Good morning, and welcome to the Ocular Therapeutix Fourth Quarter 2024 Earnings Conference Call. At this time, all participants are in a listen-only mode. After the prepared remarks, we will conduct a question-and-answer session.
[Operator Instructions] As a reminder, this conference call is being recorded and will be available for replay on the Investor Relations section of the Ocular Therapeutix website. I would now like to turn the call over to Ocular Therapeutix's Vice President of Investor Relations, Bill Slattery Jr. Please go ahead, Mr. Slattery..
Good morning, everyone, and thank you for joining us today. Earlier this morning, we issued a press release and filed our annual report on Form 10-K outlining our financial results and business updates for the fourth quarter and full year of 2024 along with several updates to our registrational program for AXPAXLI in wet AMD.
Ocular Therapeutix's Executive Chairman, President, and CEO, Dr. Pravin Dugel, will summarize recent business highlights before we move to our question-and-answer session. Joining Dr.
Dugel for the Q&A portion of the call will be Donald Notman, Chief Financial Officer and Chief Operating Officer; Sanjay Nayak, Chief Strategy Officer; and Steve Meyers, Chief Commercial Officer.
We refer everyone to this morning's press release and our Form 10-K for a comprehensive update of fourth quarter and full year 2024 financial and business results. During today's call, certain statements we will be making constitute forward-looking statements under the safe harbor provisions of the Private Securities Litigation Reform Act of 1995.
Actual results may differ materially as a result of variety of factors, including risks and uncertainties identified in the Risk Factors section of our annual report on Form 10-K and our other SEC filings. With that, I'd like to hand the call over to Dr. Pravin Dugel to review our recent updates.
Pravin?.
First, the FDA approved an amendment to the SOL-1 SPA to incorporate redosing at weeks 52 and 76, increasing potential label flexibility to every six to 12 months.
Second, due to the requirement to maintain masking until redosing at 52 weeks, we now expect topline data for SOL-1, including the 36-week primary endpoint, will be released in the first quarter of 2026. Third, SOL-1 retention has been outstanding to date.
And the vast majority of rescue treatments reviewed on a masked basis have been in accordance with the prespecified criteria of the protocol. Fourth, as a result of our updated SOL-1 strategy for redosing, SOL-R has been streamlined with a target randomization reduced from 825 to 555 subjects.
This should accelerate the time to both SOL-R data and regulatory filings for AXPAXLI in wet AMD, all the while maintaining strong statistical powering of 90% based on our expectations of how AXPAXLI will perform.
Fifth, the non-inferiority margin for SOL-R is set at 4.5 letters, and standard rescue criteria have been prespecified to align with regulatory guidance. Sixth, enrollment has been excellent across both trials. SOL-1 completed randomization ahead of schedule in December.
And we previously announced SOL-R enrollment of 311 subjects across various stages of loading and randomization as of January 10, 2025. Seventh, AXPAXLI's opportunity extends beyond wet AMD, and we expect FDA feedback on the clinical trial design for NPDR and DME in the first half of this year.
And eight, Ocular Therapeutix is well financed and has cash runway into 2028. We do not intend to finance this year. We're maintaining strong capital efficiency as we advance toward key clinical readouts and a potential NDA submission in wet AMD.
We are redefining the retina experience, setting a new standard in treatment durability, flexibility and long-term outcomes. With strong execution, regulatory alignment and clinical momentum, we're well-positioned to become a leading retina company. Thank you for your time and continued support. Operator, we are now ready to take questions..
Thank you. [Operator Instructions] Our first question comes from the line of Tazeen Ahmad with Bank of America. Please proceed with your question..
Hi, guys. Good morning. Thanks for the updates. A couple of questions for me.
Pravin, just given the stats that you provided about the continued strength of what you're seeing blinded in SOL-1 in terms of patient staying in the study as well as the redosing rates coming in as you would have expected from your prespecified criteria, can you give us a little bit more color about why you think it makes sense to make these changes, especially right now? And then, secondly, in terms of making SOL-R a smaller study, just given the high demand that there has been clearly for patients to want to be in the study, can you talk about the reasons of why it wouldn't make sense anymore to have a study of this size just to add a little bit more cushion to the data set that we're expecting? And then, I have one follow-up.
Thanks..
Thank you, Tazeen. Good morning to you, and again, thank you for your question. What you've raised is a really important point and let me try and give a comprehensive answer. And I think this really speaks to the way we've designed our SOL programs and I include both.
These are complementary trials, and I dare say that this is revolutionary and I think really quite historic. I think everyone in the world expected us to have SOL-1 and SOL-2, which really has been the tradition. In every -- in just about every trial that I know, it's been the same trial done twice.
The second trial certainly is good to get the product approved and confirm the first trial. But when you think about it, it's terribly inefficient, because it really doesn't add any extra information whatsoever.
Instead what we've designed is two trials that are always to be taken together and are absolutely complementary in the information they provide.
And this I think is a unique and, I dare say, a revolutionary historic concept that will allow for efficiency both in terms of the logistics of the trials, the commercial applicability of the product, as well as the regulatory pathway.
The bottom line in what we announced today, the bottom line is that we will potentially get AXPAXLI to patients faster and with a better label. So, let me go through the sequence of events. Two things happened. The first is that the FDA approved our redosing SPA amendment for SOL-1 at week 52 and 56.
The second thing that happened is that we noted that the retention in SOL-1 was absolutely superb, under masking, of course. So, based on these two events, we're able to increase the efficiency of both studies.
In SOL-1, what we're able to do is to get information on the first year on the durability and flexibility of the drug, because now we have information at month nine, which is the primary endpoint that remains unchanged, and at month 12.
And in the second year with redosing, what we're able to do in SOL-1 is to maximize the exposure of the drug to patients and satisfy many of the FDA's safety requirements. So, immediately, SOL-1 became a much more efficient clinical trial. And with that in mind, we're able to pass down that efficiency to SOL-R the way these trials were designed.
So, no longer did we need 825 patients in SOL-R, we could maximize efficiency in terms of our resources as well as in terms of getting the filing to the FDA by reducing the size from 825 patients to 555 patients, while maintaining the integrity of the statistics.
The impact of this is that we will potentially have a much better label, a label that is a superiority label with flexibility of six months to 12 months. And the second impact, equally important of course, is that we will get to market potentially faster and more efficiently than we were able to before.
So, both of those things terribly important in terms of the impact of what's happened today. What I want to note, very importantly also, that the primary endpoint remains unchanged. Remember, the primary endpoint of SOL-1 is at nine months. That remains unchanged. The statistics remain unchanged completely.
What we added today, what we announced today were completely added efficiency bonuses. These are complementary trials designed to work together and I believe they work together absolutely beautifully..
Okay. That's super helpful.
And my one follow-up is that, given that, as you said, the primary endpoint stays the same, can you give us a sense of what the FDA might be looking for from redosing now in SOL-1?.
Well, again, the redosing allows for us in the first year to look to get information regarding flexibility and durability of the drug. Now, we'll have information at month nine. Again, that's the primary endpoint, which remains absolutely unchanged. But additionally, we'll also have information at month 12 regarding durability of the drug.
So, potentially, there's flexibility in the label for month nine as well as month 12. And as I mentioned, with the redosing in the second year, there's more exposure of the drug to the patients. Therefore, we'll have even more data in regards to safety.
The beauty of this is that when you think about the efficiency of SOL-1 with a single injection in the first year, we'll have information for month nine and month 12, and with repeat dosing for the second year, we'll have increased safety information with more exposure of the drug to patients..
Okay. Thank you for all the color..
Thank you, Tazeen..
Our next question is from the line of Biren Amin with Piper Sandler. Please proceed with your questions..
Yeah. Hi, guys. Thanks for taking my question, and congrats on all the updates. So, maybe Pravin, let me just start with SOL-1. What was the rationale for dosing at week 76? I understand the week 52 dosing, but I was trying to understand, I guess, the rationale for week 76.
And then, second question is, for SOL-1, will all patients receive redosing at week 52 and week 76 regardless of the arm, including the control arm? And also, will those patients with prior rescues receive redosing at week 52 and week 76?.
Biren, good morning, and thank you for your question. The answer for the first one is very simple, we wanted to maximize again the exposure of the drug to patients to satisfy the FDA safety requirements, thus redosing at week 56 -- at week 52, I'm sorry, week 52 and week 76 with the study ending at week 104.
The answer to your second question, yes, every patient will be redosed at week 52 and at week 76. The redosing will occur with the same drug that the patient was randomized to regardless of rescue. And that's very important.
The answer to your question is, yes, everybody will be redosed at week 52 and week 76 with the original drug that they were randomized to. I hope that answers your question. Thank you, Biren..
That does. And I just got a follow-up.
So, on SOL-R, as a result of these changes, you clearly reduced the size to 555 patients, which I think -- was that primarily due to the safety data that you're generating from SOL-1? Because I think now you would have another 172 patients that are redosed with AXPAXLI from SOL-1, whereas I think you reduced the need for the patients to be redosed with SOL-R by about 108 patients within AXPAXLI arm..
And Biren, again, thank you. You're exactly right. Your explanation is exactly correct. What we did was we designed SOL-R originally to have 825 patients to satisfy the FDA safety requirements.
And with the redosing amendment that we were able to get from the FDA, we were able to satisfy the safety requirements with both studies combined with the ability to reduce the number of patients from 825 patients to 555 patients, while still maintaining the statistical significance. So, your -- answer to your question is exactly correct. Thank you..
Got it. And then maybe one last question. I guess from a timeline standpoint, were these changes to SOL-1 and SOL-R underway or made when the Board constructed your performance base package on Ocular share price hitting -- I think there are four different targets between $15 and $30.
So, I guess I want to understand if these changes provide increased confidence on hitting those performance targets?.
Yeah. So, Biren, again, thank you very much for the question. The answer obviously, we have discussions with the FDA that are ongoing and we want to keep those discussions confidential. We don't discuss them publicly as with my discussions with the Board.
But suffice it to say that our confidence as a company in the success of these trials are higher than ever. And certainly my confidence particularly is higher than ever and you'll see that everything in this company is aligned to make sure that we ensure the success of both trials. Thank you..
Great. Thanks for taking my questions..
Absolutely..
The next questions are from the line of Colleen Kusy with Baird. Please proceed with your questions..
Great. Thanks. Good morning, and thanks for taking our questions. So, for the -- just to maybe clarify, for the redosing of patients in SOL-1, is that just for the FDA safety requirement for redosing, or do you need to show anything for efficacy in that protocol in the second year? And then, I have a follow-up..
Colleen, good morning, and thank you for your question. The answer is that it really is for the safety requirement for the FDA.
However, what it does allow us to do, again, is get information given this -- because remember, it's not just the matter of taking the second year separately, but also taking the second year in regard to how it affects the first year.
So, what it allows us to do is to get that extra information that we will now have not only at month nine, but also at month 12. So, it does allow for the flexibility that we hope to get in the label because we have additional information now at month 12 as well as month nine.
But again, we will satisfy the safety requirements, but we will also gain additional information in the second year regarding redosing. So, this is not a requirement for hitting the primary endpoint. I want to make that very, very clear. It's important to emphasize that nothing about the original primary endpoint changes.
The primary endpoint remains at month nine and the statistics remain the same. This is added efficiency today..
Got it. That's helpful. Thank you. And then, I know when you first shared the SOL-R trial design last summer, I think it was a 48-week endpoint and then -- but that was prior to talking to the FDA. Now, you're talking about a 56-week endpoint.
So, can you just talk about what drove that change and what that means for your dosing schedule, which I believe AXPAXLI is [still being dosed] (ph) every 24 weeks? So, just kind of talk about that 56-week endpoint, please..
Yeah. Thank you, Colleen. So, you're exactly right. I think the first time you might have heard about the 48-week endpoint for SOL-R was in our June Investor Day. And I want to emphasize, if you go back and check your notes then, we made it absolutely clear that we were proposing the SOL-R clinical trial design at risk.
And I think those two words, at risk, were mentioned quite a few times in that meeting. And the reason we did that is we made it very clear, very transparently that we had not yet gone to the FDA for formal approval regarding this trial design. That's why it was at risk.
Now, we did subsequently go to the FDA and the FDA came back and told us that they preferred a primary endpoint at week 52 or later. And as you know, we have a history of doing everything per the FDA. We wanted to make sure that we did it with a minimal amount of risk possible.
In fact, we wouldn't want to take any risk as far as our regulatory pathway is concerned. So, then, we decided, given their preference to pick week 56, and the FDA has now accepted in writing our proposal to pick the primary endpoint for SOL-R at week 56. I hope that answers your question, Colleen..
Great. Thanks.
And last one, just any timelines for SOL-R recruitment now in light of the decrease in the study size?.
Yeah. So, Colleen, we did give an update at JPM, as was said in my prepared statements. Since then, what I can tell you is that we've been thrilled with the recruitment of SOL-R, and we will give you an update when appropriate, but it may be a little bit too early at this point. But thank you for your question..
Understood. Thanks for taking our questions..
Thank you..
The next question is from the line of Kelly Shi with Jefferies. Please proceed with your question..
Hi, this is [Clara] (ph) on for Kelly. Thanks for taking our question, and congrats on the update. So, you mentioned that you intend to submit NDA after 56-week primary endpoints of SOL-R is reached.
So, I understand that the primary endpoints do not change, but also just trying to understand whether you would expect to have some long-term redosing durability data in SOL-1 as well by that time? And also just want to clarify whether the FDA requires that portion of data to support the redosing flexibility portion on the label? Thank you..
Clara, good morning, and thank you for your question. Very important questions, and I want to make it very clear as to what the FDA requirements are for NDA submission versus the information that we'll gather. To be very, very clear, what the FDA requires for the NDA submission is hitting the primary endpoint in both studies.
So, again, the primary endpoint for SOL-1 at month nine remains the same. The primary endpoint for SOL-R is at week 56. And our intention is that with presumably a positive study at week 56 with SOL-R, we will submit the NDA application to the FDA. That is unchanged.
We just expect given the announcements today that SOL-R will be recruited with more efficiency given the fact that the sample size is smaller. Now, in regards to your other questions regarding other requirements, yes, the FDA does have safety requirements as you're aware.
They will be fulfilled with the combination of patients in the second year in both SOL-1 and SOL-R. In addition to that, we will also have a significant amount of information that we believe we can leverage for commercial success.
And some of which you've already talked about and we've already talked about, which is the redosing of this drug that is now available both in SOL-1 and in SOL-R. And remember, we also have a numeric analysis that we're able to do with the third arm in SOL-R, which compares this drug to high dose EYLEA.
Now that is not for statistical analysis, that's for numeric analysis, but you can imagine we will have between these two studies a significant amount of data that is not necessarily required by the FDA, certainly it's not required for approval or NDA submission, but we can leverage for our commercial advantage, and we do intend to do that.
Thank you for your question, Clara..
Thank you..
Our next question is from the line of Sean McCutcheon with Raymond James. Please proceed with your questions..
Hi, guys. Thanks for taking the question. So, for SOL-R, could you give some detail on what you think the FDA expectations are, what your expectations are for what would be an acceptable number of rescues and timing of rescues regardless of if you hit the non-inferior -- land within the non-inferiority margin? Thanks..
Sean, good morning, and thank you for your question. Your question is a very important question, of course. So, let me discuss rescues. We mentioned today, I just want to make clear that the non-inferiority margin was 4.5 letters. And I just want to emphasize that, that is because we're exactly in guidelines with the FDA.
We've always done that and we expect to do that with everything that we do in regards to study design. In regards to the rescues, we have not detailed the rescue criteria as yet for competitive reasons, but we will do so. But here's what I can tell you. We will detail those when appropriate. You can expect the rescue criteria to be of no surprise.
They will be absolutely in line with the traditional rescue criteria that you've seen in the past. The FDA has given very clear guidelines of what they think about rescues, not just for us, but for all studies. The FDA has clearly stated, and this was stated most recently by Dr.
Boyd in the American Academy of Ophthalmology meeting, that the first rescue in a non-inferiority study will be allowed as long as it doesn't affect the primary endpoint. And that is a period of approximately three months or so as a rule of thumb before the primary endpoint. All other rescues will be subject to review.
And again, that's been stated for a number of years now. That is no different than any other clinical trial, and that is a general statement that still stands. However, what I can tell you is that I believe we will have a huge advantage due to the design of our clinical trials. Remember, these are complementary clinical trials.
And remember that SOL-R will never be reviewed by any regulatory agency without a positive SOL-1 study. And when these rescues for SOL-R are being evaluated, it will be evaluated in the context of a positive SOL-1 study.
So, the regulatory agencies will have a very clear idea that this drug will last for nine to 12 months based on a positive SOL-1 result. So, again, the rescues will be reviewed in context of a positive SOL-1 study, which will define the durability of this drug, which I will think will be very much to our advantage.
Again, this also emphasizes the advantage that we have of having these two complementary studies. Thanks for your question, Sean..
Thank you..
Our next questions are from the line of Jon Wolleben with Citizens JMP. Please proceed with your question..
Hey, thanks for taking the questions, Pravin. Two from us. Can you discuss the change in powering for SOL-R now for the primary? And then, stepping back, it seems like these changes have two big implications. One is the accelerate potential timing to a filing, but then also the new label information.
But how do you think about the importance of those two? Because my expectation would be if you get a year on the label, the docs could treat and [extend] (ph), as they do anyway.
So, how much value is that 52 weeks in the label versus just getting to market quicker?.
Jon, good morning, and thank you for your questions. Again, very important question. Look, as far as the SOL-R powering is concerned, we haven't guided you to that publicly. But what I can tell you is nothing changes. We had the 825 patient number to satisfy the FDA safety requirements. The powering and the statistics really do not change at all.
We're able to reduce the size because of the redosing amendment that was approved by the FDA for SOL-1. The statistics remain very robust and unchanged for us.
In regards to your second question regarding labeling, look, as a physician, I can tell you as someone who has practiced for the last 30 years, the label becomes very important for several reasons. One is scientific. It gives you the scientific data of what this drug does, which would be very important to see.
The opportunity is there in this study to find out the durability of this drug in a scientific manner. And that is very valuable information for physicians and for patients and for payers alike. The second reason for the labeling is really for the payers, and it will give us a huge commercial advantage.
So, our goal strategically is to have the best label that the market has seen, a label that is the superiority label, which will be the first and only of its kind potentially and one with a great deal of flexibility of dosing from six months to 12 months. Thanks for your question, Jon..
Thanks, Pravin..
Our next questions are from the line of Yi Chen with H.C. Wainwright. Please proceed with your questions..
Thank you for taking my question. With respect to the NPDR and DME, once you get the FDA feedback on clinical trial design, how quickly do you anticipate to advance those two indications into clinical trials? And do you intend to advance both indications concurrently? Thank you..
Yi, good morning. Again, thank you for your question. I'm glad you asked about NPDR and DME, and I'm glad that you put those together because I think it's very important to emphasize that with the HELIO study, we have shown absolutely everything to you, which is every single eye of every single patient.
And what you'll see there is not only a remarkable result in non-proliferative diabetic retinopathy, or NPDR, but also in diabetic macular edema, or DME. In fact, every single patient who had diabetic macular edema on entry of that study improved. And what you saw in the Angiogenesis meeting is a remarkable presentation by Dr.
Ehlers, where he showed that very clearly that these patients with fluid improved significantly after a single injection after 48 weeks. And so, our goal is to pursue not just NPDR, but also DME. How the trial will be designed? Yi, we don't know yet, because we will still meet with the FDA formally.
We committed to doing that in the first half of this calendar year. That has not changed. How quickly we will implement? That depends on that meeting, so I can't say now. But what I can say and what we did say is that we are financed very, very efficiently. We are very disciplined, in our financial expenditures.
And our intent is to keep the projections the way they are, which is that we are financed into 2028. And at this point, we do not have any intention of requiring any additional funding this year and that remains. Thank you for your question, Yi..
Our next question is from the line of Greg Harrison with Scotiabank. Please proceed with your question..
Hey, good morning, and thanks for taking the question. Curious what your expectations are for the percentage of patients that could show durability to 52 weeks without rescue in SOL-1 and to what extent do you think it could be used that way in practice..
Greg, good morning, and thank you for your question. The data, first of all, it's very, very valuable information and we don't shy away from this at all because not only because it's very valuable, but we believe that we're going to win quite honestly. We believe that there are a number of patients that will go to 52 weeks.
And this is based on the US study. In the US study, we had 60% of patients that went that long with a single injection, and that was in a non-enhanced patient population.
As you know, in previous discussions, we've gone through how painstakingly and thoughtfully we have selected our patients in a bespoke manner for each study to derisk the patient selection and derisk the outcomes. And the 60% that I quote to you, it really is in a unselected non-enriched patient population.
So, we're very confident of what we will show at week 12. Remember that there are drugs that are in the market now that are approved on label for a two week or so extension, some going to four months, with not very many patients that have actually crossed that threshold in their study.
So, from our point of view, we're going to provide very valuable information here to physicians, payers and patients alike, and we have the opportunity to have the best-in-class label as well. Thank you, Greg, for your question..
Thank you. This concludes our question-and-answer session. I'll now turn the call back to Dr. Pravin Dugel for closing remarks..
Once again, I'd like to thank everyone for taking the time to join us on our call today. We look forward to updating you on our progress. And if you have any follow-up questions, please reach out to Bill Slattery, our Vice President of Investor Relations. Have a great day everybody. Thank you..
This concludes today's conference. You may disconnect your lines at this time, and thank you for your participation..