Jazz Pharmaceuticals plc (NASDAQ:JAZZ) Q1 2024 Earnings Call Transcript

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Jazz Pharmaceuticals plc (NASDAQ:JAZZ) Q1 2024 Earnings Call Transcript May 1, 2024

Jazz Pharmaceuticals plc isn’t one of the 30 most popular stocks among hedge funds at the end of the third quarter (see the details here).

Operator: Thank you for standing by. My name is Krista, and I will be your conference operator today. At this time, I would like to welcome everyone to the Jazz Pharmaceuticals First Quarter 2024 Earnings Conference Call. All lines have been placed on mute to prevent any background. After the speakers’ remarks there will be a question-and-answer session. [Operator Instructions] Thank you. I would now like to turn the conference over to Andrea Flynn, Vice President, Head of Investor Relations. Andrea, you may begin your conference.

Andrea Flynn: Thank you, operator, and good afternoon, everyone Today, Jazz Pharmaceuticals reported its first quarter 2024 financial results. The slide presentation accompanying this webcast is available on the Investors section of our website. Investors may also refer to the press release we issued earlier today, which is also posted to our website. On the call today are Bruce Cozadd, Chairman and Chief Executive Officer; Renée Galá, President and Chief Operating Officer; Rob Iannone, Executive Vice President and Global Head of R&D; and Phil Johnson, Executive Vice President and Chief Financial Officer. On Slide 2, I’d like to remind you that today’s webcast includes forward-looking statements, such as those related to our future financial and operating results, growth potential and anticipated development and commercialization milestones and goals, which involve risks and uncertainties that could cause actual events, performance and results to differ materially from those contained in these forward-looking statements.

We encourage you to review the statements contained in today’s press release, in our slide deck and the risks and uncertainties described in our SEC filings, which identify certain factors that may cause the company’s actual events, performance and results to differ materially from those contained in the forward-looking statements made on today’s webcast. We undertake no duty or obligation to update our forward-looking statements. As noted on Slide 3, we will discuss non-GAAP financial measures on this webcast. Descriptions of these non-GAAP financial measures and reconciliations of GAAP to non-GAAP financial measures are included in today’s press release and the slide presentation available on the Investors section of our website. I’ll now turn the call over to Bruce.

Bruce Cozadd: Thanks, Andrea. Good afternoon, everyone, and thank you for joining us today to review our first quarter results. I want to begin by welcoming Phil Johnson, who joined Jazz in March as our Chief Financial Officer. We’re very excited to have Phil on our executive team and look forward to his contributions to delivering value for patients and shareholders. Beginning on Slide 5, we made important progress during the first quarter, including year-over-year combined double-digit revenue growth from our key growth drivers, Xywav, Epidiolex and Rylaze along with meaningful advances in our pipeline. I’m also pleased to report that we are affirming our 2024 financial guidance. On the commercial front, we generated more than $900 million in total revenues across our growing and diversified portfolio of medicines.

Xywav revenues increased 14% year-over-year reinforcing our confidence in its trajectory and durability. Epidiolex demand remains strong, and we continue to be confident in its blockbuster potential. Our oncology therapeutic area delivered another strong quarter with 13% year-over-year revenue growth. This continues the momentum we established last year when we surpassed $1 billion in annual oncology revenue for the first time. Moving to our R&D and pipeline efforts. 2024 is an important year for Jazz with multiple late-stage catalysts for therapies targeting substantial market opportunities. We achieved a significant milestone for zanidatamab in March with the completion of our rolling BLA submission for the treatment of HER2-positive biliary tract cancer, or BTC, and we expect commercial launch in 2025 or earlier.

If approved, zanidatamab would be the first HER2-targeted treatment, specifically for BTC in the U.S. We also expect important clinical data readouts in the near future for suvecaltamide in essential tremor, zanidatamab in gastroesophageal cancer, Epidiolex in Japan, and Zepzelca in first-line small cell lung cancer. On the operational front, we are maintaining our focus on disciplined capital allocation. Our financial strength, including healthy operating cash flow, enables us to invest in the continued growth of our commercial portfolio and pipeline while also positioning us to execute on corporate development opportunities. Turning to Slide 6. We remain focused on advancing the three core tenets of Vision 2025. This includes advancing leading therapies in sleep disorders and epilepsy along with a growing oncology portfolio, investing in R&D to expand our capabilities and pipeline and making disciplined capital allocation decisions to enhance value to shareholders as we realize our ambition to be a high-growth global biopharma leader.

I’ll now turn the call over to Renée to review our commercial performance, after which Rob will share an update on our R&D progress. Phil will provide a financial overview, and then we’ll open the call to Q&A. Renée?

Renée Galá: Thanks, Bruce. I’m excited to report on the continued progress across our commercial portfolio. We delivered strong first quarter revenue growing combined revenue from our key growth drivers, Xywav, Epidiolex and Rylaze by 12% compared to the same period in 2023. As is typical of the first quarter of the year, revenue was impacted by seasonal headwinds from payor reauthorizations and inventory drawdown. Let’s get into the details starting on Slide 8 with our sleep franchise. Total revenue from sleep, which includes Xywav and Xyrem net sales plus royalties from high sodium oxybate authorized generics, or AGs, as was $430 million in the first quarter of 2024, and we remain confident in the growth and durability of Xywav.

In the first quarter of 2024, Xywav revenue grew 14% year-over-year to $315 million. I’ll take a few minutes to discuss our view of the overall oxybate market as well as several items of note from the quarter. In 2023, we saw the first competitive entrance to the oxybate market with the commercial availability of both high sodium AG and branded fixed dose high sodium oxybate. We were pleased to deliver Xywav revenue growth through this period and continue to expect Xywav to remain the oxybate of choice, including the number one treatment for narcolepsy. As expected, at the start of 2024, Xyrem was excluded from certain commercial formularies based on the availability of multiple newer oxybate products, including Xywav. Many of these patients and their physicians recognize the benefits of low sodium and chose to initiate treatment with Xywav.

I want to call out several downstream dynamics of this transition. First, we saw a significant increase in the number of active narcolepsy patients benefiting from Xywav at the end of the first quarter of 2024 compared to the fourth quarter of 2023. Second, we saw an increase in utilization of our patient support programs in the first quarter as patients navigated the transition from Xyrem to Xywav with their insurance providers. These programs provide free product for a limited duration, helping to ensure patients have uninterrupted access to therapy as they obtain Xywav coverage. As a reminder, we have achieved benefit coverage in both narcolepsy and IH indications for approximately 90% of commercial lives. While we anticipate that other plans may exclude Xyrem from formulary going forward, we expect these changes will be less concentrated and spread out over time.

We view the large number of patient transitions that occurred from the fourth quarter of 2023 to the first quarter of 2024 as a one-time event. Finally, this transition resulted in a significant decrease in Xyrem branded revenues. I will note that all of these dynamics were accounted for in our 2024 neuroscience revenue guidance. Looking at our quarterly patient metrics, there were approximately 9,900 narcolepsy patients taking Xywav exiting the first quarter, an increase of 375 patients from the prior quarter. Given the increased use of patient support programs, revenues for the quarter do not fully reflect these patient additions. We believe patient numbers are the best indicator of the long-term value and durability of this product and expect that revenues will be more aligned with patient numbers going forward as newly transitioned patients revert to being fully covered by their insurance providers.

Turning to IH, the transition dynamics associated with coverage for narcolepsy patients did not impact the IH market. We continue to view IH as the strongest growth opportunity for, Xywav and exiting the quarter there were approximately 3050 active IH patients on Xywav, an increase of 275 from the prior quarter. We are prioritizing investments to further build the market and our expanded field force is now fully deployed. These additional field personnel are focused on increasing the depth and breadth of IH prescribers. Outside of the branded oxybate business we recognized approximately $50 million in AG royalty revenue, which was driven by both patient transitions and our increased royalty rate. Given our results for the quarter and increased visibility into oxybate market dynamics since the entry of high sodium oxybates, we remain confident in the durability of Xywav and believe that we are well positioned to achieve our vision 2025 goal of $2 billion in sleep revenue.

Moving to Slide 9, we are pleased with the continued growth of Epidiolex, with net product sales of approximately $200 million in the first quarter, representing a 5% increase compared to the same quarter in 2023. As a reminder, with Epidiolex, we typically see a build in inventory throughout the second half of the year, which then burns off in the first half of the following year, primarily in the first quarter. We expect future growth to be driven by underlying demand and geographic expansion, and remain confident in the blockbuster potential of Epidiolex. Key drivers of increased demand in the U.S. included the positive response to data on the benefits of Epidiolex beyond seizure control, such as language and communication, cognition, executive function, and emotional, and social function, as well as synergies from treatment with Epidiolex plus clobazam.

We are also continuing to see increased penetration in the adult patient setting, which is supported in part by data showing that many patients may reach adulthood without a specific LGS diagnosis and by providing HCPs with clear diagnostic tools for adult patients. Further opportunities for growth include continued education to support optimal dosing, focused data generation and geographic expansion beyond the more than 35 countries where Epidiolex is currently approved, with additional launches and market reimbursement expected in 2024. Shifting to our oncology business on Slide 10, total oncology revenue for the quarter was approximately $258 million, led by Rylaze and Zepzelca. Rylaze delivered another strong quarter with net product sales of $103 million, representing a 20% increase from the first quarter of 2023.

Strong demand for Rylaze continues to be driven by several factors, including its near universal adoption in pediatric asparaginase-based oncology protocols in the U.S. and adoption of the Monday, Wednesday, Friday dosing regimen. We are also seeing usage of Rylaze in the first line setting based on the benefits of its short acting profile relative to current first-line asparaginase therapies. In addition, we remain focused on continued growth of Rylaze in the treatment of adolescents and young adults or the AYA market. Turning to Slide 11 and Zepzelca, net product sales for the first quarter increased 12% year-over-year to $75 million. We have established Zepzelca as the number one treatment for second-line small cell lung cancer patients, and we continue to hear positive feedback from healthcare providers on its clinical benefit as well as ease of use at administration for patients and their healthcare practices.

In addition to the second-line setting, there remains an unmet need for small cell lung cancer patients in earlier lines of therapy. We believe positive data from the ongoing Phase 3 trial in first line small cell lung cancer is the biggest opportunity to drive significant growth and most importantly, would provide a further opportunity to improve patient lives and outcomes. We expect data from that trial in late 2024 or early 2025. With that, I will turn it over to Rob for an update on our pipeline and upcoming milestones. Rob?

Rob Iannone: Thank you, Renée. 2024 represents an exciting time for our pipeline. And we anticipate multiple, meaningful catalysts across oncology and neuroscience. On Slide 13, we provided an overview of the key clinical programs in our diversified pipeline. And I will highlight several milestones we expect to reach in the near term. Starting with oncology and zanidatamab, we have completed our BLA submission for second-line biliary tract cancer or BTC, in the U.S., with potential for accelerated approval. Additionally, we are targeting late this year to report top line data from the ongoing Phase 3 first-line gastroesophageal adenocarcinoma, or GEA trial. If positive, we expect this trial would support registration. I will speak more to our zanidatamab development plan in just a moment.

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We are also pleased with the progress of the Zepzelca first-line trial, which completed enrollment in January. Top-line progression-free survival data for Zepzelca in combination with Tecentriq in first-line, extensive-stage, small cell lung cancer is expected at the end of 2024 or early 2025. If approved, this new indication would enable more patients with small cell lung cancer to potentially benefit from longer duration of therapy with Zepzelca. Turning to neuroscience. We expect top line data from our Phase 3 trial of Epidiolex in Japan in the second half of 2024. We also have ongoing trials for suvecaltamide or JZP385 in both essential tremor or ET and Parkinson’s disease tremor. With top line data from the ET trial expected late in the first half of 2024.

If trial findings are positive, we believe this trial could serve as part of the pivotal regulatory package. I’d also like to provide an update on JZP441, our clinical stage orexin-2 receptor agonist. We paused the JZP441 Phase 1 trial last November after observing a signal for QTC interval prolongation on automated ECG recordings. Since that time, we engaged external experts to perform manual reads of ECGs. That work was recently completed with the initial report indicating there may be a therapeutic index to exposures predicted to be efficacious in narcolepsy type 1 patients. We are reviewing this information with our alliance partner, Sumitomo Pharma and Jazz will then make a decision on next steps, if any. I expect to be in a position to provide an update on our 2Q earnings call.

Returning to zanidatamab, Slide 14 provides more detail on our development plan. We have meaningfully progressed zanidatamab development across multiple indications since bringing it to Jazz. And based on emerging strong data across indications, we remain excited about the potential of zanidatamab to transform the current standard of care in multiple HER2-expressing cancers. As was noted earlier, we completed our BLA submission for second-line BTC at the end of March and anticipate a response from FDA within the usual 60-day window. Upon acceptance, FDA would also establish the priority of review and PDUFA timeline. I’ll also note, we are planning to present more mature data from the ongoing BTC trial at ASCO this year, including overall survive.

Our development plan represents a robust investigation of this molecule in multiple tumor types including an ongoing trial in GEA that we believe would support registration in that indication in several trials in breast cancer. We’ve recently announced plans to initiate the Phase 3 POWER trial in the second half of this year, which will evaluate zanidatamab in combination with chemotherapy after progression on HER2, where we have the opportunity to be the first HER2-targeted therapy to demonstrate efficacy and safety in breast cancer patients post-HER2. In summary, we’re executing a regulatory strategy that we believe will enable us to bring zanidatamab to the market in the near-term with an initial indication in second-line BTC and the opportunity to rapidly advance other indications.

In total, we believe our development program can deliver for patients in need and generate a significant commercial opportunity of more than $2 billion. I would encourage listeners to go to our IR website and access the R&D Day webcast we hosted on zanidatamab in March, which included a detailed overview of data demonstrating zanidatamab’s differentiation from other HER2-targeted agents, how it would fit in the HER2 treatment landscape and perspectives from external thought leaders on the potential of zanidatamab to improve the quality of care for patients with HER2-expressing tumors. Turning to Slide 15. With the top line data readout from the essential tremor trial anticipated in the second quarter of this year, I’d like to highlight suvecaltamide, which is a highly selective and state-dependent modulator of T-type calcium channels in clinical development for the treatment of ET and Parkinson’s disease tremor.

There is a high unmet need for ET treatment with no new medicines approved in more than 50 years. ET can be highly debilitating with significant negative effects on a patient’s quality of life and activities of daily living, such as eating, drinking, dressing, shaving and writing and can lead to substantial impairment in physical functioning. Some patients also experienced cognitive deficits anxiety, social phobia, depression and sleep disturbance. In the U.S. and key European markets, there are approximately 2 million diagnosed patients with the prevalence estimated at approximately 11 million patients. Moving to Slide 16. I want to touch on suvecaltamide’s differentiated mechanism of action. While the exact underlying pathophysiology of ET is not clear, there is strong evidence to support the role of T-type calcium channels.

T-type calcium channels regulate the balance of calcium ions, acting as a gatekeeper to help ions both enter and leave the cell membrane. In some pathological states such as ET, increased activation of these channels leads to excessive rhythmic signals that prompt tremor. The high selectivity of suvecaltamide for T-type calcium channels makes it a promising candidate for the treatment of ET, which was demonstrated in the Phase 2 TCOM trial. Importantly, suvecaltamide is differentiated from other T-type calcium channel blockers in development as it is state dependent, meaning that it targets channels under conditions of hyperexcitability, while sparing the form of the channel, important for normal neuronal signaling. Now I will turn the call over to Phil for a financial update.

Phil?

Phil Johnson: Thanks, Rob. First, I’d like to express how excited I am to join Jazz. I came to the company because of its history of success, innovating to transform the lives of patients and their families. And because of the quality, integrity and enthusiasm of its people, which Jazz has accomplished since its founding is impressive, and we have great opportunities ahead of us to enhance our impact on the lives of the patients we serve and to create significant shareholder value. Turning now to our first quarter 2024 financial performance, Slide 18 summarizes the highlights. As a reminder, more information on our financial results is available in our press release and 10-Q. We saw continued top line growth in the first quarter of 2024 with $902 million in total revenues, representing a 1% increase over the same period in 2023.

As Renée noted, our first quarter revenues have historically been affected by several factors, including reauthorizations, which drive the use of patient support programs and inventory build in the latter part of the prior year, which leads to inventory burn in Q1. Our Q1 results are in line with our expectations and we are affirming our full year revenue guidance of $4.0 billion to $4.2 billion, including our expectation for combined double-digit growth from our key growth drivers, Xywav, Epidiolex and Rylaze and double-digit growth in our oncology therapeutic area. Moving to Slide 19, non-GAAP adjusted SG&A reflected investments dedicated to our key growth drivers, including the Xywav IH commercial initiatives, commercial support for Epidiolex in the U.S. where the market is promotionally sensitive, geographic expansion of Epidiolex outside the U.S. and educational efforts for Rylaze and AYA.

Non-GAAP adjusted R&D expense for the quarter was driven by investment in multiple late-stage programs, which we view as critical to enhancing the future value of our pipeline. We are executing on a robust development plan for zanidatamab with trials across multiple tumor types as well as Phase 2 trials for suvecaltamide in two different disease areas and programs for Epidiolex and Zepzelca that have the potential to expand those products into new geographies and patient populations, respectively. On note that our operating margin and expenses are not linear and we incur spend at the time to best support strategic initiatives for our commercial business and pipeline. Investments in our commercial business to support our key growth drivers ramped up in the fourth quarter of 2023 and extended into the first quarter of 2024.

We expect these investments to positively impact revenue as the year progresses. SG&A expenses in 1Q 2024 also included a bad debt expense and higher litigation costs, primarily related to the Avadel Patent infringement trial. Our R&D expenses, along with clinical trial activity ramped up in 2023, and we expect these expenses to remain at relatively consistent levels throughout 2024. Therefore, we are affirming our full year 2024 SG&A and R&D guidance. I’d also point out that we recorded a discrete tax expense related to expired stock options. While this significantly increased our non-GAAP effective tax rate for the quarter, we expect our full year 2024 non-GAAP effective tax rate to remain in the range of 10% to 13%. We continue to generate significant cash from our business, driven by the strength and diversity of our portfolio.

We recorded approximately $267.2 million of cash from operations in the first quarter and ended the quarter with $1.8 billion in cash on hand. Our strong financial position and operating cash flow provide flexibility to invest in priority commercial and R&D programs as well as corporate development opportunities. Non-GAAP adjusted net income of $182 million and non-GAAP adjusted EPS of $2.68 were driven by our top line growth, along with significant investment in our key growth drivers and pipeline including multiple late-stage clinical programs, zanidatamab, Epidiolex, suvecaltamide and Zepzelca, all of which have the potential to generate significant long-term value. Based on our results from the quarter and continued focus on disciplined and strategic capital allocation, we are affirming our non-GAAP adjusted net income guidance of $1.275 billion to $1.35 billion.

Since joining Jazz, I’ve spent considerable time speaking with investors and analysts and greatly appreciate the perspective and input they shared. In these conversations, I heard a concern that Jazz will overpay for an acquisition to meet our goal of corporate development, contributing $500 million to 2025 revenue. Here’s how we’re thinking about this. First, acquiring or licensing innovation from outside our walls is central to how we’ll achieve our purpose of transforming the lives of patients and their families. Second, as we allocate capital to internal projects and the corporate development, we are focused on making investments that can deliver sustainable revenues and create value for shareholders. We will remain disciplined on price and will not make an acquisition just to meet our Vision 2025 goal.

I’ll close by noting that while I’m still getting up to speed, I’m incredibly excited about the future of this company and the opportunities we have to deliver value to both patients and investors. With that, I’ll turn the call back to Bruce for closing remarks.

Bruce Cozadd: Conclude our prepared remarks on Slide 21, we’ve made important progress towards delivering on our 2024 guidance and objectives and are pleased to be affirming our guidance today. On the commercial side, we expect continued growth of our key products in 2024. And on the R&D front, we continue to advance our pipeline and to invest in long-term growth. We see multiple catalysts in the near-term, including data readouts for suvecaltamide, zanidatamab, Epidiolex and Zepzelca. That concludes our prepared remarks. I would now like to turn the call over to the operator to open the line for Q&A.

Operator: Thank you. We will now begin the question-and-answer session. [Operator Instructions] Your first question comes from the line of Jessica Fye with JPMorgan. Please go ahead.

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Q&A Session

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Jessica Fye: Hey guys, good afternoon, and thanks for taking my two-part question on oxybate narcolepsy dynamics in the quarter. First, can you quantify the headwind to 1Q from the increase in use of patient support programs as the Xyrem patients transition to Xywav? And second, do you have an understanding of how many Xyrem patients losing coverage transition to generic Xyrem or once nightly and not to Xywav? Thank you.

Bruce Cozadd: Thanks, Jess for the question. And Renée, maybe I’ll let you take both parts of that.

Renée Galá: Sure. So Jess, in terms of the – I’ll take the second question first. We’re not disclosing a breakdown of those patients in part because that AG data is not our data to share. But with respect to being able to quantify how many patients came over. I would say there was a good portion of patients that made the decision along with their HCPs to adopt low sodium Xywav and we did see and establish those patient support programs to ensure that we have uninterrupted access for those patients to be able to go from Xyrem directly to Xywav. So what we’ll see in future quarters is you should see a better representation of those patients in the revenue and the net sales that come from Xywav.

Operator: Your next question comes from Jason Gerberry with Bank of America. Please go ahead.

Jason Gerberry: Hey, guys. Thanks for taking my question. My question is about your Phase 2b essential tremor study. So if this trial is successful, I’m wondering how you’re thinking about the subsequent second confirmatory trial. Would it look something like this trial, which took roughly 2.5 years from start to data? Or could there be some sort of more abbreviated randomized withdrawal study that you could run to get yourself to goal line in a more expeditious manner? Thanks.

Bruce Cozadd: Rob, you want to jump in on that?

Rob Iannone: Yes, happy to. So first of all, Jason, remember, this is a Phase 2b trial. It would count, we believe, or contribute to the pivotal regulatory package. But we call the Phase 2b because we included three dose levels of suvecaltamide. And when we would move to, let’s call, the confirmatory Phase 3 trial, we wouldn’t necessarily have to bring all those levels forward, then ideally, we expect we would choose one dose level. So that creates a more streamlined design. And to your point, when we have data in hand and we engage regulatory authorities, we certainly, with compelling data, we’ll be looking for the fastest path to approval and look at all possible trial designs to support that.

Operator: Your next question comes from the line of Marc Goodman with Leerink. Please go ahead.

Marc Goodman: Bruce had a lot of discussions with investors over the past six months about what Jazz wants to be and what it’s transitioning from and to and just the whole big picture discussion and a lot of investors believe you want to become an oncology company, at least that’s the perception out there. Just curious, can you talk about just what is it that you expect Jazz to become what you’re looking for Jazz to be in five years, six years, seven years, just because all the investments you’re making today are obviously going to be reflected in five or six years and just talk about that and how maybe it’s evolved since what Jazz was 5, 10 years ago? Thanks.

Bruce Cozadd: Yes. Thanks, Marc. So we’re in a nice position of having growing assets on the neuroscience side of our business in Xywav and Epidiolex with, we believe, promise in front of us, including pipeline programs like the 385 program, we were just talking about. We’re also excited about what’s going on, on the oncology side of the business with double-digit growth coming from our current portfolio, led by Rylaze, but also opportunities in front of us with zanidatamab, where we’ve already got the submission complete and looking forward to a launch in 2025 or earlier. Zepzelca data upcoming, but also an earlier stage pipeline, including particular expansion opportunities with zanidatamab and beyond. So we’re excited about both those franchises.

While there has been a lot of focus on oncology and certainly the single largest program in our R&D pipeline right now is zanidatamab, I would not say we’re trying to turn the company into an oncology company. We’d like to have strength in both of our franchises. The investments we’re making, and I think Phil described it nicely in his comments are designed to both help the short-term particularly some of our commercial investments that we think can continue to generate great growth from our commercial portfolio. And R&D investments that will continue to broaden that pipeline and provide growth over the – both the near-term and the medium and long-term, but then also those corporate development opportunities, fueled by our strong cash flow and balance sheet and a history of doing transactions that continue to add to our portfolio allow us to impact more patients in more diseases, in more territories around the world.

So I think about it as having to make smart investment decisions, which we’re in a position to do given the financial strength of the company to fuel both the short and the long-term to create value for our shareholders. So execution in the short-term important, investment decisions always important, but I think that should give you a better sense for where we’re headed.

Operator: Your next question comes from the line of Annabel Samimy with Stifel. Please go ahead.

Annabel Samimy: Hi, thanks for taking my question. I had a two-part on zani. I guess the first is, how should we think about the opportunity for zani in GEA in light of the better KEYNOTE data, OS that they announced today on KEYTRUDA. And I guess, secondly, where would zani sit into this paradigm. Separately, for launch in zani and as we think about all these indications, how should we think about how rapidly new cancer drugs with superior efficacy profiles can disrupt mainstay standard of care? I guess, in other words, are these ramps going to be more rapid? Or just as challenging as say in other nonfatal conditions. So I just wanted to get some characterization there. Thanks.

Bruce Cozadd: Yes, Annabel, thanks for the question. And on the zanidatamab, first question, GEA, we had been expecting positive OS results at some point out of that trial, I think most people had. So I don’t think that changes the landscape, but I’ll let Rob comment on where zani could fit into the GEA landscape. And then on your second question, it’s all about results and uniqueness of mechanism of action and benefit relative to other therapies that determine how fast you can make progress from launch. And when we have the opportunity to bring something really new to patients in terms of benefit, particularly in the oncology space, where I think things can move sometimes even ahead of a regulatory approval, if there’s strong data that’s been presented that’s picked up in the NCCN guidelines and allows for reimbursement, you can get fairly rapid traction with a better option. Rob, you want to talk about the landscape in GEA?

Rob Iannone: Yes. So in the context of HER2 positive over expressed gastroesophageal adenocarcinoma, we think zanidatamab has the potential to be the HER2 antagonist of choice because of its differentiated mechanism of action and because of the differentiated efficacy safety profile. Certainly in the PD-L1 negative population, which we think is sizable, there is no approved PD-1 agents. And so the comparator there is Herceptin chemotherapy. But even in the PD-L1 positive population, where we think PD-1 agents are essentially interchangeable, we have the opportunity in combination with tislelizumab to show the benefit of zanidatamab, again, has a differentiated HER2 antagonist in combination with backbone chemotherapy and a PD-1 antagonist.

Operator: Your next question comes from the line of Akash Tewari with Jefferies. Please go ahead.

Akash Tewari: Hey thanks so much. Just going on the HERIZON-GEA study, how should we really interpret the JACOB trial. Here, we saw the addition of Perjeta didn’t provide any OS benefit in GEA on top of tras chemo, and this is a large base – large-scale Phase 3 what gives your team confidence that ZW25’s early data will hold up in this setting? And then maybe just on essential tremor, JZP385 effectively showed no benefit on an accelerometer measurement in its Phase 2 trial. Do you feel like there was something about how the kits were administered in that study that may have skewed those results and how confident do you feel like – how confident do you feel in your ability to show a signal on the accelerometer endpoint with your upcoming data. Thank you.

Bruce Cozadd: Yes, Akash, thanks for the questions. And maybe I’ll start on the essential tremor and then let Rob add anything he’d like on the ongoing trial and then comment on your zani question. Just to remember that the prior T-CALM study for essential tremor did demonstrate a nice benefit on TETRAS 80 activities of daily living, which we believe is a measure that’s actually more important to patients than the measurement of the quantity of tremor. What patients want is to be able to live their life to do the things they need to do to be able to drink out of a cup, to be able to button and unbutton clothes, to be able to apply makeup to do the things they care about. And we were very pleased that, that became more of a focus for the pivotal endpoints in later-stage trials. I think FDA too understands you want to do what’s really going to provide a benefit to patients. Rob, you want to talk a little bit about our ongoing trial and then pivot to zani.

Rob Iannone: Yes, happy to. And so I would agree, Bruce, that the endpoints that we prioritize as primary, not only the most meaningful to patients, but endorsed by FDA. And on those endpoints, we have confidence from the T-CALM trial. And I would just add to that, in the current Phase 2b trial with a new once-daily formulation, we’ve been able to push that dose to exposures that would be higher than in the T-CALM trial itself because we have 10, 20 and 30 milligram doses in that trial. So we think based on that, we’re positioned for success. And then coming back to the question on JACOB and GEA, the key point I’d like to make is we really believe that zanidatamab is differentiated from even the combination of Herceptin and Perjeta.

As we presented at our R&D Day, we stepped through some important data that were published in Nature Communications, showing how zanidatamab is differentiated. With two epitopes necessarily buying to distinct receptors, causing more effective receptor clustering and internalization and have demonstrated better immune function, for example, complement fixation. And so in that paper head-to-head and preclinical experiments better than Herceptin and Perjeta and the clinical data bear that out without going into great detail, if you look at the BTC data, where the response rates are over 40% and duration of response greater than 12 months, that compares very favorably to prior data with the combination of Herceptin and Perjeta. And of course, we have data in breast cancer showing activity of zanidatamab even after patients have failed frontline therapy with Herceptin and Perjeta as part of a CLEOPATRA regiment.

So that in combination with the data that you referred to, zani and chemo and then separately, a cohort of zani and chemo tislelizumab shown very promising not only response rates, but very, very durable responses. That’s what gives us confidence that our Phase 3 trial will be successful.

Operator: Your next question comes from the line of Ami Fadia with Needham & Company. Please go ahead.

Ami Fadia: Good evening. Thanks for taking my question. Perhaps I had a question for Phil, just with regards to his comments around business development. And that’s a question that we get often from investors as well. Can you talk about some of the metrics that you would use to really evaluate potential deals in terms of kind of what really could meet the bar in terms of what Jazz would be interested in executing on? And also, can you talk about capital – use of capital across R&D, business development, but also perhaps buyback of shares? Thank you.

Bruce Cozadd: Thanks, Ami. Phil, go ahead and jump right in.

Phil Johnson: Great, Ami. Thank you for the question. My first one on Jazz earnings call and even I’ve been around for all my miles to listen to these. So thanks for giving her early Mother’s Day [ph] presents. In terms of our corporate development evaluation, first and foremost, there are a number of nonfinancial criteria that we would look at. Primarily, these are things like is there an area with significant unmet need with the medicine that we’re looking at acquiring our medicines really meaningfully impact patients. Is there an efficient commercial call point. We do have a relatively focused business and want to make sure that we’re set up for success to commercialize the assets that we’re bringing in. Will allow us to leverage the expertise we’ve got in-house, the commercial footprint we’ve been built out and continue to build out, for example, with Japan coming soon.

And we’ll stay largely focused as we talked in the past, and neuroscience as well as oncology, but we have looked at things in the rare orphan space as well given the kinds of capabilities that we built up selling products with these types of limited patient populations. From a financial perspective, it really, I think, some of the traditional things that you would expect. We do want to have line of sight to getting a good return on the investment. We’ll look at things that would vary some of the key assumptions, not only draft launch label and competitive landscape, but also time line to continue to make a return on investment in the marketplace, different options for exclusivity, be that through orphan drug exclusivity through patent life or other extensions.

So I think find nothing unusual in terms of the financial evaluation that we have there. But first and foremost, we need to figure out is just a Jazz asset and one where there can be a significant value proposition for patients. In terms of capital priorities, I’d say, first and foremost, very consistent with what you’ve heard in the past from Bruce, Renée and the team were focused on driving the commercial opportunities for the in-market products that we have are dedicating significant monies to get those to as many patients as possible that can benefit from those medicines. We then are looking to rapidly progress the existing pipeline that we have. Obviously, we’re making significant investments behind zanidatamab, given the data that we generated post the licensing deal and then looking at business development to further augment our growth prospects for the future.

Once we’ve exhausted those possibilities, then we look to return excess cash to shareholders. So, I hope that gives you a sense for how we’re looking at prioritizing capital going forward.

Operator: Your next question comes from the line of Joseph Thome with TD Cowen. Please go ahead.

Joseph Thome: Hi there, good afternoon and thank you for taking my questions. Maybe one on the upcoming essential tremor readout. What is sort of the bar for clinical meaningfulness on the TETRAS endpoint? Or I guess what is your internal bar, you think, for kind of taking the program forward. And then one just point of clarification because I think in response to one of the earlier questions, the Phase 3 for essential tremor was referred to as a confirmatory trial. So I just want to make sure that was actually confirming the dose and not that that Phase 2b could potentially be used for approval and then you would do a Phase 3 confirmatory study? Thanks.

Rob Iannone: Yes. Thanks for giving me the opportunity to clarify. I didn’t mean to imply that we would get approval based on the Phase 2b just that it will be part of a package and typically in the space, FDA will be looking for independent studies to confirm efficacy. I did want to point out that when we go to that second efficacy study we’re likely to only use one dose, which would be a streamlined design because I think the earlier question had to do with, could you move more quickly than you did with the Phase 2b study. We haven’t said, in particular or specifically, what level of difference on the ADS or the performance scale that would be meaningful enough for approval or for patients. But I would just highlight that there really hasn’t been any therapies for this disease almost ever, even though things like propranolol and primidone are used.

They really have minimal efficacy. So there’s a substantial unmet need. And I would just say, based on what we saw from the T-CALM study, we think that that suvecaltamide really has an opportunity to make a meaningful difference on the endpoints that matter to patients. And overall, in terms of its provability, it will be based on that – the effect size of those primary and secondary endpoints as well as the overall tolerability, which we think will be good given the once-daily extended release and the titration that we did in the trial.

Operator: Your next question comes from the line of Ash Verma with UBS. Please go ahead.

Ash Verma: Hi there. Yes, thanks for taking my question. I just wanted to get a sense like in the long term for narcolepsy. I understand from your perspective that you believe that Xywav will remain an oxybated choice. But in your view, like what percentage of patients do you think may ultimately switch to a once-nightly or generic Xyrem? And then as you’re trying to extend your leadership in the sleep arena, are you committed to potentially pursuing another orexin or try to internally develop once a day [ph] candidate? Thanks.

Bruce Cozadd: Yes. Ash, maybe I’ll take the second part of your question first. And then, Renée, maybe you can hop in on the narcolepsy side. Rob gave you a little bit of an update on the 441 program. We’re doing a little more work there and conferring with our partner before we announce next steps. We have previously said we have other backup programs behind that as well. We find this an interesting area, certainly with a lot of promise, though development remains early in the orexin space. But in terms of a new mechanism of action, it already has proof of concept, and we’re definitely interested in the benefit that can bring to patients. Renée?

Renée Galá: Yes. Thanks, Bruce. So I would say with respect to Xywav, clearly, we saw both strong patient growth and net sales growth year-over-year, that was 14% in terms of net sales growth. And we believe that reflects Xywav as being a differentiated therapy, the only low sodium oxybate on the market and the number one treatment for narcolepsy. I would say with respect to people trying a fixed dose high sodium oxybate, we’ve said we do expect some patients to try that branded therapy. We do expect that certain patients and HCPs will want to get experience with a fixed dose regimen. What we are hearing anecdotally and also seeing with respect to patients is that we are seeing some patients not get a full night’s coverage.

We believe that there is benefit to being able to have a full night’s coverage in terms of sleep. And the flexibility that comes with the twice-nightly dosing. But more importantly, as the only low sodium oxybate on the market, we are seeing that educating on the benefits of low sodium, publishing and investing in evidence generation on this front. That message is resonating with HCPs. We have seen data showing the faster than expected negative impact from a cardiovascular perspective that patients have when they start a high sodium oxybate therapy, and we believe that patients and HCPs will ultimately continue to prioritize long-term health when it comes to their oxybate therapy with respect to [indiscernible]. These are both chronic conditions and that gives us continued confidence in the long-term growth and durability of Xywav.

Operator: Your next question comes from Joon Lee with Truist Securities. Please go ahead.

Joon Lee: Hey, thanks for the updates and for taking our questions. You had a lot of presentations at AM [ph] and one in particular was on the efficacy of Epidiolex and focal-onset seizures in the context of an Expanded Access program. And the study showed a median seizure reduction in the mid-70% range. How prevalent is the off-label use of Epidiolex. And what sort of growth opportunities do you think you have there? There’s a lot of investor interest in focal focal-onset seizures these days. Thank you.

Bruce Cozadd: Renée, do you want to take that?

Renée Galá: Sure. Well, clearly, with respect to our promotional activities, we focus our promotional activities on those indications where we are approved, that being LGS, Dravet and TSC. However, we do see continued use based on seizure type. And we do see continued use in other refractory epilepsies, and that is an area that we assume will continue to provide growth for Epidiolex. The reality, when you think about the overall benefits of Epidiolex in terms of being a highly differentiated treatment, it has broad spectrum efficacy working through a novel MOA and in an area, which is characterized by polypharmacy having a favorable and well-characterized safety profile means that the product lends itself well to being combined with multiple other therapies, in particular, for physicians that see patients that are refractory with respect to seizures.

And on top of that, they’re really starting to appreciate even more based on the data that we continue to generate and present around the benefits beyond seizures and also underpins our further investment in generating additional data such as the EpiCoM study that we’re getting underway. So we do believe we’ll continue to see growth with Epidiolex, both in our approved indications and also in other refractory epilepsies, which, again, we do not promote for. This is a long-lived durable asset for us that we will continue to look at as a global growth product with additional growth opportunities. outside the U.S.

Operator: Your next question comes from the line of Gregory Renza with RBC Capital Markets. Please go ahead.

Gregory Renza: Hey, good afternoon, Bruce and team. Thanks for taking my question. Bruce, we certainly appreciate all the color you and Philip provided on the strategic thinking as well as capital allocation, especially when it comes to internal investments. And just aside from the diversification of top line when it comes to neuroscience and sleep as well as the oncology portfolios, can you just speak to the synergies, the benefits and even the cross talk that you think is important for us to know when it comes to keeping both portfolios under the Jazz umbrella? Thanks so much.

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