Intellia Therapeutics (NTLA) Q2 2023 Earnings Call Transcript

Transcript

Operator (participant)

Good morning, and welcome to the Intellia Therapeutics second quarter 2023 earnings conference call. My name is Drew, and I will be your conference operator today. Following formal remarks, we will open the call up for a question-and-answer session. This conference is being recorded at the company's request and will be available on the company's website following the end of the call. As a reminder, all participants are currently in listen-only mode. If anyone requires operator assistance during the conference, please press star zero on your telephone keypad. I will now turn the conference over to Ian Karp, Senior Vice President, Investor Relations and Corporate Communications at Intellia. Please proceed.

Ian Karp (SVP of Investor Relations and Corporate Communications)

Thank you, operator, and good morning, everyone. Welcome to Intellia Therapeutics' second quarter 2023 earnings call. Earlier this morning, Intellia issued a press release outlining the company's progress this quarter, as well as topics for discussion on today's call. This release can be found on the Investors & Media section of Intellia's website at intelliatx.com. This call is being broadcast live, and a replay will be archived on the company's website. At this time, I would like to take a minute to remind listeners that during this call, Intellia management may make certain forward-looking statements and ask that you refer to our SEC filings available at sec.gov for discussion of potential risks and uncertainties. All information presented on this call is current as of today, and Intellia undertakes no duty to update this information unless required by law. Joining me from Intellia are Dr. John Leonard, Chief Executive Officer, Dr. David Lebwohl, Chief Medical Officer, Dr. Laura Sepp-Lorenzino, Chief Scientific Officer, and Glenn P. Goddard, Chief Financial Officer. John will begin with an overview of recent business highlights. David will provide an update on our clinical programs. Laura will review our R&D progress, and Glenn will review Intellia's financial results for the second quarter 2023 before we open up the call for your Q&A. With that, I'll now turn the call over to John.

John Leonard (CEO)

Thank you, Ian. Thank you all for joining us this morning. At Intellia, we're leading the genome editing revolution with the broadest and deepest toolbox of novel editing and delivery solutions. 2023 continues to be another year of important progress across our clinical pipeline and differentiated genome editing platform. We're particularly pleased with the significant advancement of our two lead clinical programs. Not only are these two programs potentially paradigm-shifting treatments for patients with ATTR amyloidosis and HAE, our success and learnings from these investigational therapies will help set the foundation for our broader long-term goals and strategic priorities. Starting with INT-2002, in development for the treatment of hereditary angioedema, today we announced that in just a handful of months, we were able to identify all patients required to fully enroll the ongoing phase II portion of the study.

Notably, we now expect to initiate the phase III program as early as the 3rd quarter of next year, subject to regulatory feedback. In addition to the exceptional clinical development, execution, and recent positive data update for INT-2002, we're getting very close to submitting our second in vivo IND application. This next IND submission, expected in September, will support the planned pivotal trial of INT-2001 for people with a cardiomyopathy manifestation of ATTR amyloidosis. Some estimates indicate there may be as many as 500,000 people around the world who suffer from this disease. Subject to regulatory feedback, we expect to initiate the global phase III by year-end. We believe all this progress positions us well to deliver on initiating pivotal studies for both programs, a core strategic priority over this year and next.

Lastly, I'd like to take this opportunity to thank Jean-François Formela, one of our founding board members, who retired from our board in June. Jeff's vision and leadership over the past decade have been integral to our growth and recent achievements. I'll now hand the call over to our Chief Medical Officer, David Lebwohl, who will review the lead clinical programs in greater detail. David?

David Lebwohl (CMO)

Thanks, John, and welcome everyone. I'll begin with 2001, our in vivo CRISPR-based candidate with the potential to halt and reverse disease in people living with ATTR amyloidosis after a single dose. For ATTR-CM, consistent with our prior guidance for a mid-year submission, we are on track to submit an IND application in September for a global pivotal study of 2001. We are in the final stages of preparing the comprehensive IND package and expect to initiate the study by year-end, subject to regulatory feedback. For hereditary ATTR-PN, we are continuing to make steady progress with the preparations for a phase III study. Looking ahead, we plan to present additional data from both arms of the ongoing study later this year.

Moving to 2002 in development for HAE, we have been really pleased with the interest and enthusiasm for the 2002 program from investigators and patients alike, both in the U.S. and internationally. The updated phase I data presented in June has fueled this enthusiasm even further. Across all 10 patients, a 95% mean reduction in monthly attack rate was observed after a single dose of 2002 through the latest follow-up. The median duration of follow-up was 9 months, and at all 3 dose levels, 2002 has been well tolerated and any adverse events were Grade 1 or 2 in severity. Earlier this morning, we announced that we have identified all patients needed to complete enrollment in the phase II portion of the study.

Based on the high level of interest for 2002, all slots have been allocated to current ex-U.S. sites. Other sites planned for phase II, including U.S. sites, will now be part of the planned phase III study. Following the clearance of our IND, we received a request from the FDA to provide supplemental preclinical data related to the inclusion of female patients of childbearing potential. While we could have proceeded with enrolling U.S. patients outside of this subgroup with a protocol amendment, the study was already rapidly enrolling at ex-U.S. sites and soon to finish. After discussion with the FDA, we have come to an agreement on the design of a reproductive study in mice to supplement the data that we have already supplied in our initial IND submission.

Such data are often required as part of a registrational program and will now be submitted, along with additional data being generated in advance of the initiation of the phase III study. The main objective of the phase II is to confirm the optimal dose for phase III. By enrolling a diverse patient population, ex-US, including women of childbearing potential, we are in a great position to move forward to do just that. Further, we announced today that we now expect to begin the phase III study as early as the third quarter of 2024, subject to regulatory feedback. We are full steam ahead and look forward to updating you on our progress for initiating the 2002 global pivotal study. I'll now hand the call over to Laura, our Chief Scientific Officer, who will provide updates on our R&D efforts.

Laura Sepp-Lorenzino (CSO)

Thank you, David. Beyond our lead programs, we're advancing a pipeline of in vivo and ex vivo programs towards the clinic. For NTLA-3001, our first wholly-owned in vivo insertion program, we continue to conduct IND-enabling activities and plan to submit a CTA by year-end. We're excited to be moving this program into the clinic for a number of reasons. First, there are few effective therapeutic options for patients suffering from alpha-1 antitrypsin deficiency, a frequently debilitating and fatal disease. Based on our preclinical work, we believe NTLA-3001 can normalize alpha-1 levels for patients following a single dose. Additionally, NTLA-3001 will be Intellia's first gene insertion program to enter the clinic. If successful, we believe we can apply this modular approach to a host of diseases caused by a missing functional protein where there is high unmet need.

We look forward to updating you on our progress across our R&D platform more broadly as we move through the second half of the year. I'll now hand over the call to Glenn, our Chief Financial Officer, who will provide an overview of our second quarter 2023 financial results.

Glenn P. Goddard (CFO)

Thank you, Laura. Good morning, everyone. Intellia continues to maintain a strong balance sheet that allows us to execute on our pipeline and platform. Our cash, cash equivalents, and marketable securities were $1.1 billion as of June 30, 2023, compared to $1.3 billion as of December 31, 2022. The decrease was driven by cash used to fund operations of approximately $227.3 million. The decrease was offset in part by $24.6 million of interest income, $8 million of collaborator reimbursements, $3.3 million in proceeds from employee-based stock plans, and $1.5 million of net equity proceeds from the company's at-the-market program.

Our collaboration revenue decreased by $0.4 million to $13.6 million during the second quarter of 2023, compared to $14 million during the second quarter of 2022. R&D expenses increased by $25.1 million to $115.3 million during the second quarter of 2023, compared to $90.2 million during the second quarter of 2022. The increase was mainly driven by the advancement of our lead programs and personnel growth to support these programs. Stock-based compensation included in R&D expenses was $22.4 million for the second quarter of 2023. G&A expenses increased by $8.5 million to $30.7 million during the second quarter of 2023, compared to $22.1 million during the second quarter of 2022.

This increase was primarily related to an increase in stock-based compensation of $5.1 million. Stock-based compensation included in G&A expenses was $14 million for the second quarter of 2023. Finally, we expect our cash balance to fund our operating plans beyond the next 24 months. It's certainly been a very productive first half of the year. We have a number of additional milestones still to come in the months ahead. With that, we will now open the call for your questions. Operator, you may now open the call for Q&A.

Operator (participant)

We will now begin the question and answer session. To ask a question, you may press star then one on your touch tone phone. If you're using a speakerphone, please pick up your handset before pressing the keys. To withdraw your question, please press star then two. Please limit yourself to one question. At this time, we will pause momentarily to assemble our roster.

The first question comes from Maury Raycroft with Jefferies. Please go ahead.

Maury Raycroft (Equity Research Analyst)

Hi, good morning. Congrats on the progress, and thanks for taking my question. When you get the 2001 pivotal IND cleared after filing the IND in September, can you clarify if you will disclose details of the trial design? Is base case that the trial size and duration will be similar to Alnylam HELIOS-B, or based on the BridgeBio results recently, do you have more confidence you can run a smaller study compared to Helios-B?

John Leonard (CEO)

Thanks, Maury, for the question. Good morning, to, to you and all the listeners. As we've done in the past, when we get to a state of some finality with protocols, we share the details, and we would expect to do the same here. With respect to the particulars of the study, maybe David, you could tell us whether or not the BridgeBio or Ionis approach is more or less in focus for us.

David Lebwohl (CMO)

Yeah, thanks. Yeah, the, the BridgeBio result is obviously very encouraging to us that after their first result, people were concerned that this area was hard to improve the patient's status. They were too healthy. It's clearly not true from what we see in their overall results. We do need to see the details of what they have. That will be coming up. Those details are gonna be very helpful to us in the design of our trial. We'll know more about event rates. We'll know more about the status of patients. Now, the drug itself, the BridgeBio compound, is obviously very similar to tafamidis. It works by a different mechanism. We do think that these are likely not as good as reducing TTR. As you know, we've been able to get to very low levels of TTR.

You know, we use all the information coming from this as well as later studies to size the trial. We do think it'll be about the size, pretty similar to the Alnylam trial to, to Helios.

Operator (participant)

The next question comes from Luca Issi with RBC Capital. Please go ahead.

Speaker 22

Hi, this is Rena on for Luca. Thanks for taking my question. Just wanted to ask, could you remind us what the latest thinking is on gene editing outside the liver? If I recall, I, I think you showed us some tantalizing data last year for in vivo editing of CD34, hematopoietic stem cells. Wondering if you had any update there?

John Leonard (CEO)

Generally speaking, I can tell you that we continue to work very, very hard on moving, in vivo editing outside the liver. You're right, we've presented some really, encouraging data, particularly with respect to hematopoietic stem cells, thinking down the road in terms of, things like sickle cell disease, et cetera, where, you know, the preferred approach would be not to do a bone marrow transplant, but to actually use, an LNP in vivo editing approach to, you know, avoid the, morbidity that, typically accompanies a bone marrow transplant. We continue to do that work.

I will say that we are pursuing a variety of different modalities that target even beyond HSCs, and has been typical for us in the past, as we think that we have a body of work that is ready to be presented scientifically. We will share that. Rest assured, there's, there's more to come.

Operator (participant)

The next question, the next question comes from Joseph Thome with TD Cowen. Please go ahead.

Joseph Thome (Managing Director and Senior Biotechnology Equity Research Analyst)

Hi there. Good morning, and thank you for taking my question. Maybe just one on the additional data for the women in childbearing age. I guess, was there anything that spurred this ask by the FDA? As you think about applicability to your other programs, obviously ATTR-CM is, you know, more predominantly a male disorder and older patients. I guess, is there any implications for this for the upcoming IND submission? Thank you.

John Leonard (CEO)

There's, there's no safety data that's provoked this particular request. Of the extensive work that we supplied in, in the IND, which includes very large breeding studies and careful analysis of that data, we've looked at germline cells specifically. We know that they're unaffected. Our view is that this is the FDA taking a very considered view of the space and looking for us to fill out what is a typical set of data that usually is supplied a little later in a program. From the standpoint of, of, you know, the study itself, this is something that is, is commonly done.

No clinical data, et cetera, has appeared that speaks to this at all, and we're well on our way to completing the work and supplying it to the FDA so we can get on with the study as we, as we said. I guess, I'm sorry, before I forget, the... You, you asked about implications with respect to 2001. At this point, we don't see that, and certainly your point of you look at the demography of that disease, it's typically a patient, set of patients that are older, biased to men in general, and so we just don't see it playing out in any really fundamental way with respect to the program.

Joseph Thome (Managing Director and Senior Biotechnology Equity Research Analyst)

Great. Thank you.

John Leonard (CEO)

Sure.

Operator (participant)

The next, the next question comes from Greg Harrison with Bank of America. Please go ahead.

Mary Kate (Leveraged Finance Investment Banking Analyst)

Hey, good morning. This is Mary Kate on for Greg. Thank you so much for taking our questions. It's, it's great to hear the interest from the HAE program. I guess looking at your other programs, what feedback have you received from physicians and patients, in the ATTR programs ongoing?

John Leonard (CEO)

... Maybe David, you can speak to your interactions, that they're becoming pretty extensive at this point. What are you learning?

David Lebwohl (CMO)

Yeah, thanks. Yeah, the, the biggest group that we hear from, of course, is investigators who we're in touch with around the world. I would say we've talked with every investigator who treats patients at the leading centers with this disease. There, there is a lot of excitement. We, we do know most of those sites or maybe all those sites will end up joining the study. As you've seen in some of the other studies, these studies do enroll quite briskly, and there really is a, a increasing population of patients with ATTR amyloidosis and cardiomyopathy. We also, we hear about patients through, through some of these physicians, the excitement that's there.

Well, I'll have David address why we're excited about, as you pointed out, the very, very deep reductions critically for the study, the very low variance that we see across all the patients treated so far, we're quite convinced that that's gonna be a meaningful advantage for patients. With respect to phase III readiness, we put a lot of work into preparing for that IND that will enable that phase III program. Your point about, you know, having commercial material readiness as one carries out these phase III trials is a really important observation. The idea is, you know, to complete this trial, get the results that we're looking for, have the final material in the study, and be in a position that when we achieve approval for the product, to move forward as quickly as possible to the marketplace.

We've always been shooting ahead of the duck, so to speak, and, and this is very much a, a part of, how we've been thinking about it. David, if you have something to add with respect to, TCR levels and how that translates into that clinical benefit.

David Lebwohl (CMO)

Yeah, we, we, we do believe that these deep reductions we're getting, not only being at the 90% and greater range, but also having the great consistency, means that we have the potential to benefit all patients. There aren't patients who are having lesser amounts. You know, when you have an average of 80% with other agents, half the patients have less than 80% reduction. That, that's very important. The, the other thing we're, we're learning in terms of survival advantage, I think, is what we've seen in the BridgeBio study. We, we've talked a lot about how we don't think the 6-minute walk is a great test, in fact, they, they, their study failed on that test. What we're seeing is that you do need a longer period to see the benefit of these agents.

We do think by having a large study with long follow-up, we will, come out positive on the most important endpoints, that will include cardiovascular events and, and mortality. That's what we're looking forward to, in our phase III study.

Operator (participant)

The next question comes from Yanan Zhu with Wells Fargo Securities. Please go ahead.

Yanan Zhu (Senior Analyst of Biotechnology Research)

Thanks for the questions. What would be the timeline for completing the supplemental preclinical data that, that you, you know, U.S. FDA has agreed upon about the design of? Do you think, you know, do you plan to collect certain data from the female patients of childbearing age in the upcoming phase II study? If so, what might those data points be? Thanks.

John Leonard (CEO)

Well, the particular studies that we're doing are in abbreviated form of what are typical studies that look at embryological development. That will be done well in advance of what would be the earliest phase III study start for us, which I said earlier, could be as early as third quarter. With respect to precise month and all that, it's just not gonna have an effect in terms of how the program proceeds. I think we're well on our way. David, anything different that we're doing for collecting patient data on women?

David Lebwohl (CMO)

No, it is not. You know, they get the same complete data collection that other patients get. Of course, we'll, we'll look at all patients. We look at studies by gender and other things to see if there's any difference in the effect. We, we don't expect to see any difference between males and females or older or younger women. Of course, another part of follow-up in these studies is looking at pregnancies that may occur after the study. We know we have a number of those patients who are specifically getting on the trial so they, they can move on to have successful pregnancies. Of course, we look forward to bringing that, that great result forward in the future, if we can.

John Leonard (CEO)

Yeah, just a reminder to the audience here that in the preclinical work, there's been zero evidence of that, there's any germline involvement in, in any way.

David Lebwohl (CMO)

Yeah. One of the other, you know, one other point there is, of course, we've talked about before, the prekallikrein gene is not needed at all for, for normal life span. Or a development or fetal development. We know very well from humans that this gene is not essential for embryo development.

Yanan Zhu (Senior Analyst of Biotechnology Research)

Got it. Very helpful. Thank you.

Operator (participant)

The next question comes from Dae Gon Ha with Stifel. Please go ahead.

Dae Gon Ha (Director of Biotechnology Equity Research)

Hey, good morning, guys. Thanks for taking the question. Just staying with this preclinical idea, I guess one of your peers in the Boston area also provided a pretty substantial data from animals. I believe it was NHPs as well as mice. Looking at pretty robust set of data demonstrating the germline, but still got a clinical hold. Any additional color you can provide in terms of the size and breadth of this experiment that you think will be sufficient? Has the FDA clearly outlined exactly how many sample size that they want to see before they kind of confirm that it is substantial? Kind of related to that, have they expressed any N from the phase II that might substantially get their questions answered? Thanks so much.

John Leonard (CEO)

As you've seen in, in everything we've done, we bring forward data when we have meaningful, interpretable, and consistent results that we can show you what the story is. We, we will, we will wait for that as we, whenever we bring up new data.

Operator (participant)

The next question comes from Rick Bienkowski with Cantor Fitzgerald. Please go ahead.

Rick Bienkowski (Director of Biotechnology Equity Research)

Hi, good morning. Congrats on the progress, and just a quick question from me. Last quarter, it was noted that the redosing of patients from the low-dose polyneuropathy arm of 2001 has started. I'm curious if we could expect to see any of these data from the redosing cohort in the end-of-year update, and what type of data could potentially be shared from these patients?

John Leonard (CEO)

David, do you wanna comment on redosing?

David Lebwohl (CMO)

Yeah. Okay, yeah, I mean, what we know, all three patients have been dosed at this point. It's gone well. You know, I don't think we've decided whether to put that into the next update or, or, or future update, we will, we'll, we'll talk about it as soon as we can.

Rick Bienkowski (Director of Biotechnology Equity Research)

Got it. Thank you.

Operator (participant)

The next question comes from Jay Olson with Oppenheimer. Please go ahead.

Jay Olson (Biotech Equity Research Analyst)

Oh, hey, congrats on all the progress, and thanks for taking the question. Can you talk about the rationale and the strategy behind pursuing a CTA for 3001 this year, but not an IND? What are the gating factors and timeline to filing an IND? Thank you.

John Leonard (CEO)

David, if you wanna speak to that.

David Lebwohl (CMO)

Yeah, as, as we've done in the past, I think what you've seen is we, we look at several things in the first country that we go to. We look at the, the sites that are available, the investigative sites. That's, that's very key to us, getting high-quality sites. We, we look at the regulatory environment, and all those are pieces of what, of what we put together. And in this case, we did decide, as we have in several of the other compounds, that, that going with the CTA is, is the best choice. Gating factors for an IND are, are, you know, similar to what we've had for other INDs.

Of course, you need the, you know, the, the, the pieces of CMC picture is a, is a big piece of our applications and, of course, getting agreement on, on trial designs. All those things, are possible, for a later submission to the as an IND.

Jay Olson (Biotech Equity Research Analyst)

Great. Thank you very much.

Operator (participant)

The next question comes from Silvan Tuerkcan with JMP Securities, JMP Securities. Please go ahead.

Silvan Tuerkcan (Managing Director and Senior Research Analyst in Biotechnology)

Hey, good morning, and thanks for taking my question. I just have a more general question. With the CRISPR-X cell potential approval coming up in the U.S. by the end of the year, and then potential subsequent reimbursement, is there anything from those models that we can learn that will be applicable to, for example, your ATTR programs, or is that too far off at this point? Thank you.

John Leonard (CEO)

Well, obviously, we watch those spaces very, very carefully. I don't think that the world has converged on a final model for, you know, drugs like this that are potentially curative. But I see emerging trends. There's gonna be some really interesting, I think, examples that, of course, we will study very, very carefully. Our view right now is to have the best possible drug that moves the efficacy bar substantially forward and captures savings for the healthcare system, et cetera. I think that that'll be the basis for whatever pricing model we ultimately come up with. We're confident that the, you know, health advantages and the efficacy that we expect to deliver will be of value to payers and whether it's in the U.S. or ex-US.

Silvan Tuerkcan (Managing Director and Senior Research Analyst in Biotechnology)

Thank you.

Operator (participant)

The next question comes from Steve Seedhouse with Raymond James. Please go ahead.

Speaker 23

Hi, good morning. This is Nick out for Steve. A couple questions on AATD. Are both knockin and knockout products intended to target patients with the homozygous Z genotype?

John Leonard (CEO)

David, you wanna take a shot?

David Lebwohl (CMO)

Yeah, that, that's really where the need is for the patients who, who are homozygous Z. In terms of the knockout, this is patients where the predominant issue is liver disease. That's, that's the main thing that the knockout addresses. It doesn't address the lung disease. There are a substantial group, maybe, well, I guess it's, it's certainly 15% overall, the patients who, who tend to have liver disease, and that includes patients, some patients with lung disease. The big majority of patients are the patients who need the deficiency is affecting the lungs. That, that is what the knock-in is, is gonna help with by putting in the wild type gene. Many patients will end up getting both because, as they start to live longer, the liver disease may become more important.

The liver disease can be subtle in some patients, and a lot of the physicians feel that they would wanna give their patients both agents over time. Both these agents be given, I should say, in either order. One can be given before the other, either, either one can be given before the other, so that we have a lot of flexibility in how we treat patients.

John Leonard (CEO)

It might be important for some of the listeners to remember that these are independent programs that can be brought together, but we're pursuing them as independent development programs.

David Lebwohl (CMO)

Yeah, these, these are two separate drugs that are gonna be fully developed with all, all the requirements that you have for each drug. It's not, it's not a combination program per se.

Speaker 23

Okay, got it. Thank you. From your preclinical work, do you expect the same level of neutrophil elastase in, inhibition with the AAT protein induced by 3001 compared to wild type M-AAT protein?

John Leonard (CEO)

What we've presented in non-human primate work is this approach was able to reproduce levels seen in non-human primates that were essentially indistinguishable from normal human levels of circulating Alpha-1. Our, you know, target is to accomplish just that in patients. You know, the preclinical model suggests that we may well be able to do that. Laura, is there anything you want to add to how we're thinking about Alpha-1?

Laura Sepp-Lorenzino (CSO)

Yeah, no. You need to ensure that not only you have protein levels, but those, you know, proteins are active, right. That the activity is what you need to have. You know, as John just described, that's what we accomplish in the non-human primate. The expectation is that that's going to translate to humans.

Speaker 23

Got it. Thank you.

Operator (participant)

The next question comes from Salveen Richter with Goldman Sachs. Please go ahead.

Speaker 20

Hi, this is Srikripa Devarakonda for Salveen. Thank you for taking our question. A couple of questions. The first on Intellia 2002. In your data update at EACI, you mentioned that patients were allowed to withdraw from HA prophylaxis, they've not experienced subsequent attacks. Any further updates on these patients, as in, have they remained attack-free to date? On your 2001 program, could you provide some color on your, on the regulatory discussions with the FDA on CM and PN? Have they spoken about what they would like to see in the pivotal study? Thank you.

John Leonard (CEO)

Maybe you could remind, questioner about the data we presented on 2002, and I'm sure we'll be having updates as time goes on, but-

David Lebwohl (CMO)

Yeah. I think you recall we did give updated data fairly recently on 2002. Recall is, all the patients who had received prophylaxis were able to withdraw it, and none of those patients have had a subsequent attack in that report. I should mention that, you know, we didn't use Lanadelumab as one of the withdrawals because it would affect our biomarker measures. However, what we're seeing in the phase II is we did allow lanadelumab withdrawal, and that is, we have a number of patients who'll be treated after that withdrawal. Stay tuned. More data is coming for that as, as well.

When we talk to regulators about the phase III, you know, the IND is in, we've, we've had preliminary discussions, but of course, to get agreement that involves the IND submission that we're doing in September for the FDA. We've also had extensive discussions with, with regulators outside the U.S. We feel very good that our, our trial design will address the questions that, that, that, they will have. For PN, we are a little earlier. You know, we did, we did push first on CM as a much larger medical need, more patients needing this. Also with PN, as you said, you know, we will bring you forward more details as we get agreement to the pivotal trial design.

Operator (participant)

The next question comes from Richard Law with Credit Suisse. Please go ahead.

Richard Law (Equity Research Analyst)

Hey, guys. Good morning. Can you discuss the market opportunity for HAE outside the U.S., based on the reimbursement and usage rates for brand products so far? What are the learnings for 2002 as you think about ex-U.S. market that you will need to include in your studies?

John Leonard (CEO)

The bulk of the HAE market today resides inside the United States. We're well aware of that. We do have an eye to what we can deliver outside the United States. What we've seen through the course of our phase 1 and now phase II work, is that there's a great desire to have these products, and we will do our very best to show that not only do the product, does the product work very, very well, but that it can be resource sparing to those typically centralized systems. To the extent that that market opportunity exists, we want to participate in it to the greatest extent possible.

Richard Law (Equity Research Analyst)

Can you compare and contrast the reimbursement for U.S. versus ex-U.S.? Just curious to see how the different markets would affect the product.

John Leonard (CEO)

I think that's something we can address later on as we get further down the road. Generally speaking, you know, this is information that's well publicized and available. The market has been disproportionately a U.S. market, with reimbursement rates that, that are higher. That's typically the case for most drugs, and again, we see that here. Again, we're trying to think through how this particular approach can be demonstrated to be resource sparing, to what are typically, centrally reimbursed approaches, and we'll present that data to those, you know, different systems, and we expect it will be of potential value to them.

Richard Law (Equity Research Analyst)

Great. Thanks.

Operator (participant)

This concludes our question and answer session. I would like to turn the conference back over to Ian Karp for any closing remarks.

Ian Karp (SVP of Investor Relations and Corporate Communications)

Great. Thanks for all the terrific questions and for your continued interest in Intellia and our progress, and we look forward to future updates. Have a great day and a great rest of the week.

Operator (participant)

The conference has ended. You may now disconnect your line. Thank you.

Intellia Therapeutics - Q2 2023

Transcript

Operator (participant)

Ian Karp (SVP of Investor Relations and Corporate Communications)

John Leonard (CEO)

David Lebwohl (CMO)

Laura Sepp-Lorenzino (CSO)

Glenn P. Goddard (CFO)

Operator (participant)

Maury Raycroft (Equity Research Analyst)

John Leonard (CEO)

David Lebwohl (CMO)

Operator (participant)

Speaker 22

John Leonard (CEO)

Operator (participant)

Joseph Thome (Managing Director and Senior Biotechnology Equity Research Analyst)

John Leonard (CEO)

Joseph Thome (Managing Director and Senior Biotechnology Equity Research Analyst)

John Leonard (CEO)

Operator (participant)

Mary Kate (Leveraged Finance Investment Banking Analyst)

John Leonard (CEO)

David Lebwohl (CMO)

Operator (participant)

June S Williams (Managing Director of Equity Research)

John Leonard (CEO)

David Lebwohl (CMO)

June S Williams (Managing Director of Equity Research)

Operator (participant)

Kaushik Dash (Director of Corporate Equity Derivatives)

John Leonard (CEO)

Operator (participant)

Debjit Chattopadhyay (Senior Managing Director)

John Leonard (CEO)

David Lebwohl (CMO)

Operator (participant)

Yanan Zhu (Senior Analyst of Biotechnology Research)

John Leonard (CEO)

David Lebwohl (CMO)

John Leonard (CEO)

David Lebwohl (CMO)

Yanan Zhu (Senior Analyst of Biotechnology Research)

Operator (participant)

Dae Gon Ha (Director of Biotechnology Equity Research)

John Leonard (CEO)

Dae Gon Ha (Director of Biotechnology Equity Research)

John Leonard (CEO)

Operator (participant)

Myles Minter (Biotech Equity Research Analyst)

John Leonard (CEO)

Operator (participant)

Speaker 21

John Leonard (CEO)

David Lebwohl (CMO)

John Leonard (CEO)

David Lebwohl (CMO)

John Leonard (CEO)

David Lebwohl (CMO)

John Leonard (CEO)

David Lebwohl (CMO)

Speaker 21

Operator (participant)

William Pickering (Senior Research Analyst)

John Leonard (CEO)

David Lebwohl (CMO)

John Leonard (CEO)

William Pickering (Senior Research Analyst)

David Lebwohl (CMO)

Operator (participant)

Rick Bienkowski (Director of Biotechnology Equity Research)

John Leonard (CEO)

David Lebwohl (CMO)

Rick Bienkowski (Director of Biotechnology Equity Research)

Operator (participant)

Jay Olson (Biotech Equity Research Analyst)

John Leonard (CEO)

David Lebwohl (CMO)

Jay Olson (Biotech Equity Research Analyst)

Operator (participant)