Arcturus Therapeutics Holdings Inc. (NASDAQ:ARCT) Q2 2023 Earnings Call Transcript August 7, 2023
Operator: Greetings, and welcome to Arcturus Therapeutics Second Quarter 2023 Earnings Call. At this time, all participants are in a listen-only mode. A brief question-and-answer session will follow the formal presentation. [Operator Instructions] As a reminder, this conference is being recorded. It is now my pleasure to introduce your host Neda Safarzadeh, Vice President, Head of Investor Relations, Public Relations, and Marketing. Please go ahead.
Neda Safarzadeh: Thank you. operator. Good afternoon, and welcome to Arcturus Therapeutics Second Quarter 2023 Financial Update and Pipeline Progress Call. Today’s call will be led by Joseph Payne, our President and CEO; and Andy Sassine, our CFO. Dr. Pad Chivukula, our CSO and COO will join them for the Q&A session. Before we begin, I would like to remind everyone that the statements made during this call regarding matters that are not historical facts are forward-looking statements within the Safe Harbor provisions of the Private Securities Litigation Reform Act of 1995. Forward-looking statements are not guarantees of performance. They involve known and unknown risks, uncertainties, and assumptions that may cause actual results, performance, and achievements to differ materially from those expressed or implied by the statements.
Please see the forward-looking statement disclaimer on the company’s press release issued earlier today, as well as the risk factors section in our most recent Form 10-K and in subsequent filings with the SEC. In addition, any forward-looking statements represent our view only as of the date such statements are made. Arcturus specifically disclaims any obligation to update such statements to reflect further information, events, or circumstances. And with that, I will now turn the call over to Joe.
Joseph Payne: Thank you, Neda. It’s good to be with you again, everybody. We look forward to providing our updates today on our quarterly investor call. I will begin my remarks by highlighting our progress with our ARCT-154 COVID-19 vaccine Phase 3 program. We’re pleased with the rapid development and regulatory process — progress recently made with our alliance partner Meiji Pharma toward the approval of ARCT-154 by the Japanese regulatory authorities. The ARCT-154 submission is supported by an active-controlled Phase 3 booster vaccine study that was executed during a period when multiple COVID variants were circulating. Initial ARCT-154 Phase 3 booster study results were released as pre-print last month in Med Archive. The study achieved its primary endpoint, demonstrating non-inferiority of neutralizing antibody response against the SARS-CoV-2 ancestral strain when compared to Comirnaty.
The study also demonstrated superiority of ARCT-154 in neutralizing antibody response against the Omicron BA.4/5 variant as a key secondary endpoint. The results of this trial indicate increased immunogenicity associated with ARCT-154 at 28 days following booster administration. For the ancestral strain, the geometric mean ratio of neutralizing antibodies between ARCT-154 and Comirnaty was 1.43-fold indicating elevated neutralizing antibodies against the vaccine strain versus the comparator. Based on available Phase 3 clinical data at the time of interim analysis, ARCT-154 continues to demonstrate a favorable safety and tolerability profile with no additional safety concerns identified. In today’s earnings release, we also included new ARCT-154 Phase 1/2 clinical study data, which suggested durable immune response up to one year following booster administration notably neutralizing antibody levels remained greater than 10-fold above baseline across a panel of variants including Omicron during the one-year observation — and this is during the entire one-year observation period.
In summary, ARCT-154 has shown broad neutralizing capability against multiple variants of concern and has the potential to offer not only effective, but also a longer-lasting immune response that may suggest durable protection against COVID-19. We’re very pleased with the ARCT-154 clinical data and now believe that this next-generation self-amplifying mRNA platform is meaningfully different than conventional currently approved mRNA vaccines. I will note that the ARCT-154 dose is very much lower. In our head-to-head study, ARCT-154 was dosed at only five micrograms. This is an 83.3% lower dose than Comirnaty and at least 90% lower than other approved mRNA vaccines. As previously reported, in April Meiji submitted a new drug application in Japan to support potential initial approval of ARCT-154 as a primary immunization vaccine, and in June, we were pleased to hear that Meiji filed the NDA for the booster and included the relevant data to support that booster application.
The review process with the PMDA is ongoing with Japanese NDA approval being our next targeted milestone. A positive PMDA decision would represent Arcturus’ first product approval a tremendous achievement for our company. And approval or unapproval along with the promising data that we’ve collected is indicative of the broader opportunity for Arcturus’ mRNA technology platform. I’ll now move on to provide an update on ARCT-810. This is our messenger RNA therapeutic candidate for ornithine transcarbamylase or OTC deficiency. This investigational medicine is designed to functionally replace the deficient OTC enzyme in the liver and thereby restore urea cycle activity and prevent metabolic crises that cause neurological damage. ARCT-810 could potentially reduce the need for ammonia scavengers and ease the rigid dietary protein restrictions that OTC patients face today, thus improving quality of life for those living with this disease.
In June, we announced that the FDA had granted ARCT-810 with Fast Track designation. The company has also recently received Rare Pediatric Disease Designation from the FDA for ARCT-810. Rare Pediatric Disease designation is designed to recognize those rare diseases in children in which serious or life-threatening manifestations primarily affecting patients from birth to 18-years of age. Now, due to this designation, if ARCT-810 achieves approval for a pediatric indication, Arcturus will receive a voucher for priority review of a subsequent marketing application for a different product. ARCT-810 is currently being evaluated in two ongoing clinical studies in patients. A Phase 1b study in adults and a multi-dose Phase 2 study in adolescents and adults with OTC deficiency.
The Phase 1b single ascending dose study is being conducted in the United States and has completed dosing of all planned cohorts in a total of 16 subjects. The ARCT-810 Phase 2 study is being conducted in the United Kingdom and Europe and plans to enroll up to 24 adolescents and adults with OTC deficiency. The ongoing study is evaluating two dose levels and includes up to six by-weekly administrations for each participant. We expect to share interim data on biological activity from a subset of patients in the coming months. Now, I’ll move on to ARCT-032. This is our inhaled messenger RNA-therapeutic for cystic fibrosis. This program is designed to express fully functional CFTR protein in the lungs of individuals with CF, utilizing our LUNAR delivery technology that has been highly optimized for inhaled delivery to the lungs.
Our approach is agnostic to the underlying mutations associated with the disease. And as a result, this program could provide clinical benefit across a wide range of those living with CF, including those that are not well served by currently approved CFTR modulators. In June, at the European CF Society Conference in Vienna in collaboration with the University of Alabama Birmingham lab, we reported promising data demonstrating that ARCT-032 fully restore CFTR expression and function in vitro and bronchial epithelial cells from CF donors. In the past, improvement in chloride transport in these human bronchial epithelial cells treated with CFTR modulators has been associated with improved clinical outcomes. In the ARCT-032 clinical development program continues to advance according to plan.
We’re pleased to report today the successful completion of dosing in our Phase 1 study. The study includes 32 healthy participants, including eight subjects in each of four dose cohorts being tested. We look forward to reporting interim safety and tolerability study results later this year. We received regulatory approval of a protocol amendment to allow the transition to a Phase 1b clinical study of ARCT-032 in up to eight cystic fibrosis patients. The study will be conducted in New Zealand and continuing to advance this important investigational medicine. Our strategic collaboration with CSL Seqirus and this is Arcturus’ exclusive global licensee is focused on the development and commercialization of next-generation mRNA vaccines and continues to make strong progress.
Our Lunar-Flu program, for example, continues to progress with funding and operational support from CSL Seqirus. Lunar-Flu utilizes Arcturus’ validated next-generation STARR mRNA platform. And with that, I will now pass the call to Andy.
Andy Sassine: Thank you, Joe, and good afternoon, everyone. The press release issued earlier today includes financial statements for the second quarter and six months ended June 2023 and provides a summary and analysis of year-over-year financial results. Please also reference our most recent Form 10-Q for more details on the financial performance. We are very pleased with the ARCT-154 new drug application to the PMDA in Japan and we believe that this product could represent an improved vaccine option for patients, as well as an important source of potential future revenues for our organization. Furthermore, the development and manufacturing plans supporting ARCT-154 was carried out in a financially disciplined and efficient manner.
I will remind you that the Phase 3 Japanese booster study, as well as product manufacturing-related to this collaboration are being funded by Meiji Seika Pharma and the Japanese government. Also, in April Meiji Seika Pharma entered into an agreement with CSL Seqirus whereby Meiji will be responsible for the regulatory approval, marketing, distribution, and sales of ARCT-154 in Japan, as well as coordinating manufacturing of COVID vaccine products with ARCALIS for the Japanese market. We are thrilled to announce the completion of a state-of-the-art mRNA drug substance manufacturing facility in Japan with our partner ARCALIS. A team of delegates from Arcturus led by our senior executives and scientific team attended the grand opening ceremony of the cutting-edge cGMP facility in Tokyo, Japan this past week.
The ceremony with the celebration of collaboration and partnership as Arcturus joined forces with Japanese healthcare leaders and senior government officials to inaugurate the first mRNA manufacturing facility in Japan. Located in a strategic hub for biomedical research and development, ARCALIS is poised to become a key player in the global mRNA drug manufacturing landscape. ARCALIS’ new plant meet current good manufacturing practice and is equipped with the world’s most advanced manufacturing control and quality control system to efficiently manufacture high-quality substance for mRNA Pharmaceuticals. In April 2023, we received an advanced payment of $23.6 million for the manufacturing and supply of ARCT-154 booster vaccines from CSL. The advanced payment is for specified manufacturing runs of ARCT-154, which includes the drug substance as well as the reservation fees and related manufacturing requirements.
As Joe mentioned, the Lunar-flu program continues to progress with funding and operational support from CSL and additional updates will be provided soon. I will now provide a summary of our financial results for the second quarter of 2023. Our primary source of revenues were from license fees, consulting. and related technology transfer fees, reservation fees, and collective collaborative payments received from research and development arrangements with pharmaceutical and biotechnology partners. With the three months ended June 30, 2023, we reported revenues of $10.5 million compared with $27.1 million for the three months ended June 30, 2022. The decrease was primarily attributable to a decrease in revenues of $12.7 million related to the termination of the agreement with Vinbiocare and a decrease in revenues of $12.5 million related to the agreement with the Israeli Ministry of Health.
The decrease was primarily offset by an increase in revenue of $8.6 million related to the collaboration agreement with CSL and the grant agreement with BARDA, which were both executed in the second half of 2020. Revenue increased by $58.5 million during the six months ended June 30, 2023, compared to the prior year period. The increase was primarily attributable to an increase in revenue of $87.6 million related to the collaboration agreement with CSL Seqirus and the grant agreement with BARDA. Total operating expenses for the three months ended June 30, 2023, was $65.9 million compared with $49.2 million for the three months ended June 30, 2022. Total operating expenses for the six months ended June 30, 2023, were $131.4 million compared with $104.8 million for the six months ended June 30, 2022.
Our research and development expenses consist primarily of external manufacturing costs, in vivo research studies, and clinical trials performed by contract research organization, clinical and regulatory consultants, personnel-related expenses, facility-related expenses, and laboratory supplies related to conducting R&D activities. R&D expenses were $52.7 million for the three months ended June 30, 2023, compared with $38.2 million in the comparable period last year. Primarily reflecting increased clinical research and manufacturing costs of $11.4 million and an increase of $2.9 million in personnel-related expenses. R&D expenses were $104.4 million for the six months ended June 30, 2023, compared with $83.1 million in the comparable period last year, primarily reflecting increased manufacturing and personnel costs.
General and administrative expenses primarily consist of salaries and related benefits of our executive administrative legal and accounting functions and professional service fees for legal and accounting services, as well as other general and administrative expenses. G&A expenses were $13.2 million and $27 million for the three and six months ended June 30, 2023 respectively, compared with $11 million and $21.7 million in the comparable period last year. The increases resulted primarily from personnel expenses due to increased headcount and salaries, increased travel and consulting expenses, as well as an increased rent expense associated with the new headquarters facility. For the three months ended June 30, 2023, Arcturus reported a net loss of approximately $52.6 million or $1.98 per diluted share, compared with a net loss of $21.6 million or $0.82 per diluted share in the three months ended June 30, 2022.
For the six months ended June 30, 2023, Arcturus reported a net loss of approximately $1.8 million or $0.07 per diluted share, compared with a net loss of $72.7 million, or $2.75 per diluted share in the six months ended June 30, 2022. Cash and cash equivalents and restricted cash were $380.6 million as of June 30, 2023, and $394 million on December 31, 2022. We have collected approximately $300 million in upfront payments and milestones from CSL as of June 30, 2023. Additionally, in the second quarter, we received $23.6 million under the manufacturing and supply of ARCT-154 from CSL. We expect to continue receiving future milestone payments from CSL that will support the ongoing development of the Covid and Flu programs. Finally, I am happy to report the cash runway remains extended through the beginning of 2026 based on the current pipeline and programs.
In summary, we believe the company remains in a strong financial position and has the resources needed to achieve multiple near-term value-creating milestones for the vaccine and therapeutic programs. Furthermore, with the anticipated ARCT-154 product approval later this year in Japan, we look forward to beginning to report potential commercial sales in the next few years. I will now pass the call back to Joe.
Joseph Payne: Hey, thanks, Andy. We’ve continued to make excellent progress and advanced our proprietary messenger RNA, and lunar delivery platform technologies toward later stages of clinical development. It was great to hear the progress of our catalyze and our partner there on the manufacturing facility in Japan and we are especially excited about the progress toward our first product approval potentially later this year with ARCT-154, the achievement would definitely mark a critical milestone for the platform and for Arcturus. So with that, I’d like to turn the time over to the operator for questions.
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Q&A Session
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Operator: Thank you. We will now be conducting a question-and-answer session. [Operator Instructions] Our first question comes from Yasmeen Rahimi with Piper Sandler. Please go ahead.
Yasmeen Rahimi: Good afternoon, team and congrats on all the updates, especially on the manufacturing facility. Team, could you maybe provide some color in terms of the timing of the approval in Japan and if that’s still set for the fall? Second, maybe you could also provide us some thoughts around manufacturing capacity. Would you be able to, by the time you receive approval in Japan, to facilitate and produce over 70 million doses if needed? And then the third question is on the [Technical Difficulty] program. Are you planning to share the single ascending data? Could you comment how high you ended dosing? And then lastly, what are the doses you’re moving forward into the math portion? I’ll jump back into the queue, and my apologies for so many questions.
Joseph Payne: Sure. Well, with respect to the first question on approval timeline, I can address that. You can appreciate that the review process is ongoing with the PMDA, whether it’s CMC in non-clin and clinical package insert risk management plan questions, right? These are all standard and we’re going through this ongoing process with PMDA. So it means that we remain on track for later this year with respect to approval. With respect to capacity, I’m going to turn the time to Andy to address that.
Andy Sassine: Thanks, Yasmeen. With respect to capacity in Japan, we’ve clearly indicated that with the factory will not be operational in producing until next year, and furthermore, we will defer those kind of questions to our partner ARCALIS and Meiji in Japan and CSL as well. So hopefully you can appreciate they’re in control of the commercial program here and if license out our ARCT-154 in future COVID products. So we’re going to have to rely on and depend on them for guidance with respect to capacity, but I’m sure they’ll provide it when the time is appropriate.
Joseph Payne: And to address your final question about CF. We have not, and by intention, not disclosed any of the dose levels that we’ve evaluated given that the environment is competitive, but I can share with you that each patient will receive two doses in the Phase 1b amendment. So up to eight CF patients and each will receive two doses, but the specific dose level, we’re not disclosing at this time.
Yasmeen Rahimi: Okay, great. And I’ll jump back into the queue.
Joseph Payne: Thanks, Yas.
Operator: Next question comes from Myles Minter with William Blair. Please go ahead.
Myles Minter: Hey, everyone. Congrats on the booster data as well. Nice to see that. Just on 154, if you do receive approval by year-end in Japan, do you think you’ve got the right strain in there to potentially deliver some doses in this current vaccination season? I just know one of your peers out there, Daiichi, and they got approval and then clearly stated that they will be switching to the next — they based trying to supply the current period. So that’s the first question.
Joseph Payne: Yes. Myles, thanks for joining the call. It’s good to hear you. You’re absolutely right. All the regulatory agencies including PMDA are evaluating all the variants of interest in a particular region. In this case, Japan, and Arcturus is prepared to address whatever they request. So right now, you’ve seen the profile of ARCT-154 and it’s broadly acting against a variety of variants. But if it’s deemed by the PMDA for whatever reason to proceed with another variant of interest, whether that’s XBB or something else, we’re prepared to immediately respond and we’re positioning the company strategically to do so, okay, with CSL and Meiji involved in this process.
Myles Minter: Okay. And then the second question is just on duration. Thanks for supplying that Phase 1, 2 data. We’re going to see duration of immunogenicity out of the Phase 3 booster trial and what are your sort of predictions on the commonality neutralizing antibodies sort of as we get into the 6-month to 12-month period ahead of that trial?
Joseph Payne: Yes. I’d appreciate the question. Clearly, this data we shared today is very exciting and it’s very promising. We’re happy to see just a really strong durability signal from ARCT-154, it’s a good representation of this next-generation self-amplifying mRNA platform. It’s clearly different. So with respect to the Phase 3 dataset, we intend to share that data for the six-month time point later this year. And we will be more than happy to share that at that time.
Myles Minter: Hey, cool. Thanks for the questions.
Joseph Payne: Yes. Thanks, Myles.
Operator: Next question comes from Seamus Fernandez with Guggenheim Securities. Please go ahead.
Evan Wang: Hey guys, this is Evan Wang on for Seamus. I have two questions. First on COVID. Just wondering if you could share some color on the Japanese COVID market. So you’re trying to figure out some of the opportunity for ’23, ’24, particularly with I believe first 25 million vaccine purchase from Japan. And the expectations for additional orders. Second on OTC. Wondering if you can provide enrollment update there and what we can expect from the update later this year? Will that be specific to 810 or should we expect a broader update as well? Thank you.
Joseph Payne: All right. So your first question is with respect to the opportunity for vaccine purchases in Japan. right? I guess I’ll turn that over to Andy. Do you want to address that?
Andy Sassine: Yes. I think we obviously are very excited that the Japanese government continues to purchase the vaccines, the COVID-related vaccine for its population. And historically they purchased about 80 million vaccines as of the last 12 months that we have record from the Japanese government. So certainly, the future orders that we’re currently seeing and anticipating are certainly a testament to their concern about COVID during an endemic phase here and certainly, the approval of Daiichi in Japan for a conventional mRNA vaccine made in Japan is certainly viewed as a very favorable here for not only Arcturus but our partners Meiji and CSL, because the Japanese government is very committed to ensuring that in the future Japan will be vertically integrated and completely independent of any future manufacturers for any related pandemic type of viruses.
And I think that’s pretty exciting that the government has taken on this initiative to be self-sufficient and hopefully, we can be a part of it and we’ll certainly learn more soon. But with respect to specific orders, we really cannot provide that at this time, it will certainly be developed and articulated by Meiji and CSL.
Joseph Payne: And then with respect to your second question on ARCT-810 enrollment, I think we haven’t provided specific guidance there but we encourage people to look to other rare liver disease companies on the pace of their enrollment as a basic guide as to what to anticipate.
Evan Wang: So we have finished the enrollment of the Phase 1b portion of the trial and as Joe mentioned in his remarks that we intend to share some data around the 810 later on in the coming months.
Joseph Payne: Yes. Thanks, Evan.
Operator: Next question comes from Pete Stavropoulos with Cantor Fitzgerald. Please go ahead.
Pete Stavropoulos: Hi, Joe, Andy, and team. Thank you for taking my questions. Congratulations on all the progress and the booster data presented in MET-Rx. It was nice to see the non-inferiority and superiority in neutralizing capabilities compared to an approved vaccine. So our first question regarding the manufacturing capabilities in Japan. Can you potentially leverage them for outside Japan with 154 and possibly other future candidates or will the facility be strictly focused on COVID-vaccine?
Joseph Payne: Absolutely. Peter, that’s a really good question, and thanks for being on the call. We anticipate that our callous will become a full-fledged mRNA facility with not only the capability of drug substance and drug product but certainly going to be a world-class facility for any type of mRNA capability going forward. So it’s up to our callous to announce all the specifics with respect to their capability and I’ll leave it up to them, but they do have an exciting future, and we’re a part of it and certainly we’ll have more details with our partner as soon as it becomes available.
Pete Stavropoulos: All right, thanks. And now for 032, I know that you have fully enrolled the Phase 1 in terms of healthy volunteers. And I know the focus is safety and tolerability. But now that you’re expanding the patient population, what are some of the ways that you may evaluate the pharmacodynamic response?
Joseph Payne: Yes. There is — we’re going to be looking primarily at safety and tolerability in patients. I know we’re very pleased with the results so far that we’ve seen in Phase 1 in healthy volunteers. This was the first time anyone has inhaled lunar technology and so now that we transitioned to patients in Phase 1b, that is the primary objective here because we have a stellar preclinical dataset of really positive data, so we just want to first see safety and tolerability in this Phase 1b set of patients. Having said that, we are positioning ourselves to evaluate LCI or Lung Clearance Index, and this is a sensitive measure of lung function, so we will look to see if after two doses if we can see something, but the primary objective here is just to establish safety and tolerability in patients.
Pete Stavropoulos: All right. And thank you for that. And the last question is, I know you gave a brief sort of update on enrollment and to look other programs. But have you activated all the sites, and if not, how many more can you potentially activate to help enrollment move along?
Joseph Payne: We are essentially at capacity with respect to activating sites. Our team has been traveling through Europe and following up with all the principal investigators in this manner. So we’re working hard to enroll patients and that’s the guidance we’ve provided and that we remain consistent on providing some data later this year or in the coming months.
Pete Stavropoulos: All right. Thank you very much for taking my questions and congrats on the progress once again.
Joseph Payne: Yes. Thanks, Pete.
Operator: Next question comes from Yanan Zhu with Wells Fargo. Please go ahead.
Yanan Zhu: Hi, thanks for taking my questions, and congrats on the progress. I wanted to get maybe a little more clarity on what might happen after a potential Japan approval. So I think Daiichi’s decision at least looking at the news release is by itself and it doesn’t look like the PMDA instructed it not to supply the market this original strain vaccine. So I was wondering what is your and your partners thinking. Once you receive the approval, what’s the thinking process in terms of whether to supply the market and if you do supply the market, I was wondering who is the manufacturer, is that your facility or the Arcalis facility?
Andy Sassine: Well, with respect to commercial guidance — with respect to the second, obviously. Thanks for the question, Yanan, but certainly our current manufacturing partners which represents Catalent and Aldevron in the U.S. and Recipharm in Europe would be the suppliers of any current supply. As you know, we’ve articulated the Japan facility won’t come online until next year. So any kind of orders for Japan from that facility, probably will not be until next year late or the year after, so hopefully you can appreciate that we have a dual process in place to be able to provide the Japanese market with our vaccine as soon as possible. And certainly, once the factory is up and running in Japan they’ll be able to supply going forward. Hopefully, that helps clarify that situation and Joe can address the first part of the question.
Joseph Payne: Yes. With respect to the other vaccine or vaccines getting approved in Japan, we’re very happy to see that Japan is following their domestic strategic plan. We touched on this earlier in the call a little bit. We view this very positive because we feel like we’re part of this domestic plan with Meiji and CSL but our — what sets this vaccine technology apart from all other conventional mRNA vaccines that have been approved or soon to be approved is our dose level. So our dose level is significantly lower, our CR response rates that we’ve observed seemed to be differentiating. Clearly, people have to be taking this dose level into consideration when it comes to safety and reactogenicity as potentially differentiating.
And then finally, the data we showed today, the durability data is very promising. So — and can set this technology apart. So as we work with Japan in their strategy, we definitely see a way to fit in line with their objectives to address some of the key issues in protecting their people with a vaccine strategy.
Yanan Zhu: Got it. Thanks for the color. And you touched on durability, congrats on the data. I was wondering, can you talk about the underlying biological basis for this durability and your confidence that we could see this observation replicated in the longer follow-up for the Japan study?
Joseph Payne: Yes, it’s great question. Self-amplifying mRNA is providing very encouraging durability data and your question is why. And it’s because the mechanism of how this — the self-amplifying mRNA molecules make the antigen. Conventional mRNA make the antigen for a period of time and then degrades, right? But self-amplifying mRNA, this next-generation mRNA technology extends the duration of making that antigen. So the body sees the antigen for a longer period of time. That means it is allowed to increase the antibody titer levels and that’s what we’ve seen in the Phase 3 comparison study and we’ve all — because the body sees the antigen for a longer period of time, it allows a broader spectrum of antibodies to be made.
And when you combine those two features of increased antibody titers with a broader spectrum of antibodies being created by the body, this translates into a longer-lasting vaccine and that would provide an explanation as to explaining what, and why we’re seeing what we’re seeing.
Yanan Zhu: Got it. So we might — we should be able to see something similar with the Japan study, correct?
Joseph Payne: Yes. Correct, correct. That’s what you would expect. And remember, previously we’ve seen in our Phase 1 and Phase 2 studies that the antibodies titer levels tend to increase beyond one month or beyond four weeks. So will we see that as well in Phase 3 is yet to be understood. But, yes, our expectations are high and very optimistic.
Yanan Zhu: Got it. Thanks for the color. And lastly on the OTC deficiency program. I was wondering in the news release, you mentioned you may announce data from a subset of the patients. I was wondering, could we expect one or both cohorts of the patients data being reported out and what type of changes clinically or in terms of biomarkers can be expected with a roughly a three-month duration? And lastly, would you be able to comment on any next steps that we can expect once you have reported the data? Thanks.
Joseph Payne: Well, I appreciate the question and wanting to understand additional detail on different dose levels in the OTC clinical trial. But the only guidance we’re providing today is some biological proof of concept or some biological data that will provide in a subset of patients. So I can’t provide any more detail than that. With respect to any biomarkers that we’re tracking, we will be tracking them for an extended period of time. And that includes ammonia and urea genesis and other amino acids and it can be such as glutamate, for example, can be measured but several amino acids are impacted by the urea cycle and OTC itself can be measured. The Ornithine Transcarbamylase Enzyme that’s built or expressed in these liver cells, these lever cells just as you are aware can be swept off into the circulation and measured in the plasma. And so we can track OTC levels as well and over an extended period of time.
Yanan Zhu: Got it. Thanks for all the color.
Joseph Payne: Thank you, Yanan. Good to hear.
Operator: Next question comes from Yigal Nochomovitz with Citi. Please go ahead.
Carly Kenselaar: Hi, this is Carly on for Yigal. Thanks for taking our questions. First, just curious if there’s anything more you can say about CSL’s progress on the seasonal flu vaccine. And if that work has maybe accelerated after the COVID data, do you have a sense for timelines for potentially bringing the flu candidate into the clinic?
Joseph Payne: Well, I can provide one comment, you’re absolutely right that the Meiji, CSL, and Arcturus teams are all united in the excitement over this recent dataset and that excitement bleeds into other programs. Of course, it gives us more energy and more ambition and bigger in other programs, and so your question about the flu is appropriate. We have to be very careful. It’s — I would consider even though we’re working closely with CSL, it is their program and their program to guide on. So it’s very difficult for us to just give a candid response to your question on guidance. Having said that, we look forward to continuously update the market because this is an active program for us. We’ve reported milestones on this previously this year, and clearly, this is a program of high interest for CSL. Andy, anything to add?
Andy Sassine: Yes, in my comments I obviously said that we will have updates provided soon, so stay tuned. Thank you.
Joseph Payne: Yes.
Carly Kenselaar: Okay, got it. That’s helpful. And then just on OTC and MCF, I know that the ongoing Phase 2 and OTC is active in the UK and Europe. And then you’re also recruiting in New Zealand for the CF program. Just curious, any comments on potential timelines and plans for opening sites in the U.S. for those studies? Thank you.
Joseph Payne: Well, we already have an active trial ongoing for COVID in the vaccine enterprise in the U.S. already. So we already have an active effort in the United States. And for OTC, we have an active effort in the U.S. with our Phase 1b trial in patients. With respect to CF, you can see that we have a very strong relationship with the CF Foundation, and they have considerable oversight and influence on the U.S. area and not just globally.
Joseph Payne: But we haven’t indicated any guidance as to when we will be conducting any clinical trial efforts in CF in U.S. There’ll be an appropriate time to do so but today is not that.
Carly Kenselaar: Okay, got it. Great. Thank you very much for taking our questions.
Joseph Payne: Thanks, Carly.
Operator: Next question comes from Ed Arce with H.C. Wainwright. Please go ahead.
Thomas Yip: Hi, good afternoon, everyone. This is Thomas Yip asking a couple of questions for Ed. Congrats. Congratulations on all the progress with Meiji in Japan. So first perhaps looking a little bit into the future, do you have any plans right now to expand 154’s use in populations beyond as dose in Japan? And if so what can investors think about the estimated timeline?
Joseph Payne: Yes, the short answer is yes. There’s a lot of activities. We’d like to expand because our Phase 3 trial was in adults, right? So there’s more than just adults and in Japan and CSL has a definite and Meiji has a clear interest in expanding the commercial opportunity beyond adults. So — but I can’t give specific guidance on that, that’s there’s to provide. But outside of Japan, CSL is our exclusive partner for distribution and commercialization in US and Europe, for example. So maybe looking to them to provide guidance on those efforts.
Thomas Yip: Got it. Perhaps just one more question from us regarding 032 with the CF, our interests on this and the OTC program clearly. Perhaps for the Phase 1 study, when can we expect the first CF patients to be enrolled into the study? I know you just received clearance and also what — when can we expect the initial dataset with CF patients?
Joseph Payne: Well, we’ve conservatively guided the initiation of enrollment in the second half of this year and we will allow that to unfold. And then with respect to data, that will be at a later time point. I think we’re focused on the near-term objective of enrolling — initiating enrollment for these up to eight CF patients in New Zealand in the second half of this year. With respect to interim Phase 1 safety data, interim Phase 1 safety data is also expected later this year.
Thomas Yip: Okay, got it. Looking forward to those data along with the COVID regulatory status in Japan as well. Thank you again for taking the questions.
Joseph Payne: Yes. Thanks, Thomas.
Operator: Next question comes from Yale Jen with Laidlaw and Company. Please go ahead.
Yale Jen: Good afternoon, and thanks for taking the questions. and congrats on all the progress in Japan at this moment. Appreciate the data you provided today in terms of the — both the duration, as well as the breadth of the vaccine [Indiscernible] it covers. My question to you is that, does this have any read-through in terms of the application in Japan in terms of cover broader across strength? Then I have another follow-up question.
Joseph Payne: Yes. It’s good question. The data we share today was only using a validated assay. The new strains that are coming forward are only exploratory in nature and not validated yet, so we’ve remained consistent on sharing data that’s only validated assays, right? So there’ll be no time and a place to provide that data once the assays are validated is the answer.
Yale Jen: Would that referring — you mentioned earlier that you might report six-month data in the future times so maybe later this year. Are these two connected in anyway?
Joseph Payne: If you’re referring to the Phase 3 Japanese comparator study, yes, we’re guiding that we’ll be able to share six-month durability data later this year. Correct.
Pad Chivukula: And hi, this is Pad. And I just want to make sure that you understand, we are an mRNA platform company and because of that we get to update our vaccine readily. So if there is a new strain that emerges, we can of course update our vaccine and because the platform will be approved, we can quickly commercialize that as well. And our manufacturing process is very similar to a lot of the other mRNA players.
Joseph Payne: Keep in mind that with the trial being completed in February you don’t really have the six month completion of the data until August. So by the time they collect it and analyze it, you have to give us a few months for that. So hopefully that gives you some kind of runway to understand when conceivably the six-month data could even be presented. Hopefully, it will be probably a fourth-quarter event, if you can appreciate that. Does that makes sense?
Yale Jen: Absolutely. And really appreciate the colors. And one follow-up question here. It is in terms of the 032 in the CF. In your press release you mentioned that there was some amendment being tested in Florida or being suggested for the Phase 1b study. Any colors in terms of what specific amendment has been placed?
Pad Chivukula: Yes. The amendment is in our Phase 1 was in healthy volunteers. And what we talked about was in Joe’s comments that there has been an amendment that was filed and it was recently approved to include patients in the study.
Yale Jen: So, therefore, just adding the patient versus the healthy volunteers?
Pad Chivukula: That’s right.
Yale Jen: Okay, great. Thanks a lot. Again congrats.
Joseph Payne: Yes. Thank you, Yale.
Operator: That was all the time we have for today. I would like to turn the floor back over to Joe for closing comments.
Joseph Payne: Okay. Thanks for participating on the call today, everyone. If there’s remaining questions, please reach out to the team and we’ll get back to you right away. Good night.
Operator: This concludes today’s teleconference. You may disconnect your lines at this time. Thank you for your participation and have a great day.