Arrowhead Pharmaceuticals Inc (ARWR) Q3 2021 Earnings Call Transcript

Transcript

Speaker 0

Ladies and gentlemen, welcome to the Arrowhead Pharmaceuticals Conference Call. Throughout today's recorded presentation, all participants will be in a listen only mode. After the presentation, there will be an opportunity to ask questions. I will now hand the conference call over to Vincent Anzalone, Vice President of Investor Relations for Arrowhead. Please go ahead, Vince.

Speaker 1

Thank you. Good afternoon, everyone. Thank you for joining us today to discuss Arrowhead's results for its fiscal twenty twenty one third quarter ended 06/30/2021. With us today from management are President and CEO, Doctor. Christopher Anzalone, who will provide an overview of the quarter Doctor.

Javier San Martin, our Chief Medical Officer, who will provide an update on our pipeline and Ken Myszkowski, our Chief Financial Officer, who will give a review of the financials. In addition, James Hazard, our Chief Commercial Officer and Doctor. James Hamilton, our Senior Vice President of Discovery and Translational Medicine, will be available during the Q and A session of today's call. Before we begin, I would like to remind you that comments made during today's call contain certain forward looking statements within the meaning of Section 27A of the Securities Act of 1933 and Section 21E of the Securities Exchange Act of 1934. All statements other than statements of historical fact, including, without limitation, those with respect to Arrowhead's goals, plans and strategies, are forward looking statements.

These include statements regarding our expectations around the development, safety and efficacy of our drug candidates, projected cash runway, the receipt of future milestone and licensing payments and expected future development and commercialization activities. These statements represent management's current expectations and are subject to numerous risks and uncertainties that could cause actual results to differ materially from those expressed in any forward looking statements. For further details concerning these risks and uncertainties, please refer to our SEC filings, including our most recent annual report on Form 10 ks and subsequent quarterly reports on Form 10 Q. Arrowhead disclaims any intent and undertakes no duty to update any of the forward looking statements discussed on today's call. With that said, I'd like to turn the call over to Chris Anzalone, President and CEO of the company.

Chris? Thanks, Vince.

Speaker 2

Good afternoon, everyone, and thank you for joining us today. The fiscal third quarter and the period since our last conference call has been incredibly busy for Arrowhead. We made important advances in several of our development programs. This includes discovery stage programs and early, mid and later stage clinical programs. It also includes programs from existing partnerships as well as a new business development transaction.

As a platform company, there are a few areas of critical importance where we focus our attention. First, we need to always push the boundaries of what is possible and make our TRiM platform better. Second, we need to expand the early stage pipeline rapidly and efficiently with new clinical candidates, as this will be an important source of growth in the future. Third, we need to move our mid and later stage pipeline programs through clinical studies as it gets closer, to our goal of bringing important new medicines to patients without adequate treatment options. And lastly, we need to selectively use partnering to expand the reach and maximize the value of our TRiM platform and bring in non dilutive capital that helps to fund our internal development.

I think we're doing well in all these areas. Let's take a moment to briefly review some key events in the last quarter that are good examples of this. For our discovery and early stage clinical pipeline, we had a very productive quarter. We completed discovery and optimization work on two new pulmonary programs and nominated them both as clinical candidates. They are now in the IND enabling stage, which includes GLP toxicology studies, and manufacturing of drug product for clinical studies.

We have not yet disclosed the gene and disease targets, but we'll be talking more about these programs later in the year. We also present very promising preclinical data on ARO DUX4, our first muscle targeted program being developed as a treatment for patients with fascioscapulohumeral muscular dystrophy, or FSHD, at the twenty eighth Annual FSHD Society International Research Congress. The show that the TRiM muscle delivery platform can achieve functional delivery to various types of skeletal muscle and achieve deep, durable, and dose dependent knockdown target genes. In addition, ARO DUX4 improved multiple measures of FSHD like muscle phenotype in relevant preclinical animal models. As DUX4 expression is recognized as the cause of muscle pathology in FSHD patients, Arrowhead believes that the selective targeting and knockdown of DUX4 using RNAi may prevent or reverse downstream myotoxicity and lead to muscle repair and improvement in muscle function in patients.

There are currently no effective treatments specifically for FSHD, so patients need new therapeutic options that address the root cause of the disease. We've been pushing aggressively toward the clinic with ARO DUX4, as well as the two new pulmonary candidates we nominated this year. We expect to file CTAs for all three of them by the end of the year, but securing timely slots at CROs for IND enabling toxicology studies has been challenging, so scheduling on the CTAs will be pushed into the first half of next year. That is unfortunate, but we have seen this become more of a bottleneck in the industry since the beginning of the pandemic. We have continued to work on a number of other early programs, and I'm pleased to announce a previously undisclosed target.

We recently nominated ARO C3 as a hepatocyte directed candidate against complement C3. Overactivation of the complement cascade is thought to be causative of a number of diseases, including paroxysmal nocturnal hemoglobinuria and C3 glomerulopathy. And complement mediated injury is involved in many other conditions, including IgA nephropathy, as well as many other renal, vascular, hematologic, and neurologic conditions. Complement C3 is a central node in all three of the complement pathways, including the classical, lectin, and alternative pathways of complement activation. And it has recently been shown that inhibition of C3 can be both safe and effective in the treatment of complement mediated diseases.

We have a strong track record in TRiM enabled hepatocyte directed candidates, including ARO HBV, ARO LPA, ARO AET, ARO ANG3, ARO APOC3, and ARO HSD. Clinical data from these programs gives us confidence that positive nonclinical data from the ARO C3 may translate well in humans. We believe that an siRNA capable of substantially reducing C3 levels for three months or more could be the modality of choice for C3 inhibition, and we expect to file CTA for ARO C3 by the end of this year. During the quarter, we also announced positive interim data for two of our early stage clinical programs, ARO HIF2 and ARO HSD. I'll start with ARO HIF2, which is our first tumor targeted program being developed as a potential treatment for patients with clear cell renal cell carcinoma, or CCRCC.

To date, investigational ARO HIF2 has been generally well tolerated at doses of up to five twenty five milligrams weekly. The study has now progressed to a dose of ten fifty milligrams weekly, which is currently enrolling and dosing patients. We believe that in the first two dose cohorts, ARO HIF2 is showing clear signs of meaningful target engagement, and potentially some early signs of efficacy in at least one patient. Specifically, the HIF-two alpha protein H score was assessed via immunohistochemistry. Nine of seventeen patients had tumor samples that could be evaluated, and seven of those nine demonstrated reductions in HIF-two alpha protein H scores.

These reductions ranged from minus 9% to minus 82%, with a mean reduction of minus 48%. In addition, one subject had a partial response with approximately sixty five percent tumor shrinkage, and five subjects had a best response of stable disease. We think these early results in a heavily pretreated population are encouraging for ARO HIF2 and our tumor targeted platform broadly. We also presented positive interim data for ARO HSD, being developed as a potential treatment for patients with liver diseases, such as NASH, at the EASL International Liver Congress. ARO HSD was well tolerated in healthy volunteers, given a single dose at twenty five milligrams, fifty milligrams, one hundred milligrams, or two hundred milligrams, and in five patients with suspected NASH, given a one hundred milligram dose of ARO HSD on days one and twenty nine.

All five patients with suspected NASH showed a strong pharmacodynamic effect as measured by liver biopsy at day seventy one. HSD17 beta-thirteen protein was reduced by 92% and 97% in two patients, while the other three patients' day seventy one measurements were reduced below the lower limit of quantitation. Importantly, ALT showed a mean reduction from baseline of forty six percent, with all patients showing reductions ranging from twenty six percent to fifty three percent. We believe that ARO HSD is the first investigational therapeutic to demonstrate robust inhibition of hepatic HSD17 beta-thirteen mRNA and protein expression. We are also highly encouraged to see ALT levels drop significantly following just two doses of ARO HSD.

In addition to progress on our early stage pipeline, we also achieved some important milestones for our mid and later stage pipeline. I'll start with our cardiometabolic programs, ARO APOC3 being developed as potential treatment for hypertriglyceridemia, and ARO ANG3 being developed as a potential treatment for mixed dyslipidemia. We recently started two Phase 2b studies, one for each program. We intend to initiate four or more studies across the two programs, including a Phase three study. Javier will give more details about the studies, that have already started dosing in a few minutes, but we believe the studies together will give us a robust picture on the pharmacologic activity of each medicine in various target patient populations.

We are intending to identify the optimal dose and dose intervals to enable us to move confidently into multiple phase III studies. In addition to our cardiometabolic programs, we had multiple important events in the last quarter for ARO AAT, also known as TAK-nine ninety nine, being co developed with Takeda as a treatment for the rare genetic liver disease associated with alpha-one antitrypsin deficiency. First, we presented additional positive interim forty eight week liver biopsy results at the EASL International Liver Congress. These results demonstrated that ARO AAT treatment led to rapid improvements in multiple measures of liver health, including fibrosis, with substantial and sustained reductions in the level of mutant AAT protein. Mutant AAT protein has been identified as the cause of progressive liver disease in patients with alpha-one antitrypsin deficiency.

ARO AAT treatment was generally well tolerated after up to one year of treatment. This is very important data and suggests to us that the drug is doing what it is designed to do, and that removing the mutant AAT protein can give the liver a chance to begin the healing process, even when intervening in patients with late stage liver disease. We and our partners at Takeda were thrilled to see these results, and we have received similar responses from physicians and others in the alpha-one treating community. We also fully enrolled the ARO AAT Phase II SEQUOIA study, with the fortieth patient being dosed recently. Combined with the various cohorts in the open label 2,002 study, we will have paired biopsies from approximately 50 patients receiving various dose levels and various treatment durations.

Lastly for ARO AAT, we are granted breakthrough therapy designation by The US FDA. ARO AAT was also previously granted Orphan Drug Designation and Fast Track Designation from the FDA, and Orphan Designation from the European Commission. Our goal is to expedite the development path of ARO AAT, and each of these important designations provide potential ways to achieve that. We will work with regulatory authorities and our partners from Takeda to identify the best path to bring this important drug to patients quickly. Now moving on to progress that we've made with partnering.

As I mentioned, we believe a platform company should use partnering selectively to expand the reach and maximize the value of the platform technology and to bring in non dilutive capital that helps to fund internal development. This is a key component of our business strategy and an area where we've seen important recent progress. The collaboration with Janssen, which was executed toward the end of twenty eighteen for ARO HBV against chronic hepatitis B infection, included an option on three additional programs. During the previous quarter, Janssen delivered written notice of its intent to exercise its option right for the first of those programs, ARO J and J1. This earned ARO had a $10,000,000 option exercise fee and signals Janssen's intent to move forward with clinical studies.

Also during the quarter, we announced a global collaboration and license agreement with Horizon Therapeutics for ARO XDH, a previously undisclosed discovery stage candidate being developed by Arrowhead as a potential treatment for people with uncontrolled gout. Arrowhead received $40,000,000 as an upfront payment from Horizon and is eligible to receive up to $660,000,000 in potential development, regulatory and commercial milestones, and is further eligible to receive royalties in the low to mid teens range on net product sales. Horizon will receive a worldwide exclusive license to the therapeutic and will be wholly responsible for clinical development and commercialization. This is a great example of an attractive partnering opportunity. It expanded the reach of our technology intended to enter independently and brought in non dilutive capital.

It also brought in needed expertise in the gout field to help understand the disease, the clinical path, the tremendous unmet medical need, and a dominant player in the space with an existing commercial organization. For all these reasons, we thought Horizon was the ideal partner, and the deal made perfect sense for both of our companies. We look forward to working closely with Horizon as we advance this potential new therapy for patients in need. As you've heard, this was a busy quarter with lots of exciting events. However, drug development doesn't progress in a straight line, and invariably, are surprises.

Sometimes these surprises lead to leaps forward, such as the faster than expected liver healing in our ARO AAT program. And sometimes these surprises can be more unwelcome. We experienced the latter in the ARO ENaC program, our candidate being developed as a potential treatment for cystic fibrosis last quarter. To review, we voluntarily paused the clinical study of ARO ENaC after receiving a preliminary update from an ongoing chronic toxicology study in rats that contained unexpected signals of local lung inflammation. Because of this preliminary update, we instructed investigators to pause new screening, enrollment, and any further dosing of investigational ARO ENaC, pending additional data from the ongoing chronic rat toxicology study, and an additional ongoing chronic primate toxicology study.

We have not seen any concerning safety or tolerability signals in people enrolled in the ARO ENaC 1,001 study. However, we place the safety of patients that participate in our clinical trials above all else. So we will continue to keep the ARO ENaC clinical study on pause for now. We do not yet have full data back from the toxicology studies, nor from additional studies that we are conducting internally, so we do not yet know the extent of the findings. We are investigating this fully and are still in the information gathering stage.

We should know more in the coming weeks and months, and we intend to provide an update when we are able. With that overview, I'd now like to turn the call over to Doctor. Javier San Martin. Javier?

Speaker 3

Thank you, Chris, and good afternoon, everyone. I want to give an update on our clinical studies and provide details on the design of a couple of our newest studies. First, I will discuss ARO HIF2, which is designed to inhibit the production of HIF2 alpha to treat clear cell renal cell carcinoma or RCC. We were encouraged by the positive interim results from the first two cohorts of ARO HIF2 one thousand and one. A Phase 1b dose finding clinical study in three cohorts with advanced clear cell RCC.

We're currently enrolling cohort three, which is designed to include up to 10 patients who will receive a weekly IV infusion of ten fifty milligrams of ARO HIF2. The study is designed to evaluate the safety of ARO HIF2 to determine the recommended phase two dose and to assess pharmacokinetics and preliminary efficacy based on RECIST and post dose tumoral expression of his two alpha and his associated genes. Patients will continue to receive weekly ARO HIF2 indefinitely until they experience disease progression, have a complete response, or they discontinue. Our intention is to share additional interim data from this study, including data from cohort one, two, and initial results from cohort three at an appropriate medical meeting in the future. We have not yet selected the intended meeting.

The next program I want to detail is ARO HST, our investigational candidate for the potential treatment of alcohol and non alcohol related liver disease. Within the interim data we presented at ESOL was highly encouraging. And in fact, our presentation was highlighted in the ESOL official scientific press conference on NAFLD and NASH. It was exciting to see ALT levels drop significantly following just two doses of ARO HSD. We expected a high level of target gene no doubt because our TRiM system has been extraordinary consistent across our different liver directed programs.

But improvement in ALT at this early time point was very welcome surprise. This data and the strong genetic evidence of HSD17 beta 13 as a potential therapeutic target provide us with increased confidence as we design further clinical study for ARO HSD. We're thinking about innovative designs that seek to answer key questions about the medicine, the disease, and the mechanism of HSD17B3 inhibition. And what early signs of improvement may look like. We're approaching this in a similar way to how we approach ARO AAD.

In the meantime, we're still conducting the phase onetwo in patients with NASH or suspected NASH. And we're happy to report that the study is fully enrolled. As Chris mentioned, we start dosing in two Phase 2b studies of our cardiometabolic candidate ARO APOC3 and ARO ANG3 during the last quarter. I will give a brief description of these study designs, so you all can think through potential timing. We intend to initiate additional studies shortly and we will provide details on the design of the additional studies when they start.

For ARO APOC3, we initiated ARO APOC3 two thousand and one. A double blind placebo controlled Phase 2b study to evaluate efficacy and safety of ARO APOC3 in adults with severe hypertriglyceridemia or SHTG. Three dose level of ARO APOC3, ten milligrams, twenty five milligrams, and fifty milligrams will be evaluated against placebo in participants who have mean fasting triglycerides of greater than or equal to 500 milligrams per deciliter at screening. A total of approximately 300 participants will be enrolled in the study. All those cohorts will enroll in parallel with 100 participants per dose cohort randomly assigned in a three to one ratio to receive ARO APOC3 or placebo.

Each participant will receive subcutaneous injection on day one and week twelve. The duration of the study is approximately fifty four weeks for screening to the week forty eight end of study examination. The primary objective of the study is to evaluate the safety and efficacy of ARO APOC3 in adults with SHTG, and to select a dosing regimen for later stage clinical studies in this patient population. For ARO ANG3, we initiate ARO ANG3 two thousand and one, a double blind placebo controlled phase 2b study to evaluate the efficacy and safety of investigational ARO ANG3 in adults with mixed dyslipidemia. Three dose levels of AROH3, fifty milligrams, one hundred and two hundred milligrams will be evaluated against placebo in participant with mixed dyslipidemia who had the following screening.

LDL cholesterol greater than or equal to 70 milligrams per deciliter, or a non HDL cholesterol greater than or equal to 100 milligrams per deciliter. And mean fasting triglycerides between one hundred fifty and five hundred milligrams per deciliter. A total of approximately 180 participants will be enrolled in the study. All those cohorts will enroll in parallel with 60 participants per cohort randomly assigned in a three to one ratio to receive a subcutaneous injection of ARO ANG3 or placebo on day one and week 12. The duration of the study is approximately forty two weeks from screening to the week thirty six end of study examination.

After completing the week thirty six visit, participants will be eligible to continue in an open label extension study. The primary objective of the ARO ANG3 2,001 study is to evaluate the safety and efficacy of ARO ANG3 in adults with mixed dyslipidemia and select a dosing regimen for later stage clinical studies in this patient population. I will now turn the call over to Ken Myszkowski, Arrowhead's Chief Financial Officer. Ken?

Speaker 4

Thank you, Javier, and good afternoon, everyone. As we reported today, our net loss for the quarter ended 06/30/2021 was $29,900,000 or $0.29 per share based on 104,100,000.0 fully diluted weighted average shares outstanding. This compares with net loss of 13,600,000.0 or $0.13 per share and 101,800,000.0 fully diluted weighted average shares outstanding for the quarter ended 06/30/2020. Revenue for the quarter ended 06/30/2021 is 45,900,000.0 compared to 27,400,000.0 for the quarter ended 06/30/2020. Revenue in the current period primarily relates to the recognition of a portion of the $300,000,000 upfront payment received under our collaboration agreement with Takeda, as well as a $10,000,000 option exercise payment received from Janssen for the ARO JNJ-one program in May 2021.

Revenue for the Takeda agreement will be recognized as we continue to work toward completing our performance obligations of managing clinical trials in process and certain manufacturing related services. The remaining $230,000,000 of revenue associated with Takeda collaboration is anticipated to be recognized over approximately two years. Any additional milestones achieved with our collaboration partners would be additive to this projection. Revenue in the prior period primarily related to the recognition of a portion of the milestones received from our license and collaboration agreements with Janssen. Our performance and revenue recognition under the Janssen agreement for HBV is substantially complete.

Total operating expenses for the quarter ended 06/30/2021 were $77,800,000 compared to $43,300,000 for the quarter ended 06/30/2020. This increase is primarily due to increased candidate specific and discovery R and D costs as company's pipeline of clinical candidates has both increased and advanced. Net cash used by operating activities during the quarter ended 06/30/2021 was $29,600,000 compared with net cash used by operating activities of $33,400,000 during the quarter ended 06/30/2020. The key driver of this change was the $10,000,000 option exercise payment received from Janssen for ARO JNJ-one program in May 2021. Excluding any potential milestones from our collaboration partners, we estimate our cash burn run rate to be 50,000,000 to $60,000,000 per quarter.

Turning to the balance sheet, our cash and investments totaled $644,700,000 at 06/30/2021, compared to $453,000,000 at 09/30/2020. The increase in our cash and investments was primarily due to the upfront payment received from Takeda, offset by cash used by operating activities. In July, we also collected the $40,000,000 upfront payment due under our recent collaboration with Horizon. Our common shares outstanding at 06/30/2021 were 104,200,000.0. With that brief overview, I will now turn the call back to Chris.

Speaker 2

Thanks, Ken. As I mentioned, we think we're making strong progress across the spectrum of activities required to be a successful platform company. We are innovating on the platform, pushing the bounds of what our TRiM technology can do. We are rapidly and efficiently feeding the early stage pipeline with new candidates that may be engines of growth for Arrowhead in the future. We are moving our mid and later stage clinical programs progressively closer to our goal of bringing important new medicines to the patients who need them.

And lastly, we are selectively and responsibly using partnering and business development when it makes sense to do so. This last quarter saw important and tangible progress in all these areas. Thanks again for joining us today. I would now like to open the call to your questions. Operator?

Speaker 0

Thank you, Chris. Your first question comes from the line of Maury Raycroft from Jefferies. Your line is open.

Speaker 5

Thanks for taking my questions and congrats on the progress. I was wondering for the bottleneck for the CTA filings for DUX4 and the two pulmonary candidates, can you comment on whether this has anything to do with waiting for additional preclinical data for MENAK?

Speaker 2

It does not. It has to do with just finding slots at CROs. We talked about this, I think, a few conference calls ago, that since the pandemic, there's been a nonhuman primate shortage. And also, pulmonary, studies are a are a bit more difficult to do because there's not many CROs that do them. So given all that, we've just had a bit of a bottleneck.

And so we'll get these done. It's just that we're going to get them done a quarter or two later than we had hoped.

Speaker 5

Got it. Okay. And then also just wanted to check on if you're providing a status update on how the ENaC NHP study is going. And you mentioned you may know more in the next few weeks and months. Is it fair to assume that there could be an update on this in FORTU then?

Hi. This is Naina on for Alethia and thank you for taking our questions. We are wondering if you could share more on your DUX4 program and how it compares to competitors. And also if there's any read through from the Phase 2b results for losmapimod, which missed on the primary endpoint in change of DUX4.

Speaker 2

Yeah. So, so I'll let I'll let James comment on that. I don't I don't well, I'll let him comment on that. I don't know that there's read through, you know, with with the with the other one because it's different, you know, it's a different compound entirely, of course. But, James?

Speaker 7

Sure. Maybe I'll take the first question first about the, how we compare with the competing programs. There's not a whole lot out there, you know, with regards to the other oligo programs. The targeted antisense programs are all preclinical, and there's really not much data available. And and so the the primary difference would be the the way that we target the muscle cells that we use a peptide targeting ligand versus their antibody or antibody fragment approach.

So that's I think that's the main difference as far as comparing. And there's really no way to compare efficacy or knockdown levels as the other competing programs have not shared any data at this point. And then the other question was around the fulcrum read through. Is that right? Yeah.

It's it's, it's tough to say. I mean, it's a very different compound, different mechanism. I think they did highlight the, the challenges associated with a biopsy study in, in this population and with this specific target where there's this sort of stochastic expression of the target that that may be difficult to, to catch or to monitor, if you will, with biopsy. And so we will look at downstream gene expression, but we'll likely also look at other parameters that might help us select a dose for later stage clinical studies.

Speaker 5

Yeah, Javier. This is Javier.

Speaker 3

I wanted to add another comment about this data, which I think despite the biomarkers, the clinical data in some aspect was positive. So I think the target still is in a good place because if you look at the PLO and the physical function, there is a number of those that were statistically significant. We don't know how clinically relevant those changes is and we're looking at that to try to see if some of those changes correspond with the minimal relevant changes. And that I think will help us to understand this. So I think there is a mix of results here despite the biomarker now being positive.

But there is clinical signs of potential improvement in this patient population, which I think is crucial for the pathway.

Speaker 8

Okay, that's helpful. Thank you.

Speaker 2

Thank you.

Speaker 0

Thank you. Your next question comes from the line of Esfer Rizovelli from UBS. Your line is open.

Speaker 8

Hey, thank you for taking my question. I have two, one on ENaC. So it's historically been a tough target, but what are some takeaways from the tox signals that you're seeing? Is it specific to the lung or is there evidence of exposure in other tissues? And what would your considerations be if you find that the tox is limited to the lung?

Speaker 2

So so let me just say with two words, and I'll hand it over to to James on this. The the tox that we saw or that we heard about you know, again, we haven't had, you know, a final report on on this on this rat study yet. And so and so we have we have limited data, but but what we understand is that it was it was local lung inflammation. We don't we don't see I mean, we didn't see broader, issues. I we don't know if that's species specific because, as I said, we don't have, the NHP data yet.

We don't know if it if it is sequence specific or is target specific. There's you know, we're we we are really just starting to, you know, to, to get into this. And what

Speaker 7

was the other part of the question? Is

Speaker 8

Well, the other part of the question was if you sort of consistently see that the toxis when you get the NHP data, if you see the toxis limited to the lung, would it I mean how would you interpret that? Is that a good thing because you know the drug is getting to the lung and you just have to find another target that works maybe in a different indication? Or would you have to go back and change the chemistry?

Speaker 7

Speaker 12

Thanks for taking our question. This is Sonia on for Salveen. We were just wondering, like, beyond the pulmonary target and the muscle target, what other extrahepatic tissues would you be looking to go into on the forward?

Speaker 2

So we have active programs in a number of areas. We have not disclosed other areas that that that we need to go after or that we're working on. So, yeah, just stay tuned on that. Look. You know, we we have we have mentioned in the past, though, that that CNS clearly is a target rich environment, so it's a place that we wanna go at some point.

We are not there yet, but there's a number of of tissue types that we're looking at.

I will answer the last of those questions, and then I'll hand the rest over to James. So we do not have plans to seek a partner right now for this program. Look, that may change in the future, but right now we are happy to take this forward. You know, this is directly in our wheelhouse in terms of preclinical development. You know, this is hepatocyte directed construct.

We feel good about going to the clinic. And so let's see what the data look like, and then we can make a decision on partner versus non partner at some point in the future. James?

Speaker 7

Hey, sure. I'll take the first part of the question that I think was about C3 versus C5. So, you know, c three in the complement cascade is a central node that is involved in all three different components of that pathway, the lectin, the alternative, and the the classical pathways. So if you can inhibit c three, you can really take out everything that's downstream of of c three. And and so the effects should be broadly applicable to various complement mediated diseases.

Now specifically to two interesting indications, PNH and C3 glomerulopathy that Chris mentioned during the earlier remarks. PNH is a disease that's been reasonably well treated with C5 inhibition. However, there is a component of that population that is refractory to treatment due to extravascular hemolysis that's primarily driven by C3. So that residual that population with the residual anemia that's refractory to C5 inhibition could be specifically treated with, potentially treated with C3 inhibition. There is another population, the C3 glomerulopathy patients, where their disease is really driven by excess, C3 activity and deposition of C3 fragments in the glomeruli.

So that's really a C3 driven disease. Beyond those, there are other conditions that are, where the the disease is complement mediated, maybe not as specific to C3 as those other two conditions, but complement mediated. And we think that C3 inhibition may have, applicability in those other complement mediated diseases. So I I think that covers maybe both the first and the second question about c three versus c five as well as the other indications.

Speaker 1

One other question was about when when we can enter clinical development. By the end of the year. End of the year. Yeah.

Speaker 2

See. Or we'll be filing a CTA by the end of the year.

Speaker 13

Got it. That's helpful. And then just a a follow-up on on the gout program. Can you tell us where ARO XDH would fit in the gout treatment paradigm and the potential cadence of the $660,000,000 in potential milestones from Horizon? And to the extent that you could comment when the program could be expected to enter clinical development?

Speaker 2

We can't tell you too much about that, about any of those, actually. So the so we we we did not split out what the you know, how the $660,000,000 of potential milestone payments could be achieved. With respect to how this could fit into a into a clinical paradigm, you know, this is this is one of the reasons we chose Horizon as a partner. You know, this this is their business, and we'll be working closely with them. But, ultimately, this is their decision, and so I don't wanna step on their toes and and tell you, you know, something that we believe when when, when this is really gonna be their business.

And with respect to what you asked, when they're gonna get into the clinic, we don't know the answer to that. Still an early program. You know, we're we're just working on it right now. And so, you know, it's, we still have a ways to go.

Speaker 13

Got it. That's helpful. Thank you very much.

Speaker 2

Speaker 5

So excited for the back half.

Speaker 3

Thank you, Ted.

Speaker 0

Thank you. Your next question comes from the line of Keith MacKay from Sheridan. Your line is open.

Speaker 14

Yes, hi, thanks. Yes, Chris, just following up on the new lung programs. What are the similarities between the construct for those versus ENaC? I mean, obviously, you're going to have a different sequence for the targeted gene. But are you using the same targeting ligand?

So help us try to better understand what the potential read across of risk is from the ENaC tox.

Speaker 2

Right. So we're using the same targeting ligand. As you say, different sequences. I I would expect that we'll be using less material, in the in the next two because at least in in animal studies, they both appear to be more potent than ARO ENaC. Is that important?

I don't know. But but I believe that's that's that's well, I know that's the case for animal studies, and and we'll see if it translates into humans. And so it's again, you know, until we have more data, it's just too early to to speculate on how or if, you know, that what we saw in the CrocToks in rats may translate to other sequences.

Speaker 14

Okay, thanks for that. And then just for HIF, the biopsies that you received and the fact that some of them weren't usable, can you just further characterize that? And how do we think about the risk there going forward of not being able to get good data to do your assessments.

Speaker 7

James? Yeah, so far, well, I'll make one comment about the study design. The protocol allows us to enroll up to a sufficient number of patients to get, enough biopsies that we think are adequate paired biopsies to make to do our analyses. As was described in the press release, you know, the biopsy samples are not always analyzable. But so far in the first and second cohort and then and so far in the third as well, I mean, we've been able to get enough biopsy samples to do the work that that we need to.

Speaker 11

Hope that

Speaker 2

answers the question.

Speaker 14

Yes. Thank you.

Speaker 0

Your next question comes from the line of Mayank Mamtani from B. Riley. Your line is open.

Speaker 15

Hi. Good afternoon. This is Sawyer Kasme on for Mayank. Thanks for taking our questions. Maybe a brief one on on HIF two.

Could you provide any color on kind of how the enrollment's been tracking maybe in the context of the Merck program nearing nearing approval or just increased awareness on DHL disease associated with RCC?

Speaker 7

Yeah. Enrollment has been, actually really good in that program throughout. We've not seen any challenges with enrollment, and all the slots have filled very rapidly. I know that the Merck study is ongoing, but it has not detracted from enrollment into this study.

Speaker 15

Great. And then maybe on, HBV, do you have any insight into kind of what forum J and J might present the twenty four week off treatment data from Reef? And or any high level thoughts on on kind of what we can incrementally learn from that study?

Speaker 1

Boy.

Speaker 2

No. I can't give you any guidance on that. Look, we look forward to seeing those data, but I don't know what their plans are, to be honest, about where that could be presented.

Speaker 15

Got it. Fair enough. Thanks for taking our questions, and congrats on the progress.

Speaker 2

Thank you.

Speaker 0

Thank you. Your next question comes from the line of Mani Foroohar from SVB Leerink. Your line is open.

Speaker 11

Hey. Good afternoon. This is Rick on the line for Mani. Thanks for taking our questions. Just two from us.

Speaker 13

So first, for for HIC two, could you speak to some

Speaker 11

of the variability of knockdown seen in the data? I know there aren't a lot of data sets exploring RNAi in tumors. So could some of this variability just be due to the heterogeneity of tumors in general? Or is it something that could potentially be resolved by looking at higher doses or either earlier lines of patients?

Speaker 7

Yes. I think that that you hit the the nail on the head. I mean, I think there's heterogeneity of of expression in the in the tumors and across from patient to patient and and also, you know, heterogeneity in between impaired biopsies. You're not necessarily getting into the same area of the tumor. So heterogeneity is definitely an issue and probably explains a good component of the variability.

Speaker 11

All right. Got it. All right. Thanks. I also have a much more broad question.

So just in general, Arrowhead's approach to extrahepatic delivery seems to be focused around targeting integrins with specific ligand conjugates. Could you maybe speak to why these, are so favorable to target as a class of molecules? And if the company is currently exploring any other targeting strategies preclinically?

Speaker 2

Arrowhead Pharmaceuticals - Earnings Call - Q3 2021

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