growth in 2025, but really, it will be incredibly exciting to follow what will happen in 2026 when the blood-based biomarkers really make a dent in the diagnosis process and the subcutaneous version becomes available so that the patients can take the drug at home or in a much easier way with the healthcare practitioner than they do today with infusions.
So we believe that 2026 will be a very exciting year to follow. We then turn to the next slide, looking a little bit more detail on our figures. Starting on the left-hand side, you see that our net revenues were SEK 101 million for the quarter. Historically, as you can see, they have been fairly lumpy, and it has been smoothing out a little bit now when the royalties are growing. I'm happy to say that it will be lumpy again since we will start to generate quite significant milestones in 2025. We have already said that we expect a $100 million upfront payment from BMS that will be recorded in its entirety when the agreement is closed. We're also expecting some milestones from ASI, so we could probably expect some 30% more than we expect from BMS by milestones from ASI.
So all in all, I would say in the sort of $130 million range for 2025. Over time, the recurring revenues will increase, but not then in 2024. You see, the royalties were $97 million in Q4 of this year. They will continue to grow, but they will be smaller than the milestones in 2025. The co-promotion revenues will also start growing over time, but probably not to a significant level in 2025, as the launch in the Nordics will most likely take place in the beginning of 2026 rather than in 2025. If we then turn to the costs in the middle graph, you see that the operating expenses increased to $143 million in Q4. R&D was roughly 67% of that. And the total costs for 2024 were $459 million. That's actually a little bit lower than we guided for the year.
That is due to the fact that there were some CMC costs that did not occur towards the end of the year since we entered the deal with BMS. I guess that's beneficial that we were lower than our forecasted costs. For 2025, we do expect the costs to increase. Our project portfolio is progressing well. We spend more on our clinical trials and CMC programs. We expect the costs to increase by roughly 50% to 80% in 2025. It's really hard to make a good estimate, so we will have to come back to that. If I would guess today, we are, I would say, in the 50% to 80% increase range. Looking then at the operating profit, our operating loss was SEK 53 million for the Q4. As Gunilla mentioned, we are expecting to be very profitable in 2025.
And if you put the numbers together, the pre-tax profit for 2025 should be in the neighborhood of roughly SEK 1 billion, which is a really, really strong result for a company like ours. If we then turn to the next slide, some more details. You see the net result for the Q4 was SEK 31 million. That's roughly SEK 20 million better than our operating loss. So that's primarily due to the financial net of roughly SEK 10 million and the negative tax effect of SEK 12 million. If you look at the cash flow in the middle graph, it was roughly in line with the result. Typically, it's usually a little bit worse than our result since we have accounts payable that continue to grow with the growing royalties since there is a lag between the payments and the recording of the revenues.
But this time around, we did not see that effect. But going forward, we still expect to see the cash flow trailing the net result. And on the right-hand side, you see our cash balance. We ended the year with roughly SEK 780 million in cash. We, of course, expect that position to grow significantly in 2025. So we will end 2025 with an even more solid position so we can really focus on doing what is right long-term for the company and sort of focus on the right projects and focus on entering the right deals. As Gunilla mentioned, we will partner our programs if we find the right deals, but we don't have to. And that's a significant strength that I'm really happy to have as CFO of this company. So with that, I will hand the word back to Gunilla for some closing remarks.
Thank you so much, Anders, and then we're coming to the final part of the presentation with upcoming news flow and some closing remarks. Next slide, please, so if we look at our upcoming news flow, during this quarter, we are eagerly awaiting the HSR clearance process for the BMS agreement, and of course, we hope for a positive outcome to be followed by an upfront payment of $100 million. We are also eagerly awaiting a CHMP response at the end of February, and we are looking forward to more regulatory responses. Next important congress is AD/PD in Vienna in the beginning of April, and there we look forward to presentations on both lecanemab and also on exidavnemab. We are also preparing for our first capital market day, 2nd of June.
And then during the Q3, we are waiting for more regulatory responses and the exidavnemab safety review and progression into the high-dose part of the phase IIa study to follow that. So then we go to the next slide, and I would like to summarize today's presentation by saying that our pipeline is progressing really well, and we have very encouraging BrainTransporter data that has been presented and generating a lot of interest. Leqembi is now approved in 10 different geographies, and the sales of Leqembi continue to increase. Royalties revenues continue to grow, and it's gratifying to see that we're helping more and more patients. And thirdly, our financial position remains strong. We have almost SEK 800 million in cash, and we expect to be profitable this year and onwards. Next slide, please.
So, by that, I thank you for your attention, and we're happy to take some questions.
If you wish to ask a question, please dial #5 on your telephone keypad to enter the queue. If you wish to withdraw your question, please dial #6 on your telephone keypad. The next question comes from Joseph Hedden from Rx Securities. Please go ahead.
Good morning. Thanks for taking my questions. Firstly, to Anders, just on the milestones, just hoping to clarify there. Was that you're saying you expect in the ballpark of $130 million is available overall? And so that includes the BMS upfront payment and then presumably the EU approval milestone, but also possibly a sales milestone in there?
Yeah, that's correct. I messed it up a little bit. So yes, we are expecting $100 million from BMS and then roughly, well, a third of that in addition from Eisai. So you're correct. We're expecting a sales milestone and a regulatory milestone from ASI.
Okay, brilliant. That's great. Thanks. And then possibly just on now that we've had a couple of weeks since finding out there were additional questions after the positive CHMP, have you been able to find out what additional kind of safety information that came out that has been referred to by the European Commission? What was the new emerging data after the CHMP?
So I don't think we should comment anything about an ongoing process. So we just have to wait now and stay tuned and wait for the review. But I think, I mean, what we have been reassured by ASI is that there are no new safety signals that the current information and the data which is available should be able to address the questions.
Okay, thanks. And then just lastly from me, when you're talking about the BMS deal, and congratulations, it's a fantastic deal. You said that several parties were interested. So where are you seeing the interest there? Is that specifically in the pyroglutamate antibody portfolio, or is it for programs involving the BrainTransporter technology specifically?
I would say both. And what we see now is continued interest both on our BrainTransporter technology to utilize that together with other companies' assets. And for example, also for our alpha-synuclein portfolio, where we have exidavnemab, and we have also an antibody combined with our BrainTransporter technology that we call 2238. So I would say both.
Okay, that's great. Thanks, Gunilla. Thanks, Anders.
Thank you, Joseph.
Hi, team. Thank you for taking my questions. Maybe a first one in terms of...
The next question comes from Luísa Morgad o from Van Lanschot Kempen. Please go ahead.
Hi, team. Thank you for taking my questions. Maybe to start out, you mentioned the costs over 2025. Could you elaborate a bit in terms of where do you expect to, of course, redirect the stream that you will have from the royalties and the BMS deal? What are your priorities within your pipeline?
So yeah, if I start a little bit, I mean, we focus, of course, on the most fully developed program that we have in our pipeline. And when we get closer to the clinic, then we will start to generate significant CMC costs. And then, of course, we are running one clinical program for exidavnemab, and the cost for that will continue to increase.
As for what other program we can engage in in the future, we will probably come back a little bit more on our capital market state to see what we do in the future. Maybe Gunilla wants to comment on more than that.
Yeah. No, but I think definitely, I mean, exidavnemab, when you are in clinical stage, that costs a bit more than being in the early discovery stage. And then also, I mean, we have another really interesting program we haven't talked about today, which is also Alzheimer, the next generation Alzheimer program that we are evaluating together with ASI, BAN2802. That's also a very exciting program that we, of course, will continue to invest in. And then also the BrainTransporter. I mean, that's an area where we invest and will continue to invest.
Because as I tried to explain, I mean, there is a lot of opportunities for this technology, and there is so much more we can do also with our programs, but also to prepare this technology for other modalities and so forth, and then we haven't talked today about our TDP-43 program, but that's also a very important program, both with naked antibodies, but also combined with our BrainTransporter technology, and then, I mean, the GC ase program for Gaucher disease, where we are opening up the avenue also with enzyme replacement therapies, so I think that we have some really, really interesting programs at different stages in our portfolio, and then we will, of course, look at expanding when we have more money.
Okay, perfect. That's very clear. Maybe a final question in terms of, so you mentioned the blood-based biomarkers that should be approved very soon or somewhat soon and could be confirmational as well. Could you expand a bit here in terms of what do you expect of how this will be combined, of course, with all the other methods of diagnostics and confirmational, of course?
Yeah. I think right now, I mean, they are already used for screening and in different kinds of triaging systems. I mean, if you have clearly a strong result, then you know that you have an amyloid pathology. And if you don't have it, then you know it's something else. It's not Alzheimer's disease. It's especially in those in the middle where you need to have the confirmational part through PET and CSF, or CSF, I mean.
But I think now also more and more data is coming in, and they're working on, I mean, both the regulatory processes and use the guidance and so forth that will also then help with the confirmatory part directly. And I think that would be very important because that opens up. So then you're not dependent on PET scans and PET centers and so forth. You are not dependent on doing CSF sampling and lumbar puncture. So I think that will open up the possibilities for a much, much more broad spread. So I think this is a really important part. And I'm so pleased to see that it's going faster than I thought some years ago, and it's really progressing so well. And there are several companies who are developing blood-based biomarkers.
Of course, we are agnostic to which one it is, but I mean, there are several coming that can help to simplify the patient journey.
Okay, Claire, thank you for taking my questions. That's all.
Thank you so much, Louisa.
The next question comes from Rajan Sharma from Goldman Sachs. Please go ahead.
Hi, thanks for taking my question. So firstly, just on exidavnemab, sorry, in MSA, could you maybe just kind of talk to your rationale for exploring the drug in that setting? And then also, could you just kind of help us understand specifically what it is you're exploring? Is it still dosing, or is it just trying to gain additional confidence in the mechanism? And then secondly, when would you expect an update on a go-forward decision? And then I have a follow-up for Anders as well.
Yeah, so if I start then with exidavnemab, I mean, we are really pleased to see how the progression of the phase IIa study in Parkinson's disease, how that is evolving. And we started with a low dose first, and then we will do an evaluation of the safety in Q3. After that, we will then go to a higher dose in Parkinson's disease. And we are also thinking about then going into another panel with MSA patients in order to prepare for different to open up more possibilities for phase IIb. And as I said, I mean, I see several possibilities for phase IIb. It could be Parkinson's disease. It could be Parkinson's disease dementia. It could be Lewy body dementia. It could be preclinical Parkinson's disease. And it could be MSA. So what we are doing is really preparing ourselves for different opportunities for phase IIb and onwards.
Okay, thank you. And then maybe just to clarify on that then, so if you decide to progress in MSA, for example, does that mean you won't progress in some of the other indications, or could you potentially do multiple indications with the drug?
So I think, I mean, there are multiple opportunities. And I think that we will follow, of course, the whole field of alpha-synuclein, but there are many possibilities. And we have also then, of course, I mean, we have exidavnemab, and we have also the next generation, 2238, with BrainTransporter. So we see different opportunities or different possibilities to drive in several indications. And we are at the moment reviewing different opportunities and different pros and cons with different indications. So we will come back to that.
And also it depends on, of course, if we are doing this ourselves or if we have a partner at that stage.
Okay. Perfect. Thanks, Gunilla. And then I just had a follow-up for Anders on expenses in 2025. And I think you said 50% to 80% growth in 2025 on expenses. So could you just kind of help us understand what gets you to the bookends of that range? And then maybe if you could just discuss expectations for tax in 2025 as well. Thank you.
Right. No, so well, most of the increase will, of course, then come in R&D. And it's very, very hard to give a proper forecast for R&D costs because it really depends on how fast our programs evolve.
So we may have a guess in the beginning of the year, and then things start to go faster in some projects and slower in other projects, and that's a big, big effect on the costs. So I don't really want to go into too much detail because then I will just be wrong because things will really evolve during the year. But expect most of it to come in R&D, most of the increase. And for the tax, yes, if we, for example, would make a pre-tax profit of SEK one billion, we will pay roughly SEK 200 million in tax for 2025. So we will be paying taxes, and it will probably be in that range that I mentioned.
Thank you very much.
Thank you. There are no more phone questions at this time. So I hand the conference back to the speakers for any written questions and closing comments.
Okay, thank you so much, so we've gotten a few written questions. I'll start with one from Frederick Tor at Redeye, and he wants to know if we're planning any study with lecanemab in patients with Down syndrome. That's something we've been talking about in the past. Gunilla, maybe you can clarify.
Yeah, thank you for the question, Frederick, so as you know, I mean, we have data showing that lecanemab binds to postmortem brains of Down syndrome, which is exactly what you would expect, and we are reviewing this opportunity and having discussions. This is a patient population where you should be a bit careful because they have a higher risk of side effects, but also they have an opportunity to get an effect, so yes, we have plans, but it's not imminent, but we are definitely looking into this for the future.
Good. Thank you. Nils Åker Törlin has written a bunch of questions. Some of them came early in the call, so I think we've answered most of them. He wants to know a bit about if we can say anything on the competition with Eli Lilly. I think that might be something that we haven't commented on. The subcutaneous, we've talked about the different adverse events, if we can say anything about that, but I think you mentioned, Gunilla, that they are in line with the phase III studies as far as what we've seen so far, but maybe if you want to say anything on what we see in competition or what we've heard about competition yet by either Biogen or Eisai, what they've mentioned. Do we have anything we can say? Not really, right?
Eisai commented a little bit. In the US, they are, of course, seeing competition from Kisunla. They are not sort of overwhelmed by the competition. And so it hasn't had a really large impact on their sales. That was their comment. As for the traits of the products, how they are compared with each other, we won't comment on that. There haven't been performed any comparative trials, so we refrain from commenting on that.
I think one clear benefit for Leqembi will be in the future, the subcutaneous administration, for example.
Yeah. Payments from BMS to expect in 2025, Anders, I think you've mentioned the expectation there.
Yes. So we expect to get the upfront payment once HSR clearance has been achieved and the deal has been closed. So that could be recorded in the first quarter if everything goes to plan. So then we'll record the full $100 million. Other than that, we're not expecting to record any other revenue in 2025 from BMS.
Thank you. And then, Gunilla, you did mention there was a question here about the why not collaborate with ASI regarding BT, but you mentioned about.
We are. So maybe I should clarify that. Yes, we are collaborating with ASI also on the BrainTransporter technology. I mean, this technology can be utilized for many different programs. And we have then the PyroGlue program has now been partnered with BMS, but we also have the BAN2802, which also is an undisclosed target for Alzheimer's disease, disease-modifying properties that we have combined with our BrainTransporter technology. And that is in a research evaluation agreement and a collaboration with ASI where we are reviewing that program. So definitely.
And additional potential BT agreements, I think you also highlighted as a great potential for the future. So I think we mentioned that.
Then we have a question here from Yoel Blad, and he wants to know if we can elaborate a bit further on the CHMP meeting in February and then how long after that meeting that we can expect a decision from the EU Commission. And also then if that could be when the sales could start in Europe following a positive decision from the EU Commission.
So I will start, and then I'll hand over to Anna-Kaija. So I'll just say, I mean, the CHMP meeting, as I said, we now will be eagerly waiting the outcome of their discussion at the end of February. And then after CHMP, the normal process is then that it goes to the European Commission. And we expect then their response within 67 days. And we just have to have patience and wait and see. So that's the process.
And then when do we expect to start selling in Europe, Anna-Kaija?
Well, I think maybe something to add here is also that, of course, after the formal EC decision is the clarification of the risk minimization measures with the CAP and the PASS. So it depends also a little bit on that when those are approved and rolled out. And usually, I mean, the first countries to launch in Europe, as you probably know, is in Germany and Austria. But I think there's a lot of question marks around those still steps that you mentioned. So it's difficult to set a date, I would say. And it's up to ASI to comment on that.
And then in the Nordics, when can Nordic patients have access, Anna-Kaija?
Yeah. And as you know, we have then the market access process with the HTA countries. So we will have to start with the health economic evaluations. And when it comes to those timelines for hospital products, there is no exact timeline. But based on ASI and our experience, it's usually around a year at least. And especially since this is a new treatment modality which is coming for the authorities. So we expect that there will be, of course, a need to educate on the therapeutic area, and they will probably have questions on how to evaluate the effect, etc., etc. So I think we shouldn't underestimate that need to educate also the authorities and payers on this specific area and Leqembi. So it will take some time, but we are prepared for the questions with ASI. Thank you.
Thank you. We have another question from Frederick from Redeye. And he's wondering about the timeline of the BMS program. If we can say anything about that, when do we believe that could reach the clinic and then potentially the market? And anything we can say on market potential or addressing patient population and if there's anything that differentiates it from Leqembi in that sense when it comes to potential patient population?
So I can just say that. I mean, now it's, of course, up to BMS to drive this forward. We had in our plans to go into phase I next year, 2026. But of course, it's now up to BMS how they will drive this. They are very committed and have great plans for this program, but I will refer to them to comment on that. But I see. I mean, there is a huge market potential both for example 2803 and for 2802 and for many others.
I mean, this is a huge patient population where there is a clear unmet medical need. I think Leqembi is coming and really being the first one to help out, but I think there will be more, and there is room for many different alternatives in the future. So I think that's my answer right now.
Yeah. Good. Then we have a couple of questions here from RBC. And then the first one is, do we believe that the maintenance approval, and I assume that that refers to the IV approval that came just now, will move the needle in any way for Leqembi when it comes to the launch? Or do you think it's more of a wait and see for the induction dose of subQ before we really can see a difference in the market?
I think it is an important approval because the patients who have been on treatment for 18 months, of course, it's good for them to be able to have less frequent dosing. So they want to continue dosing and getting the most benefit out of the treatment. So I think it is important. And then when they also then later on get the subcutaneous alternative instead, even more convenient. But of course, the most important one is when we have the subcutaneous auto injector also for induction, and that's 2026. But I think every approval is important, but the subQ will definitely, I expect, to move the needle.
Yeah. Thank you. And then beyond infusion capacity, which we know has been somewhat of a hurdle in the US, which now, as Anders alluded to, seems to be easing off. Are there any other hurdles on getting patients started that we can comment on?
I mean, of course, there have been other challenges, for example, with the diagnosis side. If you are depending on a PET scan and the reimbursement of PET tracers, which has also been solved to some extent. And also, people have gotten more and more used to doing CSF sampling and lumbar puncture. But of course, the blood-based biomarkers will really help here. So I think that is an important part as an example. And I think what the blood-based biomarkers already have helped to make sure that those patients who are coming for confirmatory through CSF or PET scan are the right patients and have not been diluted into patients who are not the right patients as a capacity issue. So I think that, I mean, step by step, there are several things happening. And Anna-Kaija, I want to add.
Yes. I think also what we hear, both from the U.S. market, but also here in the Nordics, is that I think the quality of the patients being referred to the memory clinics also needs to be improved, I would say, because if you look at some studies that have been done both in the U.S. and in Sweden, is that there's only a fraction of the patients today at the clinics who are kind of eligible for a potential treatment. So I think that this will be an important thing to work on for the clinics and for us in the future.
Thank you. And then a question from Peter Herrmann. How important do you consider the AHEAD 3-45 study to be for the extended use of Leqembi in the long run? And it seems to him to be a very important study. And he also talks about competitors. Maybe we can just comment on if there are any similar studies ongoing as well.
I'm really excited about the AHEAD 3-45 study, especially when you look at the data that Eisai have presented from the CLARITY AD study when they look at the very early patients who have lower levels of amyloid in the brain, or if you look at those with low TAU, for example. If you look at those patients who are at a very early stage, they seem to have a quite high proportion of being stable or even improve. I think in this AHEAD 3-45 study, by starting early individuals who have the pathology, but not yet symptoms. Think about if we can really push forward the time for when symptoms appear or potentially maybe even stop. I think this is a very important study to follow.
And I think ASI is doing a tremendous piece of work here together with the Alzheimer Clinical Trial Consortium who are driving the program. And they are really pioneering. There are other studies also in this area since the whole field realized that it might be even better to go as early as possible. So I think this is really good for patients that we will be following. And then again, blood-based biomarkers will be very important. And they're already utilized in the AHEAD study in the screening phase.
Thank you, Gunilla. Thank you, Anders. Thank you, Anna-Kaija. I think that was the last question that we have here. And there doesn't seem to be any more people on the phone lines either calling in. So I think that concludes today's call. Thank you, everybody, for listening in, and see you next time.
Thank you. Bye.