Okay, good afternoon and welcome to day one of the Barclays Global Healthcare Conference. My name is Carter Gould, covering U.S. biopharma. I'm pleased to welcome Merck to the stage. Merck is one of our top picks to start the year, and it's been a good year for Merck. Joining us from the company, Jannie Oosthuizen, President of Human Health U.S., as well as Peter Dannenbaum from the IR team. Welcome, Merck. Thank you very much for joining us. Maybe before we get started, we can either just jump into Q&A if you want to make some opening comments, but I think we were just going to jump in as we discussed here.
Well, I mean, I can just make a few comments, but thank you for having us, Carter. It's good to be back. You said it. I think it's an exciting time to be at Merck. We're benefiting from strong execution across our clinical program, across our commercial organization, and we continue to anticipate good growth as we move forward, driven by our key products: oncology, vaccines. We're also very excited this year to launch the V116, but I'm sure we'll get into. We're also starting to see our pipeline maturing. We're getting line of sight of significant areas opening up, continuing to be in oncology, immunology, cardiometabolic vaccines, anti-infectives. So really a good place to be.
Okay, great. Well, looking forward to talking with Peter Dannenbaum as well. So thank you for that. Maybe let's start with sotatercept because we got the PDUFA right around the corner, and sotatercept has been one of our favorite molecules since the Acceleron days. Maybe start first, and Merck has been sort of very positive on the commercial opportunity here. Just kind of your level of enthusiasm around this becoming a foundational asset in PAH going forward?
Yeah, absolutely. So as I said, this is really one of the exciting launches this year. It's pretty soon. PDUFA is the end of March. And we're really excited for two reasons. The one is really it's a new area for Merck to move into, so a lot of excitement as we move into a rare disease space. But also, if you think about PAH, there's really been no significant innovation in the last 10 years, and we know this is a patient population with significant unmet needs. So we're really excited to bring a meaningful therapy to market. And I think since we've seen the data at ACC in 2023, there's just been really strong excitement within the treatment community.
We know, as physicians started to think through what sotatercept was bringing to their patient population, a lot of them have specific patients in mind that they think should receive this therapy as soon as possible. The majority of patients are treated by highly specialized PAH specialists in the Centers of Excellence. There's about 115 in the U.S. treating half the patient population and PAH experts outside of COEs. This is a close-knit community, so we know that there's a strong uptake.
Okay. I think when we spoke last year, we talked a little bit on the back end of ACC. There was some chatter around the bleeding risk. We've now seen some longer-term update data earlier in the year with longer-term follow-up, and there were some additional bleeds. Can maybe just talk about your confidence in that profile and the potential for REMS or some other kind of potential troublesome language and how that impacts the commercial opportunity, which you still seem to be very positive on?
Yeah, that's right. So we have seen with the ongoing SOTERIA study, which is the open-label, ongoing longer-term study following STELLAR, we've seen more patient observations. So there has been some differentiated outcomes with some of those additional patients coming in. But I have to say, from a results perspective, we continue to see lasting clinical benefit. We do not see discontinuations as a result of bleeding. And we've also observed that most of the more serious bleeding is associated with other conditions, whether it's low platelets, use of anticoagulants, steroid use, or maybe even prostacyclins. So certainly something that we will continue to monitor. We take this very seriously, and we will continue to report on what is observed. In terms of REMS, this is really it's a decision in the hands of the FDA, so we'll have to wait and see how they think about this.
But we feel very confident about the profile and how we think we're going to bring this to market.
Okay. And then as we think about that launch, is that something that Merck is going to make easy for us to follow, or are we going to see those scripts as they kind of hit on a weekly basis, etc.?
Yeah, I think we're working through what are the datasets going to look like. I think we would like to see the number of patients that we make any impact to. And if we have, I would say, credible data sources, we will like to report out on that as much as possible.
Okay. And then maybe just last one on that side, in terms of expanding the field for us and being in a position ready to go out of the gates here in a couple of weeks?
We are very ready. We were preparing to be ready for any early positive surprise in terms of an approval. As I said, this is a really small treatment community, so we've built a rare disease model through which we can really reach these centers effectively and keep the best support of patients and physicians who's already navigating a fairly complicated journey and make sure that we make it as easy as possible for them to access and get sotatercept.
Okay. So you had some other positive kind of updates here in the past two weeks. What we thought was a very positive ACIP meeting for V116 didn't seem to get as much attention from the street, but can you talk through sort of your takeaways from that meeting, specifically touching on the potential expansion of that standard risk population down to 50 years old?
Right. Yeah, I agree. I think it was a very positive ACIP meeting, and what we were really encouraged about was the recognition by the committee of the population-specific vaccine that we bring forward and the value of being population-specific, right? So we've often talked about serotypes. V116 is 21 serotypes. It is one more than PCV20, but the importance is really the disease coverage that comes about because of the serotype composition. And that's where we encourage about the conversation within ACIP to bring down that age recommendation to 50-64. If you just think about it, there's 120 million people in the United States over the age of 50. 60 million are sitting in this population of 50-64, and 60 million so basically 50/50, 50-64 and 65+. So this is really a significant patient population.
We also believe that an age-based recommendation is much more effective in terms of getting segments vaccinated versus a risk-based, which is what it is today. And it's also good from a health equity perspective to make it age-based rather than risk-based. So that lowering of the age recommendation is really positive in terms of the conversation. And we know that V116, because of the serotype composition, is about an 83% disease coverage, residual disease coverage for adults, which is a good 30% higher than what PCV20 is providing. So really a huge incremental benefit for patients both at a lower age as well as potential revaccination over the age of 65.
One of the things I think that there's obviously some new data cuts at ACIP that we hadn't seen before, but I think one of the things that's still a take to investors is those patients that maybe have already been vaccinated with Prevnar or at least got the first dose with Prevnar and then going in and potentially retreating with V116. Any expectation how the ACIP and the guideline-making bodies will sort of respond to that?
Yeah. So that's a population that we studied in STRIDE- 6 in terms of revaccinating everybody that's been vaccinated more than 12 months before with another pneumococcal vaccine.
Right. But it was sort of a bucket total.
Right. So in that population, we saw the immunogenicity and that expansion from 53% disease coverage to 83%. So that's where we will continue to have data exchange with the ACIP and hopefully get to that discussion to open up that revaccination above the age of 65.
Okay. And sort of this encouraging data you've seen with V116, sort of what does this then portend for your effort in the pediatric opportunity? You've talked about a second program to go after pediatrics. Is that still the game plan, or does the positive data here sort of change that plan in any way?
No, there's a few things we're doing. There's at-risk children and teenagers who could benefit from a V116 vaccination. So we studied that in STRIDE- 13. But we will continue to work on V117, which is a further expansion of our current vaccine serotype profile. So that is still early stage, but we will continue to develop population-specific vaccines, including for pediatrics, moving forward.
So I think Rob, on the last earnings call, he talked about a $3 billion TAM for V116. And when we think about that, was that sort of the adult population, as you kind of outlined it there, or is the younger, the expansion down to the 50-year-old cohort, that additional does that include the pediatric opportunities you just talked about with V116 for at-risk? Kind of what's in, what's out there?
That's focused on the adult opportunity, both in terms of lowering the age recommendation as well as that revaccination over the age of 65.
Okay. So that's two pretty compelling launches. And I guess the backdrop of, frankly, you've had a lot of KEYTRUDA line extensions in your past. It's got to be exciting to sort of have these new dynamic kind of happen.
It really is. It really is. Yeah.
Okay. And maybe one thing that also has kind of gotten lost in the mix is you're going to potentially have an oncology launch this summer too with the Daiichi asset. Can you talk about how you see that playing out and what that fits in the paradigm?
Yeah. So a big part of our business development focus has been to expand outside of oncology, but also to diversify within oncology. And we signed a fairly significant collaboration agreement with Daiichi Sankyo towards the end of 2023. That includes three ADCs. The first one is. The PDUFA is the end of June. It's a HER3 ADC that we will launch in later-stage metastatic EGFR-mutated non-small cell lung cancer. So really an exciting launch. It's a small indication, but really a launch as we get this collaboration and partnership going with our partner, Daiichi Sankyo.
Okay. And maybe you also just closed the Harpoon deal, and small cell has been sort of that maybe calling it a white whale isn't totally appropriate here, but it's been the one thing that sort of has been a bit of a challenge for Merck despite KEYTRUDA winning in a number of other places. Can you talk about how that fits in? Is that an opportunity to bring back KEYTRUDA in small cell, or is it really just sort of living on its own merits with the asset in question here?
So one of the ADCs within the deal with Daiichi Sankyo is the B7-H3, which is really the one that we're looking at for small cell. You're right. Small cell has been the most elusive, one of the most elusive parts of the lung cancer space that we've explored. So hopefully, we can crack it with B7-H3. And the DLL3 is pretty much going to play a role within the small cell investigation.
Okay. But at this point, no real sense in how they're going to kind of coexist, or?
I don't know. That's maybe a question.
Let the data play it out. Okay.
That's right.
Okay. Maybe it's a good segue to focus back to KEYTRUDA and sort of these early-stage lung approvals and how that part of the launch is going. It was a very big part of the narrative. In 2023, you told us it would take time, but it was clearly helping the sales trajectory. Now with sort of a little bit more time, maybe an update on that front.
Yeah. So I think, Carter, you're right. If you go back, I think we talked about 25% of KEYTRUDA sales will come from early stage by 2025. In fact, in 2024, about 27%-28% of KEYTRUDA sales will be related or driven by the early-stage indications. And over the past few years, we've launched in early-stage melanoma, early-stage renal cell carcinoma, early-stage triple-negative breast, and these have been strong growth drivers. And in early 2023, we launched our first early-stage lung indication with KEYNOTE- 091, which is KEYTRUDA in the adjuvant setting. And towards the end of last year, we launched KEYNOTE- 671, which is the perioperative, pre-surgery followed by surgery and then KEYTRUDA in the adjuvant phase with 671. And it's really going really well. Early stage is driving close to 60% of our oncology growth right now. So yeah.
Okay. And so when you think about sort of what's the next step to drive that inflection of adoption of KEYTRUDA here, is it just more awareness, better testing, better screening? At this point, kind of where does it sit?
I think we feel really good. We've taken a strong share leadership position already in the early stage with KEYNOTE- 091. We continue to expand that with KEYNOTE- 671. The treatment rate, there are really two big drivers if you look at early stage. The one is diagnosis in that early stage. You need to be diagnosed, obviously, and in lung cancer. That is still a big challenge. The screening rates are low, so there's a lot of work needed to further increase lung cancer screening. And then the treatment rate itself, when we launched with KEYNOTE- 091, treatment rate was sitting at around 35%. We've been able to bring that up to 60% right now. So we're making meaningful progress in terms of having diagnosed patients treated.
The other thing we need to do is we need to get more patients diagnosed in the early stage so that they can be treated.
Okay. That's probably a good segue to the subcutaneous KEYTRUDA and how that fits in here and to the extent that it can help accelerate things into earlier adoption of KEYTRUDA in the adjuvant setting. I mean, I think there's always a focus on sort of potentially extending the life of KEYTRUDA, but maybe that's too simplistic a way of thinking about it, and there is sort of a broader opportunity in growing the pie, right?
Yeah. I mean, SubQ has really been a focus to innovate for patients, right, in terms of bringing a level of convenience in a difficult disease where you have to come back frequently for an infusion, right? So the one aspect is to really make it as simple as possible for patients to be longer-term on an infused product like KEYTRUDA. And the second one is there's also a significant efficiency for the practices administering these medications. So we are developing a Q3W formulation of SubQ KEYTRUDA as well as a Q6W. We see the although the Sub Qs can be used for any one of the KEYTRUDA indications in combination with any medication that is in label, we see it really as of particular value where KEYTRUDA is used either as a monotherapy, and that could be in some still some metastatic settings.
But in particular, in the early stage, if you think about the adjuvant phase where patients come back for almost a year, if they can get just a SubQ injection every six weeks in a few minutes, that's a very convenient way. And then where KEYTRUDA is used in combination with oral anticancer treatments, right? So really, you don't need to sit in an infusion chair. It's an easy way of administering it. But again, as I said, physicians can obviously use it in combination with infused treatments as well.
Okay. And we're still going to get that data, hopefully, by second half of this year and that we're going to support.
Yeah. That's right. Yeah.
Okay.
I think it's September this year that we'll see the data.
When you think about how much of the opportunity SubQ might be able to let you hold on to, certainly, your competitors have put out different bogeys in terms of what they think. Love to hear the updated Merck line.
Yeah. So that optimal place where we think SubQ can provide the most value for patients and practices, we project that to be more or less 50% of the KEYTRUDA volume by 2027, 2028. So we would say that about 50% of KEYTRUDA volume that would be a good place to use SubQ KEYTRUDA.
Okay. And then any initial thoughts on sort of how you might think about the pricing there relative to IV KEYTRUDA and just how you might manage that?
Yeah. We would definitely pre-LOE of the IV, we would definitely price SubQ to make sure that patients can access it. So it doesn't need to be at a premium to the IV, for instance. I mean, we could, but we're definitely going to be sensible to make sure that patients have access. This really should benefit patients in a significant way. And as we think about biosimilars coming into the market, the same thing. We will need to be cognizant of biosimilar pricing. We can probably get, I would say, some premium versus biosimilar pembrolizumab. But again, we would be very much focused on making sure that patients have access to SubQ in that treatment setting.
Okay. As we were talking a minute ago, you talked about KEYTRUDA in early-stage renal cell. Renal cell is clearly a place where you guys have had a lot of success. You've been expanding upon that now with WELIREG. Had the positive data last year. WELIREG got off to a fantastic start to the year. In your view, kind of what drove that inflection? And maybe just talk about your enthusiasm for WELIREG as you see that playing out going forward.
Yeah. WELIREG has been probably an understated launch within our oncology portfolio when we first came in for a rare disease, VHL-related renal cell, as well as hemangioblastomas, CNS. But it really has played a significant role in that population where there really was no treatment. And we got to about $219 million of sales in 2023. We grew 77% in 2022, so it's been a strong uptake within that setting. And I think we can still do more within VHL-related disease. And then with the data coming through the registration on LITESPARK-005, we are now able to push into advanced renal cell carcinoma in the second, third-line plus setting following IO and TKI. And we're seeing a really strong uptake. That's a heavily treated population, but physicians are really happy with what they're seeing with WELIREG
Given sort of the safety profile of the asset, I guess, is this something ultimately you see more as sort of like a frontline metastatic drug or an adjuvant-setting drug? It seems like as an oral with pretty tolerable, that would be well-positioned in the adjuvant setting.
Well said. I think given the profile of WELIREG, it's a HIF-2α inhibitor. We see that as we move into the adjuvant setting in combination with KEYTRUDA, as we see it in the frontline setting, the first line as a triplet in combination with KEYTRUDA as well as LENVIMA. And in the second-line setting, we can combine it. I think it's in combination with lenvatinib in the second-line setting.
Yeah. LENVIMA as well.
Yeah. LENVIMA. Yeah.
Okay. Maybe if we can switch gears back to cardiovascular a bit. It was certainly something that dominated the conversation last year coming on the back of ACC and its sotatercept data, the updates on PCSK9. And you came up with new bold kind of targets on how you see the CV part of the portfolio progressing over the next foreseeable future. The PCSK9 part is a little bit more execution mode, but at this point, how you see an oral fitting into the broader opportunity given all the other dynamics we've seen in the space sort of fits and starts with the injectables. They seem to be on a better trajectory now. But just sort of your level of confidence in an oral in this type of segment.
Yeah. As a company, when we look at oral PCSK9 and we said it, I think last year at ACC, aspiration is really to democratize the most potent LDL cholesterol-lowering agent around the world, right? So the ability to take an injectable PCSK9 into a tablet, there's just endless opportunity to get this to every part of the world and make sure that patients benefit broadly. When you look at the United States, 85% of cardiovascular disease is still driven by atherosclerotic disease, right? So that's still high. We know that 70% of high-risk patients are not well-controlled per standard today, and only about 5% of the U.S. population have access to an injectable PCSK9.
When you bring all those things together, and there's going to be some hard work to bring that together and make sure that we get the right policies in place and treatment guidelines and standards, but I think that does spell that there's a huge need, and this product can make a meaningful difference in how we manage cardiovascular disease moving forward.
Okay. So outside the U.S., completely aligned. I think we get that. In the U.S., it's tough to think of a better example where sort of the challenges with IRA are going to be sort of put to the test in terms of how you think about a launch strategy here. So how important is having that CVOT data when you go to market here with an oral?
Yeah. I mean, I would say it's always better to have it rather than not. Are we going to hold back?
We'll push it ourselves. Yeah. You're going to hold back. Yeah.
I mean, if our Phase III plays out and it's administrable, we will bring this product forward to patients. We've seen increasingly cardiovascular outcomes better with the injectable PCSK9s. We believe that physicians will infer a class effect as well. But we will bring this forward to market in advance of our CVOT, and we will continue to develop our own CVOT data.
Okay. As we go back, and I'm sure I'm getting pinged in that I didn't ask a question on sotatercept sort of value, right? Clearly, again, with approval just sort of weeks away, I know you're not going to reveal pricing here, but at least when ICER did their pricing analysis, they threw out a $400,000 sort of assumption per year. Any sort of immediate reaction to that? Is that a fair assumption, totally off the wall?
Yeah. I mean, Merck, as we always do, we will price to the value of the medication, the value to the system, the value to the patients, right? Yeah. So hopefully, soon we can reveal that price, but we think that we are asking a fair price for what value sotatercept will bring to these patients.
Okay. Maybe a broader question, and I'd love to get Peter to chime in here. Just given all the chatter around IRA and sort of how that changes the calculus going forward, you've had some lawsuits with the government. And at this point, kind of what's the message in terms of expectation around pricing negotiations and how you, when you have to make your internal assumptions and anchor around the world going forward, how are you doing that in this sort of ever-changing world? I gave Peter the easy question. Yeah.
So we're in negotiations on Januvia, as you know, and when we have something more to say around how those negotiations are going, we'll communicate that. More broadly, on our lawsuit, the district court judge has heard both sides, and we're awaiting the district court judgment in that case. Big picture on IRA, it doesn't change our company strategy or approach. We will remain an innovation-driven company. And while we don't agree with the price negotiation component of the IRA, and we think it has adverse effects on the industry longer term, we think we can still, if we bring the right innovation to patients and to the market long term, we can still do well as a company.
Okay. Great. We'll have to wrap it up there, but two weeks with sotatercept PDUFA. Have a good luck. Thank you.
Thank you so much.
Thank you, Carter.