Gilead Sciences, Inc. (NASDAQ:GILD) Morgan Stanley 21st Annual Global Healthcare Conference 2023 September 12, 2023 11:30 AM ET
Company Participants
Dan O’Day - Chairman, Chief Executive Officer
Andy Dickinson - Chief Financial Officer
Conference Call Participants
Terrence Flynn - Morgan Stanley
Terrence Flynn
Great. Thanks so much for joining us, everybody. I'm really pleased to be here hosting Gilead. Before we get started, please see the Morgan Stanley Research Disclosure website at www.morganstanley.com/researchdisclosures. If you have any questions, please reach out to your Morgan Stanley sales representative.
I'm Terrence Flynn, the U.S. Biopharma Analyst here at Morgan Stanley, and we're very pleased to have Dan O’Day with us. Dan is Chairman and CEO, and Andy Dickinson, who is the company's CFO. But thank you both for taking time out of your day to join us today.
Dan O’Day
It’s a pleasure.
Question-and-Answer Session
Q - Terrence Flynn
I thought maybe we'd start off high level. Obviously diversification has been a key part of the Gilead story and part of your mandate Dan as you came in as CEO.
And so maybe give us an update and kind of the progress that you've made with the team in terms of diversifying the company away from HIV and also what's left to be done as you look out over the next several years here.
Dan O’Day
First of all Terrence, thanks for having us and for hosting the conference. I'm delighted to be here with Andy and a little tag team on this and thank you all for your interest in joining. I think we've made tremendous progress. If you asked me, if we would have been in this position when I took over four and a half years ago, I would have said I can't imagine we'd be this far along.
So we've just made, and I think on two fronts, one on the commercial front, which I think is punctuated by seven quarters of consecutive growth, really strong growth, excluding Veklury. Then secondly, the organization that Andy and I and the team have built around execution on the portfolio, and I think the metric on that is 21 Phase III trials. I'll get into that a little bit.
But on the commercial front, I mean it's largely in two different areas. One is Virology continues to perform really, really well. I mean just using the last quarters as an example, we had that 9% growth in our core HIV business, which was incredibly strong.
Biktarvy is now a $10 billion asset in our portfolio. And that's juxtaposed with the progress we made in oncology. At the end of the day, we're very confident about our ability to meet our target of more than a third of our revenue coming from our oncology business by 2030, and the reason for that is the following.
I mean, last year we had around $2 billion in business on our oncology business. Through the first half of this year, we're now on a $3 billion run rate. Our cell therapy business is growing at 27%. Trodelvy is growing at 63%. So we've got great confidence around the commercial execution in our programs. And that's supplemented on the transformation side by the depth of that portfolio. Those 21 Phase III trials are playing out across our therapeutic areas.
I mean for HIV, just to talk a little bit about it, we've got now more than nine potential combinations with long-acting treatments. Importantly, and I know we'll get back to this, but on the PrEP side with lenacapavir we have four trials, and those are going to be reading out. The two first trials will be reading out towards the end of next year, beginning of the following year with lenacapavir for PrEP, which we think will really transform the HIV PrEP market and eventually the treatment market.
We've got COVID trials underway with Obeldesivir. This year's marked a third indication for Trodelvy and Hormone Receptor Positive HER2 negative, and we're coming fresh off. In fact, I was just in Singapore at the World Lung Cancer Conference on the EVOKE-02 data where we saw some really promising data for Trodelvy in lung cancer, first-line lung cancer where we had the ongoing work in second-line lung cancer.
That combined with the fact that we more than doubled the portfolio with 64 programs across the entirety of the portfolio, but particularly in oncology, HIV, cell-therapy, which is growing really nicely and strongly from the portfolio perspective.
So I would say we are far from done. I think Andy and I would not be declaring that we're in any way in pause mode. We're going to continue to execute. And very importantly, we're going to continue to now – because we've gone through a really important build over the past several years. The organization is a very different organization than it was, and we've significantly increased our investment in R&D, for instance.
But we're now at a phase where we are – we are at a stage where we're investing, I think, appropriately overall in the range of where we want to be with R&D. So managing expenses, managing our ability to make sure we focus on the operating margin and also on our EPS is something that Andy and I are both very committed to on the course of this transformation journey over the next several years.
Terrence Flynn
Okay, great. I guess in terms of just on the BD front, maybe we'll just segue there to Andy. And it sounds like we should expect more kind of partnerships, more collaborations, more kind of normal course-type stuff as opposed to anything kind of mid-cap.
Andy Dickinson
Yes, I think that's exactly right. We've been consistent for the last couple of years. We did what we needed to do to diversify the business, to have the anchor asset in Trodelvy and oncology. Obviously, the cell therapy acquisition was incredibly important. And you're seeing this in the business performance that Dan highlighted. I mean, we have above-median growth in our base business, which I think the market tends to underappreciate today given where Gilead was historically.
So we have this incredible momentum in the base business. We have a very strong portfolio as Dan highlighted, much broader. We're going to continue to build it out. But what you see over the next couple of years is more likely to be what you saw in 2022, what you've seen this year so far.
A lot of important early-stage licensing deals, smaller acquisitions, I think our belief is that any healthy company will continue to look broadly at external assets and to bring in external assets. But our focus is really on late-stage, pre-clinical, early-stage clinical assets. That's the part of our portfolio today that we'd like to build out further. And again, that will drive robust growth above and beyond where we are today.
Dan O’Day
We don't talk about that much, but Andy and the team have built up a really interesting early inflammation portfolio too, both within our own research and externally. And that's kind of the third leg of the transformation journey that will come in the 2030s. But we think in generations, kind of in terms of how we're going to approach the portfolio and how we expand that out and so that will continue to be very interesting, coming across for all of the oncology and inflammation.
Andy Dickinson
Yes, absolutely. I mean, the other thing that's worth mentioning, when you look at oncology and you just step back in terms of – and we hear this consistently from the outside advisors and KOLs, broadly I think people believe that there are four big areas of growth and real potential to change patients' lives over the next decade or so.
One is cell therapy. The other area is antibody drug conjugates, in particular the TROP2, maybe the HER2 as well. TIGIT is another area, and then some of the targeted oncology therapies. We are clearly today a leader in three of those four, and we have some early-stage programs against targets like PRMT5 and KRAS G12D that we're excited about that should enter the clinic.
So from an internal perspective, I think our belief is we very purposely and systematically looked at, where is the oncology world going? Where's the immunology world going to Dan's point? And then we’ve slowly and kind of methodically build out a portfolio that we expect the street to gain much greater appreciation for over the coming years, similar to what you saw in the Trodelvy EVOKE-02 data. I think people are fully starting to appreciate now and will continue to appreciate over the coming weeks and months, so clearly good progress.
Terrence Flynn
Great. Well, maybe I had a couple of follow-ups on that. I guess first Dan, your comment on, you are committed to EPS growth here. So maybe just help us think about that margin opportunity here back. Have you talked about kind of the top line growth objectives, but how do you think about kind of the margin trajectory from here when you think about commitment to that EPS growth?
Dan O’Day
Yes, I'll start and then Andy can add a little color. I think, at the macro level, we had under-invested I think on the R&D side for a long time at Gilead. So we had a lot of catching up to do over the past several years, and we did that both through capital allocation and M&A that we've talked a little bit about, but also in building the nature of our business internally.
But now we're at a stage where we're roughly in the low 20% of R&D spend versus sales, and we think for a healthy company that's firmly focused on innovation, that's a good range to be in. And we're also at a stage where we can expect to see – again, we doubled the portfolio from probably 30 programs in the portfolio to 64, and it's not just about the numbers. I think also the quality, the nature of our portfolio, the risk-reward profile.
And I think we're now going to be at more of a steady state where we'll start to see these 21 Phase 3 trials that we're executing on now, which is pretty extraordinary when one thinks about what we've built up, particularly the new muscles in oncology, which are different than actually doing trials in virology, as all of you know.
But now we'll see trials naturally, as one would think in a more mature company relative to investment, trials rolling off and new trials starting. So you start to get much more of a steady state in the R&D. We've done the same thing in the commercial organization by building up in both cell-therapy and outside of cell-therapy, a strong commercial execution organization that will have leverage as we put new indications into that over the future.
So I think with those as kind of key drivers, and we're very focused. Andy, leading in this on the G&A side to make sure that we're constantly looking at optimizing and bringing, if you like, Gilead into the forefront. In many ways, we can leapfrog because of the investments. Perhaps the other investment we had in the past on systems, but leapfrogging in terms of efficiency and being effective around G&A.
So, I mean I'll let Andy comment on – obviously we're not guiding trades to particular EPS and sales lines, but... [Multiple Speakers]
Andy Dickinson
We have, I mean maybe to step back. We moved from this growth where Dan highlighted that we underinvested significantly, I think in R&D historically you've known the company for a long time. We made up for a lot of that. We've almost doubled our spending overall. We needed to.
Even with that, we have incredibly strong operating margins today. So we still have one of the – a top operating margin in the industry. And as Dan said, we're kind of moving from that growth and execution phase to what I would call an execution and optimization phase, and there's a lot of room to optimize the business over the coming years. And you're going to see the switch from expenses, even though I mentioned earlier that the base business growth was incredibly strong over the last couple of years. It has been, and we don't expect that to change. You know, the expense growth will moderate, and that will cross over in the foreseeable future.
So to Dan's point, we don't provide long-term guidance on this, but in the foreseeable future, you're going to see that expense growth cross over. It will be less than what we expect to be our base business revenue growth and then you'll see the leverage in the model.
We are still a very small company relative to many of our peers. We have less than 20,000 employees globally. We are agile, and there's a lot of room in the model. So when you drive the top-line growth that we've seen and that we expect to kind of increase over time and the expense discipline, you're going to see a lot of that fall to the bottom line. Not that different than Gilead historically, it's just again, it was a very different business model.
So we're getting to that point where we expect a crossover, and we have a lot of it. Back to your portfolio comment, we have an incredible strong portfolio, not only in oncology but also in virology, with areas like PrEP that should drive that outsized growth, all of which should fall to the bottom line here in the foreseeable future.
Terrence Flynn
Okay. Great. The other kind of related question based on some of your comments Dan was, obviously we're going to enter a post-IRA world. Back half of the decade, that does have implications for cancer drugs. I think most specifically small-molecule cancer drugs. So if you think about investing in innovation and this diversification to cancer, how does this new IRA world impact some of those decisions you are making in prioritizing spend?
You mentioned inflammation as another area where probably it would be less of an impact. So maybe just speak through like what is Gilead as a company doing to navigate the post-IRA world?
Dan O’Day
Yes. I think there's a lot yet to be understood about the post-IRA world. So I think the two things that we do understand well in IRA are the inflation rebates and the Part D reform, both of which I think are clearly manageable within our portfolio. And I believe they eventually help – I mean, they do help patients out of [inaudible] costs. So we’re really a component of things like the Part D reform. It's really the negotiation piece, which is obviously the piece that I think is damaging for the entire industry.
When I put that towards the Gilead portfolio and make it specific for us, I think we're in a slightly different position than other companies. First of all, we don't have really any major patent expertise at all on our prices. It's a relatively useful portfolio when one looks at both the HIV side and clearly the oncology side, because we just got into this four and a half years ago.
So presently, I'm one that wants to make sure we wait and see a little bit about how this is going to play out in terms of the longer-term portfolio. We haven't made major shifts to our portfolio for the reasons I just mentioned, the usefulness of it and where we're going. I also believe that some common sense will come back into some of the IRA at some point in time.
And we have to continue to do what's right for patients. So we want to leverage our small molecule business. We want to continue to leverage all the innovation we have in all the modalities, cell therapy and also biologics and we'll see where we go.
But on the negotiation side, we don't expect any impact on our business for the next several years. We'll have to see how that impacts and would impact probably a small portion of our portfolio in that period of time. And you combine that with the growth drivers that Andy was talking about. Let's just take the HIV business. We are confident that we'll be able to drive a positive CAGR, well through the end of this decade and beyond with the introduction of, first of all, Biktarvy continuing to make progress as the standard of care and treatment.
Descovy continuing to do well in prevention. And then lenacapavir in all of its forms, opening up the prevention market, which today in the United States and probably still undercounted is only around 20% penetrated. And the ability for a long acting we think - can more than - at least more than double that market by the end of the decade.
So we've got growth drivers that underlie this uncertainty if you like, around the IRA. And then you put on top of that the oncology portfolio, really because it's so useful, it will not be affected by the IRA.
Don't get me wrong. I'll continue with my multiple hats to work with policy makers, to take away as much as possible what I think are the perverse incentives in the IRA that are not good for patients and diseases. But I'm just speaking merely about how it impacts Gilead.
Terrence Flynn
Okay, understood. Maybe going back to oncology, you mentioned you were in Singapore for World Lung. So maybe just give us the highlights of the EVOKE-02 data and what that means for kind of next steps and how the paradigm could evolve here in the first nine months.
Dan O’Day
Yes, it's really exciting. Andy started to tee it up in terms of what I also saw at World Lung, which is this concept in particular in lung cancer of having the era of TROP2 ADCs and TIGIT kind of coming together.
Now, the real highlight at World Lung was specifically related to TROP2 ADCs. And for us, I think, remember now we've got three indications with Trodelvy, more than 20,000 patient experience with Trodelvy. And we're now taking that up in lines of therapy in breast cancer and in some new therapies like lung cancer.
Look, I think the EVOKE-02 data was tremendous. It was really even beyond our expectations in terms of what we might see in early stage data. And I think it speaks really well for the future of patients with lung cancer, what we might be able to do to help them.
Specifically, what EVOKE-02 does is, in our mind it de-risks the ongoing EVOKE-03 trial, which is now recruiting patients for PD-L1 high, because of this 69% -- well, three major aspects of the EVOKE-02 data; One is the response rate, second is the durability, and third is the tolerability profile.
But as we looked, and the thought leaders that I met with at Singapore looked at the data, they saw that 69% overall response rate in the PD-L1 high compared to and the appropriate comparison here is really to look at protrude on monotherapy, because that is the standard of care which has a response rate of somewhere around 39% to 45%. So that's one piece of the puzzle.
But we know that OS is what counts in lung cancer. So then you have to combine the durability where we're seeing patients go, 88% of patients are still on therapy after six months, whereas we know even in those patients, and it's less than the majority of patients that are treated with a chemo combo in that frontline setting, really four cycles is really the maximum that people can tolerate platinum.
So if you combine the response rate with the longer durability, that's what gives us confidence in those curves being able to continue to separate and potentially, we think, have a great confidence around showing the OS and PFS data that's to come in EVOKE-03.
And then of course in the PD-L1 lower population, that same durability is occurring as well. Combine that with a tolerability profile that has been manageable in breast cancer and bladder cancer, manageable toxicity effects like temporal diarrhea associated with the beginning of injections and neutropenia that physicians know how to handle.
I think in comparison to other TROP2 ADCs where there are other side effects like ILD and stomatitis, we feel like we're in a really good position with the TROP2 ADC as we go into both, first and second line lung cancer. Combine that with the TIGIT data that we exposed on Rx7 and the opportunity to potentially look at – seeing those curves continues to separate and we have ongoing trials there.
I think it gives us optionality in our frontline setting depending on how the data reads out from both an efficacy standpoint and a tolerability standpoint. So we're -- I was very encouraged by what I heard at World Lung from the thought leaders there on this data.
Terrence Flynn
And I guess big picture, does this – I mean, my view is that this could become a more fragmented market. Again, you hear and you think about biomarkers, etc. You already have PD-L1. Again there's some talk from the Merck side, more so looking at TROP2 expression. So do you think that's the likely path we're going down or do you think it's going to be kind of the best regimen, winner-take-all market in first line lung like we have now with KEYTRUDA?
Dan O’Day
Well, I think it will remain to be seen. I mean, it was interesting, every presentation that I saw at World Lung, we are – the community, is looking for biomarkers. So far there's been no compelling evidence to suggest, particularly with TROP2, which is more than 80% expressed in most tumor types by the way, not just lung cancer. That doesn't bode well necessarily, at least in our hands with the data that we've seen so far, to have a patient subset.
Particularly I think, and one has to look not only at the class, but also at your particular molecule, because our molecule is different than other TROP2 ADCs. It has a linker that's been purposely designed to kind of allow the target to effuse in the tumor microenvironment as well, which may mean that you need even less TROP2 expression to get a beta. So I think it would be great.
I mean, I come from a history of 30 years of looking for personalized medicine and I'm a big believer in that. And I think what we're seeing so far in our TROP2 and TRODELVY in our hands is an all-timer medicine, because of the way that's expressed. So we'll continue to look, not for lack of wanting, but I think largely in the first-line setting and the second-line setting in Lung, we think at this stage it's likely an all-timer strategy.
Terrence Flynn
Okay, great. Maybe one other related question in lung. We are talking about TIGIT. Your former colleagues, they had some data that leaked out relating to TIGIT. What are the implications of that data for your TIGIT program and what does it mean in terms of how you think about your Phase III program there?
A - Dan O’Day
Yes, I'll start and I want Andy to add into this. But I'll just say again, back to my experience at World Lung, I think the interesting thing about the recent data from Roche, perhaps unintentionally available to everybody is that the curves continue to separate.
There'll be a lot of debate around the statistical analysis and how or what alpha was spent on the interim versus the end, but I think what everybody is encouraged by is the continued separation of curves. And that – and I speak more specifically to our ARC-7 data that’s in our own hands, where we see a curve that has the potential to also differentiate and discriminate. So, I'll get Andy involved here. [Multiple Speakers] He’s a bit of the expert here.
Andy Dickinson
Yes, I like nothing better than to speak to the science. [Multiple Speakers]. We believe, based just on our ARC-7 data, that we've demonstrated that TIGIT is active and additive to PD-1 therapy. The Roche data just further validates that from our perspective.
The question that has to be answered, that we think is fair, is the magnitude of the benefit. But you see a very clear benefit in our data; you see a clear benefit in their data, regardless of whether they hit statistical significance. That has more to do with the sizing and powering of their trial, how they use their statistical alpha.
So we're moving full speed ahead with Arcus. We have a tremendous amount of confidence. We've highlighted many times our TIGIT. Dan mentioned this earlier. It's a little bit different, especially in terms of the FC engineering. We have an FC null TIGIT that we think helps, certainly in the side effect profile with injection site reactions. It also should – there's the potential for the FC-competent TIGITs to deplete Tregs in the periphery, which we think can be problematic from the side effect profile.
So we really like the program. We're very enthusiastic. And maybe when you fast forward, again to your question in World Lung, there's a possibility where you have PD-1 plus TIGIT, PD-1 plus TRODELVY. There's also a possibility five years from now that the standard of care, at least in certain parts of the first line non-small cell lung cancer is a tripling of TRODELVY plus our TIGIT plus PD-1.
So we're pretty excited. And again, it's early days. There'll be a lot of data that we and others are able to develop over the coming years. But again, our overall belief is that TIGIT is additive to PD-1, and this just further reinforces that.
Terrence Flynn
Okay, great.
A - Dan O’Day
And you know, having a sort of involved camps as this data develops, I think really gives us. We're the only company with – who built two molecules at an advanced stage, where I think we can be able to learn from data. Not only our data, but competitive data, and pivot our programs appropriately. So it gives us a lot of flexibility for sure.
Terrence Flynn
The one we get on the commercial side is, as we think about Roche as a TIGIT, Merck, you guys. Merck is working on a co-formulation. You guys know this well from HIV. Does that represent a disadvantage in any way from a commercial perspective as you think about the future of the market if there is, let's say a biosimilar PD-1, but Merck has a co-formulation of a TIGIT and a PD-1? So how does that tie into what we were just talking about, where you guys have lots of different pieces as well?
A - Andy Dickinson
Yes, we don't see it as a disadvantage. I mean we follow closely what Merck and others are doing in this space. I think the world that we see down the road is that the PD-1 should be fungible at the end of the day. Obviously we're doing studies, the Arcus studies are with zimberelimab. We're doing a lot of studies with pembro. Some of the – one of the studies with Arcus has a pembro reference arm.
But our vision of the future is that the PD-1’s likely become fungible, and then you're really thinking about it kind of from a pricing perspective and a commercial perspective. But we don't believe that we're at a disadvantage by not co-formulating. In fact, it's probably the opposite in our mind, that by having the best TIGIT that can pair with any PD-1, we think we're going to be in a very strong position down the road.
Dan O’Day
Yes, and maybe Andy already mentioned this, but one of the things about triplets, I think having the flexibility to adjust dose and schedule for different molecules, we think is a potential advantage.
Terrence Flynn
Great. Maybe moving on to the cell therapy franchise, obviously another important growth driver as you talked about Dan. As we look ahead here, maybe just give us an update on kind of key drivers. I'm sure second line is one of those. And again, anything else as we think about the forward opportunity set here for second line and Yescarta in general?
A - Dan O’Day
Yes look, I think it’s good that we’re – Andy and I could say we're in the first or second inning of cell therapy and hematology alone, let alone the other potential indications. But we're very excited about where we stand right now. We're able to fulfill on the manufacturing side more than 95% of the patient need and patient – per patient. So I think we've got lots of capacity and lots of ability to follow this.
We're at the beginning. So in the third line setting where arguably every patient should be offered that, only about 30 patients are offered it today and get to the stage to benefit from. Now after five years, 50% of patients are essentially in a relatively curative state. And we're just beginning, probably 10% penetrated in the second line setting.
So, like any new technology and new therapy, you go back to transplant. Years ago – it does take some years to change the behaviors of physicians that are used to a particular modality. But the way we're increasing the authorized treatment centers in this country and around the world, working with community oncologists to get them to refer and really working the model out here in the United States so that the referrals can potentially be within these large community oncology networks, is really important.
Obviously, moving up in lines of therapy, expanding geographically in hematology. And then I think, we're just beginning to kind of tap into the potential with our deal with our CELIX [ph]. We'll be looking forward to getting into the BCMA and multiple myeloma area in the next several years. And then beyond that we think, more broadly in terms of the role of TB19-mediated inflammatory diseases.
I think as a major player in cell therapy, we think there's a lot of opportunity, but there's also a responsibility to make sure that as these technologies advance, that we bring them onto, if you like, the platform, and that's the concept.
So it's not that we're going to do everything ourselves. We have a tremendous ecosystem of talented companies out there and biotechs that are working on different targets. They come to us. They want to talk to us about how can they get their assistance on our platforms. And I think that's a really good position to be in, is that we can continue to evolve the science and all the potential benefits of cell therapy.
Terrence Flynn
Is there enough capacity out there right now at centers, or what is Gilead doing to try to help bolster capacity? Or is this more of a move to kind of like out-patient what's ultimately [inaudible].
A - Dan O’Day
I think both will be the case. I mean, and you can feel it in here, but we're rapidly expanding our authorized treatment centers. You know, we were at the end of last year around high 200, and now we're in the 350, so we're expanding that. And more importantly, just the number of authorized treatment centers, it's making sure they are in the right places that can allow those community referrals to occur.
But beyond that, of course we're looking into expanding outpatient as people get more comfortable with this. And we want to make sure that in certain therapeutic areas where allogeneic will come to fruition, that we're in a position to do that.
But the reality is with autologous. We're now down to a stage where we've really significantly reduced the vein-to-vein time in a very reliable way. As I said before, more than 95% of patients are fulfilled. So I think – and the benefit of course of having autologous, as that's been demonstrated over the years too. Andy, do you want to...
A - Andy Dickinson
Yes, I'd just say financially again, just a step back. When we acquired Kite, whatever it was, six years ago, our vision, and it still is today, that cell therapy is going to be a major treatment modality that will develop over 20 or 30 years. It's always going to be slow and steady. So fast forward to where we are today, six years later, we have roughly, give or take, $2 billion in sales this year.
We've become more efficient in terms of manufacturing. We've brought our cost of goods down substantially over the last five or six years. We're more efficient in manufacturing. We can manufacture quicker, that's still changing. But this is just the very beginning, so a $2 billion business.
And Dan highlighted earlier, in the core markets when you're showing in DLBCL, take third line plus, 46% of the patients appear to be cured, still five years out or six years out. And there's still a massive number of patients. I think 15% of the patients over second and third line plus are getting cell therapy today.
Fast forward years from now, just in DLBCL and multiple myeloma, you can see the scale of the business that you can grow. It's like, in my mind cell gene like right. And then you add on top of that immunology in terms of what that can do with some of the incredible data.
So it's very early days, but we're really proud of where we are. We have a great team. We have a great set of products and a great pipeline, and it's just the beginning. I think again, we believe, like our broader oncology business, the world will come to appreciate the growth and the long-term potential of the business more and more over the coming years. It's really exciting to see where it's come so far.
Q - Terrence Flynn
So is that cell gene, I think it was doing $15 billion in myeloma revenue. So is that guidance?
A - Andy Dickinson
[Multiple Speakers] I'm very focused on cell therapy. So we've said this. I mean, the cell therapy market overall is much, much larger than I think people appreciate. Even today in fact, the cell therapy market from a dollar standpoint is bigger than people appreciate, because unlike Kite, where you have a 96% success rate, many of the competitors have a much lower success rate in manufacturing, yet the products are used. They just don't get reimbursed for them.
So I'm not going to provide long-term guidance, but rest assured, we see this as the very beginning. And for any large company operating across cell therapy, being substantially larger in terms of revenue than where we are today is reasonable from our perspective and frankly, expected, so more to come.
Terrence Flynn
Great. Well, thank you so much, both of you. I appreciate your time.
Dan O’Day
Thank you, Terrence. I appreciate it.
Andy Dickinson
Thank you. I appreciate it.