Taysha Gene Therapies Q3 2025 Earnings Call - Breakthrough Therapy Designation and Pivotal Trial Launch Propel Rett Syndrome Program

Conference Operator: Good day, everyone, and welcome to the Tacea Gene Therapies Third Quarter twenty twenty five Earnings Call. At this time, all participants are in a listen only mode. Later, you will have the opportunity to ask questions during the question and answer session. Please note this call may be recorded and I will be standing by if you should need any assistance. Is now my pleasure to turn the conference over to Haley Collins.

Please go ahead.

Haley Collins, Investor Relations, Taysha Gene Therapies: Thank you. Good morning, and welcome to our third quarter twenty twenty five financial results and corporate update call. Earlier today, issued a press release announcing financial results for the third quarter ended 09/30/2025. A copy of this press release is available on the company’s website and through our SEC filings. Joining me on today’s call are Shah Nolan, Cacea’s Chief Executive Officer Dhukumar Nagandran, President and Head of R and D and Kamran Lamm, Chief Financial Officer.

We will hold a question and answer session following our prepared remarks. On today’s call, we will be making forward looking statements, including statements concerning the potential of TATIA-one hundred two, including the reproducibility and durability of any favorable results initially seen in patients dosed to date in clinical trials, including with respect to functional milestones to positively impact quality of life and alter the course of disease in the patients we seek to treat our research, development and regulatory plans for our product candidates, including the timing of initiating additional trials, reporting data from our clinical trials and making regulatory submissions, timing our outcomes of communications with the FDA on the regulatory pathway for TATIA-one hundred two, the potential for the product candidate to receive regulatory approval from the FDA or equivalent regulatory agencies, our ability to realize the benefits of breakthrough therapy designation for TAECA-one hundred two and the market opportunity for our programs. This call may also contain forward looking statements relating to TACIA’s growth, forecasted cash runway and future operating results, discovery and development of product candidates, strategic alliances and intellectual property as well as matters that are not historical facts or information. Various risks may cause Katia’s actual results to differ materially from those stated or implied in such forward looking statements.

For a list and description of the risks and uncertainties that we face, please see the reports that we have filed with the SEC, including in our annual report on Form 10 ks for the full year 12/31/2024, that we filed 02/26/2025 and our quarterly report on Form 10 Q for the quarter ended 09/30/2025, that we filed today. This conference call contains time sensitive information that is accurate only as of the date of this live broadcast, 11/04/2025. Seysha undertakes no obligation to revise or update any forward looking statements to reflect events or circumstances after the date of this conference call, except as may be required by applicable securities laws. With that, I would now like to turn the call over to our CEO, Sean Mullen.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Thank you, Haley, and welcome everyone to our third quarter conference call. I will begin with an update of our recent corporate activities and progress across our TATIA-one hundred two Rett Syndrome program. Sukhu will then discuss the new supplemental analysis from Part A of our REVEAL Phase onetwo trials. Cameron will follow-up with a financial update, and I will provide closing remarks before opening the call to questions. In the quarter, we believe we made meaningful progress that sets the stage for what could be a transformative period ahead for Taysha.

The recent regulatory clarity and progress we’ve achieved, which was enabled by the strength of our REVEAL Part A dataset, rigorous data evaluation methodology, and our natural history data analysis allows us to focus on executing our REVEAL pivotal trial and advancing towards BLA submission with clarity and confidence. A major milestone was the receipt of FDA breakthrough therapy designation for TATIA-one hundred two at the September. This designation is designed to expedite the development and review of therapies for serious conditions that have demonstrated preliminary clinical evidence of substantial improvement over available treatments in one or more clinically meaningful endpoints. TATIA-one hundred two received breakthrough therapy designation based on the FDA’s review of available safety and efficacy data from all 12 pediatric, adolescent, and adult patients treated with Taysha one hundred two in Part A of our REVEAL Phase onetwo trials, including clinical data from the previously disclosed May 2025 data cutoff. Receiving Breakthrough designation highlights the FDA’s recognition of both the significant unmet medical need among the estimated ten thousand patients suffering from Rett syndrome in The US, and the therapeutic potential of TATIA-one hundred two to redefine the treatment paradigm for this devastating disease.

Notably, over eighty percent of programs with breakthrough therapy designation that proceeded to file for approval have ultimately received FDA approval. We look forward to continued engagement with the FDA as we advance toward potential registration. In September, we finalized alignment with FDA on our REVEAL pivotal trial protocol and statistical analysis plan in support of our planned BLA submission for TATIA-one hundred two, following resolution of remaining clinical and statistical queries. Importantly, our previously aligned upon key design elements remain unchanged. In line with FDA’s guidance for cell and gene therapy programs that was issued in September, we believe that by prospectively aligning with FDA on the statistical analysis plan for our pivotal trial helps ensure that the dataset collected will be considered reliable and suitable for BLA submission.

We are enrolling 15 patients in the developmental plateau population of Rett syndrome, with a primary endpoint of response rate, which is defined as the percentage of patients who gain or regain one or more of the 28 natural history defined developmental milestones. A response rate of thirty three percent, equivalent to five out of fifteen patients, is the minimum threshold for success sufficient to achieve our primary endpoint. Notably, we’ve observed a one hundred percent response rate across the 10 patients in Part A of our REVEAL trials. Additionally, we align with the FDA on a six month interim analysis that may serve as the basis for BLA submission, potentially accelerating our planned BLA submission by at least two quarters. As previously disclosed, the data from Part A of the REVEAL trials demonstrated an eighty three percent response rate at six months post treatment, with five of the six patients treated with the high dose TATIA-one hundred two achieving a developmental milestone.

We observed a consistent pattern of sustained milestone gains with a deepening of effect or additional milestone gains over time. By nine months post treatment, the data demonstrated a one hundred percent response rate across the six treated high dose patients in Part A. We believe these data support both the suitability of the six month time point to demonstrate clinically meaningful efficacy, and that the six month efficacy data may be representative of treatment effects at twelve months. We believe this enabled our alignment with FDA that a six month interim analysis may serve as the basis for BLA submission. It’s important to understand that we believe we received breakthrough therapy designation and achieved FDA alignment largely due to the results of the rigorous clinical evaluation methodology applied to our video evidence developmental milestone data from Part A of the REVEAL Phase onetwo trials.

In Part A, videos were centrally rated by multiple independent reviewers using milestone definitions from the pivotal trial protocol to ensure an objective, consistent evaluation of milestone gain and regain in the developmental plateau population, where these gains are not expected to spontaneously occur. By adhering to rigorous milestone evaluation criteria based on natural history, this approach minimizes bias and avoids over counting milestones by ensuring the milestones are truly eligible for gain or regain. As a result, this provides a reliable reflection of TATIA-one hundred two’s disease modifying therapeutic effect and ensures that the pivotal trial is well powered to demonstrate efficacy. We will continue to have frequent and consistent interactions with the FDA. We presented our REVEAL Part A data from the May 2025 data cutoff, including the new supplemental analysis, which provides supportive evidence that further reinforce TATIA-one hundred two’s consistent multi domain impact on activities of daily living at the Child Neurology Society Annual Meeting in October.

Sukhu will discuss these results shortly. With the strength of our Part A clinical data and a clear FDA aligned path to potential registration, we believe we are strongly positioned to initiate our REVEAL pivotal trial and accelerate execution towards BLA submission. Dosing of the first patient in our REVEAL pivotal trial is scheduled and on track for this quarter, with additional patient enrollment expected to continue across multiple sites this quarter. On the heels of our strong clinical and regulatory progress, we are thrilled to have regained full global rights to our TATIA-one hundred two Rett Syndrome program. We regained these rights in October following the expiration of our 2022 option agreement with Astellas, which had granted Astellas an exclusive option to enter into a negotiation period to license TATIA-one 102 and certain rights with respect to change and control transactions.

We appreciate the collaborative relationship we’ve had with Astellas and the unencumbered rights to TASIA 102 that we now hold enable us to focus on driving long term value with full strategic flexibility and optionality. We continue to build out our infrastructure to support advancing TATIA-one hundred two toward late stage development and potential commercialization, if approved. This September, we strengthened our commercial leadership team with the appointment of David McNinch as TACIA’s Chief Commercial Officer. David brings over two decades of experience in global commercialization and strategic market development across multiple therapeutic areas. Most recently, he served as chief business officer at Encoded Therapeutics, where he led the commercial and partnering strategy across the company gene therapy portfolio.

He previously held senior commercial roles at Prothena as well as Intramune, where he led the launch of Aspriot, the first FDA approved treatment for idiopathic pulmonary fibrosis, and supported the company’s acquisition by Roche. David reports to Sean McCullough, Taysha’s Chief Business Officer. Previously at AveXis, Sean led the development and execution of the commercial launch of ZOLGENSMA for spinal muscular atrophy, the first FDA approved gene therapy for the treatment of a monogenic CNS disease, which has reached blockbuster status. With an estimated fifteen thousand to twenty thousand patients with Rett syndrome across The US, EU, and UK, compelling clinical data from Part A of our REVEAL trials, and a minimally invasive commercially advantageous delivery approach, we see a significant opportunity to address a profound unmet medical need and drive long term value. We believe our strong balance sheet, team with proven gene therapy experience, and the clear path to registration strongly position us to initiate our REVEAL pivotal trial and accelerate execution toward BLA submission.

I will now turn the call over to Sukhu to discuss our clinical progress in more detail. Sukhu?

Sukhu Nagandran, President and Head of R&D, Taysha Gene Therapies: Thank you, Sean. As Sean mentioned, the regulatory progress we’ve achieved to date was enabled by the strength of our Reveal Part A data and our natural history data analysis that allows us to objectively measure developmental milestone gain and regain in the developmental plateau population using each patient as their own control. At the Child Neurologist Society Annual Meeting in October, we presented a comprehensive review of our Part A dataset using the evaluation frame point and endpoints of our pivotal trial. As previously reported, hundred percent of the ten patients in Part A achieved one or more natural history defined developmental milestones following treatment with TASHA one hundred two with a consistent pattern of early gains that are sustained and new achievements continue to emerge over time following TACHA-one hundred two treatment. These milestones were all video evidence and assessed by independent central raters according to the definition of milestone achievement from our pivotal trial protocol.

These criteria enabled a reliable, objective, and consistent assessment of TESHA one hundred two’s efficacy and importantly show that our pivotal trial is well powered to establish the therapeutic impact of TESHA one hundred two. Additionally, we presented a new supplemental analysis of revealed party data that captured supportive evidence of additional skill gains and improvements outside of the 28 natural history defined milestones. These gains are derived from the adapted Mullen scales of early learning, the revised motor behavior assessment or RNBA, and the observer reported communication ability assessment, which are RET validated structured assessments that evaluated pre specified skills and quantifiable improvements. The results show that in addition to the development milestones achieved across the treatment cohort in Part A, patients consistently gain multiple additional skills and improvements in core disease characteristics across the domains of autonomic function, communication, fine motor, and gross motor areas. We believe these findings reinforce the consistent broad therapeutic impact of tesia one hundred two on activities of daily living that are important to caregivers and clinicians.

As we continue to prioritize safety, I’m pleased to share that tesia one hundred two continues to be generally well tolerated with no treatment related serious adverse events or dose limiting toxicities across the 12 pediatric, adolescent, and adult patients treated with the high and low doses of taysha one zero two in part a of our revealed trials as of October 2025 data cutoff. We are encouraged by the data we have collected from part a of our REVEAL trials, which we believe support the potential of taysia one or two to provide meaningful benefit to children, adolescent, and adults living with Rett syndrome. We look forward to reporting longer term Part A clinical data in the 2026. I will now turn the call over to Cameron to discuss financials. Cameron?

Cameron Lamm, Chief Financial Officer, Taysha Gene Therapies: Thank you, Sukhu. Research and development expenses were $25,700,000 for the three months ended 09/30/2025, compared to $14,900,000 for the three months ended 09/30/2024. The increase was driven by BLA enabling process performance qualification or PPQ manufacturing initiatives, revealed clinical trial activities, and higher compensation expenses as a result of increased headcount during the three months ended 09/30/2025. General and administrative expenses were $8,300,000 for the three months ended 09/30/2025, compared to $7,900,000 for the three months ended 09/30/2024. The increase of $400,000 was primarily due to debt issuance costs incurred in connection with the refinancing of our existing loan and security agreement with Trinity Capital that are recorded in general and administrative expense under the fair value option and was partially offset by lower legal and professional fees.

Net loss for the three months ended 09/30/2025 was $32,700,000 or $09 per share compared to a net loss of $25,500,000 or zero one zero dollars per share for the three months ended 09/30/2024. As of 09/30/2025, PACHA had $297,300,000 in cash and cash equivalents. We expect that our current cash resources will support planned operating expenses and capital requirements into 2028. I will now turn the call over to Sean for his closing remarks. Sean?

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Thank you, Cameron. With breakthrough therapy designation and finalized FDA alignment, together with our strong balance sheet and full strategic control of TATIA-one hundred two, we believe we are entering the pivotal phase of development with focus and confidence in our ability to redefine the treatment landscape for Rett syndrome while driving long term value. We remain on track to dose the first patient in our REVEAL pivotal trial with additional enrollment expected at multiple sites this quarter. Additionally, we expect to report longer term clinical data from Part A of our REVEAL Phase onetwo trials in the 2026. We look forward to providing further updates as we initiate our REVEAL pivotal trial and advance TASER 102 towards BLA submission.

I will now ask the operator to begin our Q and A session. Operator?

Conference Operator: We’ll take our first question from Kristen Kluska with Cantor. Your line is open.

Kristen Kluska, Analyst, Cantor: Hi, good morning everybody. Thanks so much for taking my question. Just curious this time around in the pivotal trial, you have a lot more evidence going for you. So can you talk about the pipeline of interest and demand for being in this trial and then your thoughts about how long it could take to fully enroll?

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Sure, Kristen. Thanks for the question. I would say unequivocally that the demand to be in the trial is exceptionally high. I think the fact that we’ve been relatively consistently putting out both safety and efficacy data as we have maturation occur in this study. And keeping close contact with the advocacy groups, centers of excellence, KOLs has led to a strong demand.

So with that as a backdrop, let me just turn it over to Sukhu to give a little bit more flavor and and then maybe just give timeline and, you know, parameters around what we expect enrollment could potentially take.

Sukhu Nagandran, President and Head of R&D, Taysha Gene Therapies: Thanks for that question, Kristen. So as Sean highlighted, we have multiple sites, more than 15 sites identified for our clinical trials program part b. All of these sites are at centers of excellence. And very interestingly, many of these sites have 100 plus patients per site who have the diagnosis of Rett syndrome, and many of these patients could qualify for a Part b trial. And this includes pediatric, adolescent, and adult patients who will be part of the process.

Now furthermore, let me highlight that in the best case scenario, we could potentially enroll and recruit all 15 patients within a three month time period. And a more conservative timeline could be between three to six months. And as I said, many of these sites already have multiple patients identified, and there’s significant interest in our gene therapy program. Use the efficacy already and safety already disclosed in the partner trial and the ease of route of administration that we have to deliver a gene therapy that already shows significant clinical impact. Thank you.

Yeah.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: And maybe just one more thing to add. We highlighted it in the press release, but to Sukhu’s point, we’ve got dosing schedules for the first patient already scheduled this quarter. And we expect other patients to enroll at multiple sites this quarter as well. So I think that speaks to both the demand and the alacrity at which the sites have worked to initiate the pivotal trial.

Sukhu Nagandran, President and Head of R&D, Taysha Gene Therapies: And you know, sir, Christian, one more point I should emphasize is many of these sites may be able to dose more than one patient in kind of a staggered parallel fashion. So we might be able to get one, two, or three patients two, three weeks apart at some of these sites, which would further accelerate our timelines and hopefully make the submission of the BLA timeline even shorter and make this product available to deserving patients who have Rett syndrome.

Haley Collins, Investor Relations, Taysha Gene Therapies: Thank you.

Conference Operator: Our next question comes from Salveen Richter with Goldman Sachs. Your line is open.

Salveen Richter, Analyst, Goldman Sachs: Good morning. Thanks for taking my question. I was just wondering if you could touch on expectations for the longer term data in the first half of next year. And also, you know, help us understand in the context of your discussions with the FDA what they have signed off on in terms of that, you know, minimum threshold for success here that’s sufficient for filing? Thank you.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Thanks for the question, Salveen. For for the first part of the question relative to, you know, what updates will be given the first half of next year, I think it’ll be consistent with what you’ve seen. You know, as the as the data matures, we’ve tried to look at things as a full cohort. So ultimately, we wanna get to we have all 12 patients at at twelve months, and I think that’ll be very important, you know, data to look at relative to the six month time point, where are we at twelve months with these patients. And so we’ll do that.

In addition to that, I think it’s important to continue to provide updates relative to the safety profile. So we want a little bit of flexibility here that we could potentially give an update in the first quarter with almost twelve months of data we could do. We could wait for the second quarter. But we just want to make sure that the market’s aware of the fact that we do plan to give you know, further updates both in terms of safety and efficacy that we think will be very enlightening and informative relative to the predictability of the approval of the pivotal trial. So that’s number one.

Number two, as it relates to FDA alignment, you know, we highlighted in the script, and I think it’s really important that back in September, the FDA put out guidance that’s very consistent with everything we’ve done to date in our interactions with them, which is very specifically, they want alignment on your SAP before you start your clinical trial. Like, that is the highly recommended path to take. And and that’s exactly what we’ve done. You know, we submitted the SAP going back as far as January. When we got the okay to go ahead and submit the the final SAP and the clinical protocol by the end of the second quarter without end of phase meeting.

We did that. We’ve we’ve answered all the then subsequent queries from the statistical analysis plan question and clinical questions. And we actually even reached out to the FDA, because we had believed we’d answered all their questions. And we sent them a note and said, we just want to confirm that there’s no other outstanding statistical or clinical questions. And they said confirmed.

So we feel everything that we’ve just presented, you know, with the NF-fifteen, the threshold of a responder being, you know, the gain or regain of one milestone, and crossing the threshold of having a thirty three percent response rate all ties to the statistical plan that we’ve submitted. So we feel we’re very much in alignment with the FDA. And the other thing I would just note is that per the FDA’s internal SOPs, you know, these milestone meetings where you’re talking about, you know, the final protocol, the SAP, you know, internally, the directors are at those meetings. So I I I can’t give you specific names who are there, but that is the protocol. So we feel, you know, again, supremely confident at this particular point in time.

We’ve done everything that this FDA, you know, has asked us to do. We’ve been in full alignment with them the entire way. And I would argue we were in full alignment with the Peter Marks regime as well. And I think that’s all because of the integrity of the data and the quality and rigor of the data collection that we’ve put forward. So we think we’ve checked all the boxes.

We’ve double checked, and we’re told we’re good to go. And that’s why it’s full steam ahead on patient enrollment right now.

: Thank you.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Thank you.

Conference Operator: Our next question comes from Tazeen Ahmad with Bank of America. Your line is open.

Tazeen Ahmad, Analyst, Bank of America: Hi, guys. Good morning. Thanks for taking my question. I wanted to get a little bit more color on how you’re thinking about the way we should all be thinking about the data from the younger patients, meaning the two to six year old relative to the six plus year olds as it relates to efficacy in particular? And then on safety, should we be expecting to see a staggered release of safety data on that younger population relative to the older population?

Basically, when could we expect to see data start to come in from that cohort base? Thanks.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Yeah. Sure. Thanks for the questions, Tazeen. Number one, think the headline is our goal is to ensure that by the time we submit the BLA under any circumstance, that these two to five year old population is included in that. Okay?

So that we would have a, you know, a very broad, you know, two plus label effectively. And so the way we’re stepping through that is this quarter, we’re in we’ll be having dialogue with the FDA. You know, we’ve submitted the protocol to them, so we’ll be getting some feedback, you know, on that. It is a safety focused study. We’ve we have had discussions with the FDA, formal meetings with the FDA, where we we basically made the following request.

That for this population, we wanna establish safety, number one. We will collect some efficacy data, of course. But what we proposed was that we could extrapolate efficacy from the six plus population, and that that would be sufficient for you know, getting this younger group into the label. And the FDA agreed to that. So that’s how we’re gonna step through it.

We would we would anticipate, you know, beginning to dose these patients, you know, once we have alignment with the FDA, probably towards the middle of of twenty twenty six. Again, because it’s safety, we think the trains will align on time in terms of BLA submissions, and then we’ll follow, you know, efficacy over the course of time in this patient population to see, you know, if there’s things that are unique there. If appropriate, you know, we could certainly update the label with any new data we have. But again, to just restate the primary goal, it’s that at approval, you would have a label of two plus with no specific constraints relative to efficacy that’s been collected. It’s the full population that you’re getting approval on.

Conference Operator: Our next question comes from Gil Blum with Needham and Company. Your line is open.

Gil Blum, Analyst, Needham and Company: Good morning, and thanks for taking our question. So maybe just another one on protocols here. How much leeway do you think the agency provides regarding the method of video review? And is it fair to assume that all companies in the space receive the same guidance on that? Thank you.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Yeah. Gil, I would say in our experience, the the most time we spent in dialogue with the FDA was around the rigor of the data collection for the primary endpoint. They were very much focused on how we were going to do that, that there was high fidelity in the data, and that there was high inter rater reliability. And in fact, what we did to further bolster our case with the FDA is we actually ran a pilot at multiple sites testing the DMA with multiple central raters. And we submitted that as, you know, in in part of our data package, you know, to get the protocol approved, and also, you know, in the breakthrough therapy package as well.

And so, you know, all I can say is that, like anything, you’re as good in our space. You’re as good as the data that you’re collecting. FDA was super focused on that. So I’m assuming anyone going into a pivotal trial, you know, would would be held to the standard of a minimum of video evidence and having it centrally adjudicated. I think the question is, you know, have you run the experiment, and do you know that the methodology you’re employing is gonna give you the result that you anticipate?

And what we feel good about is we’ve run that we’ve run that result. You know, we’ve collected the data from, you know, our part a study, and we’ve done, you know, central raters with that. But then the pilot study, which we really haven’t talked too much about, but but we ran that in the background, again, at multiple sites. And and that gives us the confidence and and hopefully, you know, gave the FDA confidence, that what we’re putting forward is is highly rigorous, high end fidelity, and, you know, high end inter rater reliability.

Gil Blum, Analyst, Needham and Company: Thank you for all that.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Thanks, Gil.

Conference Operator: Our next question comes from Biren Amin with Piper Sandler. Your line is open.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Hey, good morning. Thank you for taking our questions. This is Michael on for Biren. Are there any updates on your plans in Europe or discussions with the EMA on the applicability of Part B? And separately, is the bar for the interim analysis similar to that for the final twelve month analysis?

Thank you. Yeah. Thanks, Michael. Thanks for the question. You know, first and foremost, you know, our our focus has been and and will be on The US number one, two, and three.

I mean, that’s that’s the biggest market out there. You know, we’ve been historically resource constrained both financially as well as human resource capital wise. We’re we’re in a better position now, but we’ve really worked to make sure that we are as aligned as possible with the highest probability possible, you know, to get things approved as safely and as quickly as we can in The US. We will continue, and what we’ve been doing, Michael, with with Europe and The UK is is working to enable them, you know, so stepping through regulatory, you know, dialogues and and things of that nature. We think that as we further generate data in part a and also get into part b, that will further inform those those discussions and will give us even clear line of sight to what the options we have.

I mean, we know we’re gonna have multiple options to go into Europe. You know, there’s some that we’ve taken in the past that would be the most efficient and make the most sense for all parties involved. You know, we we wanna see if we can work to enable that. The other thing too is from a policy perspective, I think we all know the challenges on both sides of the pond. You know, we wanna make sure we focus here at home and and lock in those things.

And we can also, you know, take the time while we’re collecting the data to see how policy also shakes out from an ex US perspective as well. So the long term goal is to enable Europe for sure. It’s just a question of stepping through it in a very thoughtful manner.

Conference Operator: Our next question comes from Maury Raycroft with Jefferies. Your line is open.

Gil Blum, Analyst, Needham and Company: Hi. Congrats on the progress and thanks for taking my questions. Wondering if you could tell us anything additional about timelines for IRB approvals for the additional two to five sites that you’ll need for the pivotal. And just when thinking about enrollment for this study, is there anything more you could say about number of patients you could potentially have enrolled by end of this year? Just helping provide some line of sight to potentially getting to data from the pivotal by the end of next year.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Yeah, Maura, it’s a great question. I think we can provide more information in either Q1 or sometime in the springtime, I think as we have better line of sight. Again, just from a power stepping through it, we’ve protocol to the FDA. We’ve got a you know, waiting for their feedback on that. You know, that’ll certainly inform things.

You know, we’re doing I would say contextually, right, we’re doing for the pivotal trial 15 patients. This is a smaller subset of patients, so we would anticipate the number of patients to be less than 15 in in this study. You know, I think that from a IRB perspective, it it will be a new protocol, So it’ll have to go through the process of, you know, contracting, IRB approval, ethics, you know, all the things that you that you have to do. I can tell you that there are, as you would anticipate, multiple sites, of course, that wanna, you know, be a part of this. So I don’t think that’s gonna be, you know, an issue.

We just wanna make sure that, number one, we get alignment first and foremost with the FDA on the protocol and the associated statistical plan that we’re putting forward. And then number two, that from an operational perspective, we’re doing things in a manner that is most efficient and doesn’t by any way impede the enrollment of the six plus population. So the way we see this based on the fact that the primary endpoint in the little kid study is safety, you know, we we think the two trains are gonna come back together. And, again, just to make the point that we do anticipate including that data along with the six plus pivotal data in the BLA submission with the goal of getting a broad label.

Gil Blum, Analyst, Needham and Company: Got it. Okay. Thanks for taking my questions.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Thanks, Maury.

Conference Operator: Our next question comes from Jack Allen with Baird.

Haley Collins, Investor Relations, Taysha Gene Therapies0: Congrats on all the progress made over the course of the quarter. I guess my first one was on the broader sentiment of the FDA. There was quite a bit of news over the weekend and Monday morning drowning CBER and some changes outside Cedar. And I just wanted to get a sense for any thoughts that the team has as it relates to management interactions with the agency, whether the agency is functioning as expected and what your plans are going forward to interact? And then briefly on the younger patient cohort, I also wanted to ask about how you’re thinking about dose.

As you go into younger patients, you could theoretically increase the relative exposure if you’re treating smaller patients with a fixed dose. I’m just curious if you have any plans to address that potential issue.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Yeah, Jack, let me start with the second part of your question on dose. It’s going to be one hundred to the fifteenth, but we’re going to adjust for brain volume. So we wanna make sure that none of those younger kids get any more dose on a per kilogram basis than anyone we’ve dosed so far safely. So, you know, we’ve given that a lot of thought. The ClinVev team’s done a super job.

Again, we’ve got that in front of the FDA. So we’re being very thoughtful about that safety perspective. So more to come on that once we have the protocol finalized. As it relates to the FDA, you know, what we can point to is is a couple things. And I said this earlier.

We had we had good alignment with Nicole Verdant. Right? I mean, nothing that we’ve changed we’ve done nothing since the the new regime’s been in that’s different in terms of our natural history assessment, our proposed endpoints, etcetera. And I’ve used this term before, but no one has pushed us off the ball. And the reason we believe that is because we have levered data collected in a very rigorous manner to make our case with the FDA.

Number two, the approach that we’re taking is exactly what the FDA wants. So that’s why we referenced this FDA guidance from September where they’re basically saying, hey. For seen in for gene and cell therapies, we want alignment on your protocol and your SAP before you start to study. So what are we doing? We’ve taken our first in human study.

We’ve learned from that. We’ve done the natural history analysis. And now what we’re saying is based on what we learned, we’re gonna we’re gonna propose a prospective pivotal trial with the following endpoint and the following statistical analysis plan, and we’ve worked with the FDA to get that into, you know, a situation where they’ve signed off on that. So we’ve done ex exactly what they wanted. Our understanding is any of these milestone meetings, you know, like signing off on a protocol or, you know, breakthrough designation, which I can talk about in a second.

But internally, the the directors are are in those meetings. So, you know, we’ve checked and double checked to make sure we’re not misinterpreting things. We’ve gotten confirmation of that. We feel like we’ve done everything that the FDA has has asked us to do. And more importantly, we’re not asking them to do something that’s out of course.

You know, it would what we’re not doing is we’re not taking this the part a data and saying, oh, you know what? Let’s we’re gonna we want you guys to, you know, go back, and and we’re gonna propose now that we’re doing a DMA, and and we’re gonna do this developmental milestones. So we want you to approve our data based on, you know, a statistical plan we put in front of you after the fact. That is not something that we’ve done. We’re we’re taking a more traditional approach and starting a new study.

Sukhu wants to add some information.

Sukhu Nagandran, President and Head of R&D, Taysha Gene Therapies: Yeah. One thing I would add, Sean, is that under doctor Vine Prasad and Vijay Kumar’s current leadership of CEBA, they have their team has followed the spirit of the RMAT designation in CEBA and the breakthrough designation that we have achieved. So our interactions have been very fluid and very constructive and very useful. So I just wanted to emphasize that.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Yeah. I mean, Jack, one last thing on on breakthrough to to the point Suku’s making. The internal SOP at FDA for breakthrough is that when a breakthrough request comes in, the directors are made aware of it. They then send it to the review team and assign them to review it and let them know the recommendation. And so that means that eyes are on things.

And again, we’ve done the best that we can to be data driven in all of our requests. And and therefore, again, we feel the fact that the breakthrough was granted, you know, in September under this current regime in the manner that they like. We followed their guidance that they’ve issued in September in terms of protocol for pivotals as well as SAP. You know, we’re we’re we’ve tried to step through it, you know, in exact manner that they want. And I would argue the exact manner based on data that any administration would want.

So, you know, that’s why I I kinda went back into the way back machine with with the Peter Marks group, but it is important, and I do think it’s relevant to say they agreed with what we were doing as well based on the way that we were going through it. So I’ve always said data drives, you know, is the currency of the realm, and and we believe that’s the case. We’re just gonna keep moving forward and be as transparent as we can with the agency. And as a result of having breakthrough, you know, we now can set up even additional meetings with them, which we’ve already done, you know, to to start to talk about BLA submission process and things of that nature.

Haley Collins, Investor Relations, Taysha Gene Therapies0: Thank you so much. That’s great color.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Thanks, Jack.

Gil Blum, Analyst, Needham and Company: Our

Conference Operator: next question comes from Chris Raymond with Raymond James. Your line is open.

Haley Collins, Investor Relations, Taysha Gene Therapies1: Hey, thanks. Just a couple of commercial questions here maybe. So you’re starting the commercial build out now with the hiring of a Chief Commercial Officer. Maybe talk about the footprint you’ll need, how it will look, and maybe the milestones that we should expect, you know, in terms of, I guess, you know, access progress. And then maybe a related question.

You know, of the 28 developmental milestones, are there any that you think matter more, you know, be it communication, fine motor, or gross motor milestones in terms of clinical acceptance among the physician community or or in terms of ease of access that we should be thinking about? Thanks.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Yeah. I think to start with your second question, all of the 28 milestones that we’ve selected, we did in concert with KOLs and with the advocacy community. So, like, if you were talking to some of the KOLs, they would talk about higher order milestones. So there’s 51 milestones, Chris, in the natural history database. You’ll you’ll hear, like, that language because these are the milestones that that, you know, from a clinical and from a functional perspective, really do matter across the three different domains.

So, you know, I wouldn’t say, you know, anyone rises to the level more than anyone else. It’s all relevant to the particular situation of each individual patient. I will say that when you talk to the parents, you you know, communication is top of mind with them. You know, they they want to know, you know, what hurts, what do they want, are they hungry, you know, how can they make them feel better, those kinds of things which make a lot of sense. But that’s why we feel we’ve reached that agreement with the FDA that any one of those 28 is relevant.

And I think what we’re also trying to show is that over time, not only are there more milestones being gained of the 28, but the whole purpose of the supplemental analysis was to show that outside of that, I mean the 28 are a mechanism for us to get approval. But outside of that, in multiple scales, whether it be done from the clinicians or rated independently like the Mullen or the ORCA, which is the parents, what they’re saying that they’re noticing. The point of that was to say beyond twenty eighth that we’ve talked about, there’s a lot of other things happening that are great. And we’re seeing good things. The parents are seeing things.

The clinicians are seeing improvements in function. You know? And all of that is gonna be, you know, what we put forward to the FDA in the final package and would also be part of what we discussed with payers. Sue? Yeah.

Sukhu Nagandran, President and Head of R&D, Taysha Gene Therapies: Thanks, Sean. And one more thing I would add is that, Chris, is that as our trial design, this patient has their own control. Every milestone matters. So it doesn’t matter what the milestone is out of the twenty eighth to the patient, to the parent, or the caregiver. All of them actually matter, and all of them have impact on activities of of daily living.

And given our Part A dataset, my hope as a physician and clinician is that, there will be no patient left behind over time as we gather more data from Part

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: B. Yeah. And then the first part of your question, Chris, about commercial, you know, I’d say a couple of things. First, you know, in you’re you’re definitely on the leading edge of the curve here. You know, we think starting in the first quarter, we really are going to put more color around how we see the commercial opportunity.

I think for starters, it really is underappreciated how large the patient population is. So we’re doing a lot of work, you know, relative to claims data analysis and and things of that nature to put finer points on things. We’re also looking at the launch of debut. I mean, that’s gonna be a good surrogate for potential uptake. And the more that we’re digging into things, you know, the more robust we think the opportunity truly is, particularly in a situation where, you know, the data set that we’re going to be able to discuss with payers and also get the treating clinicians and the families, you know, hopefully excited about what they’re seeing, is that, you know, no one’s been able to demonstrate functional gains before in a neurodevelopmental disease, even in adults.

So that opens up a really significant opportunity. And you know, we also have known from the get go that using CGI and RSBQ and those type of scales is going to mean absolutely nothing to the payers. They do not care what, you know, a CGI score actually is. They want to know what they’re paying for, and what they’re going to be paying for is going to be improvements in function or gains of function that haven’t been demonstrated, which is why we feel so strongly that this endpoint for gene therapy is the right way to go. You know, an example is in Canada, the HTA denied debut being reimbursed because they couldn’t determine the clinical relevance of a 0.3 change in CGI.

So again, I think we’re going to be on really strong ground with the data set that we’re putting forward in a very significant patient population. And the other thing I’ll say just in terms of the team, you know, David McNinch is our new Chief Commercial Officer. He’s got a ton of experience. He and I worked together at Interimmune, you know, on the launch of Espria, which was a big success. David was also recently at Encoded.

He knows gene therapy very well. He reports to Sean McCullough, who’s our chief business officer. Sean was on the Zolgensma launch team. So, you know, we’ve got, you know, a very stacked group internally. And I would say on the medical affairs team, you know, our head of medical affairs, Alon, you know, ran med affairs in Canada for Acadia.

So, like, we we feel like the field team and the commercial team called the external facing group. We’ve got just a stellar all star team. And we’ll continue to put out more perspective on that as we generate the data and move towards the BLA submission. Great question.

Haley Collins, Investor Relations, Taysha Gene Therapies1: Excellent. Thanks.

Conference Operator: Our next question comes from Yanan Xu with Wells Fargo Securities. Your line is open.

: Great. Thanks for taking our questions. I wanted to dig into the statistical plan a little bit. Thanks for all the color so far on the call regarding alignment and the FDA. Given that the trial design is novel and there is not a external control arm per se, wonder how the p value is derived.

And also, in terms of the interim analysis, how unambiguous or subjective the threshold is for triggering filing based on interim. In other words, do you run any risk if you file on interim? Just wondering regard to the actual data and the p value in making that decision. Thank you.

Sukhu Nagandran, President and Head of R&D, Taysha Gene Therapies: So that’s a good question. So I’ll try to answer that for you in in in kind of very simple straightforward terms. So the evaluations are not subjective. They’re actually quite objective. Because remember, we have a natural history that is very tightly analyzed, and the FDA accepted a natural history analysis.

But it’s very clear on these once these patients get above six years of age, they do not gain new milestones or they do not regain milestones. And our evaluation process for achievement of my new milestones or regain a milestone is video recorded. And as Sean has pointed out earlier, it’s very rigorously evaluated by blinded central reviewers. And there are different reviewers for the six month interim analysis as well as the twelve month interim analysis. So you have to keep that in mind as well.

Now remember also the six month interim analysis, all 15 patients dosed have to reach that six month time point before we break the blind on the video evaluations and before we share the information of the data with the FDA for potentially filing on the BLA as we complete the study at twelve months. And that dataset will also be available at the final filing of the BLA. So what we do is by the six month interim analysis process, we have the opportunity to shorten the timeline of filing of the BLA by two quarters or more. So, again, the six month interim analysis also does not really have significant impact on the p value, you know, the power of the study given that the loss of the alpha is actually minimal. And it’s a 33 responder rate.

That is all that’s needed really to meet our primary endpoint, whether it’s a six month or twelve month analysis. And keep in mind that usually none of these patients at six months reached a new milestone or regain a lost milestone. Therefore, any milestone gained one by one patient is miraculous. So I believe it at that from a clinician’s perspective. I think we have something that I hope that we can gather the data quickly and get our dataset to the FDA so that we can make this therapy available to patients as soon as possible.

I hope that answers your question, Yanan.

: Yeah. Yes. Great. Thanks for the color.

Conference Operator: Our next question comes from Joon Lee with Truist Securities. Your line is open.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: Hi, good morning. This is Mehdi on for Joon, and thanks for taking our question. So the the the question is I just wanted to ask you to please remind us what is the actual definition of regaining again? And assuming that, you know, at the six months in between data is positive, how soon you can start filing for BLA?

Haley Collins, Investor Relations, Taysha Gene Therapies: Thank you.

Sukhu Nagandran, President and Head of R&D, Taysha Gene Therapies: Yeah. Thanks for that question. So this is Sukoo, and I’ll respond to that question because it’s thanks because it’s important that’s clearly defined, and the audience understands what it means. So remember again, natural history. Once patients with Rett syndrome reach the age of six and above, they do not regain a lost milestone.

So I’ll give you an obvious one. Let’s assume a patient before six years of age with Rett syndrome can sit up without support, and they lose it completely and now cannot sit up without support. Post treatment with tesa one zero two or gene therapy through lumbar puncture, if that patient now again is able to sit without support, that is a regain of a lost milestone. A gain of a new milestone is something where the patient before the age of six, for example, can never use their fingers due to significant stereotactic movements, and therefore cannot pick up a teaspoon or a cup to feed themselves. Post treatment, this milestone is now achieved where the patient can actually use their fingers, which they’re never done before, can pick up a spoon or a cup and feed themselves.

That is the gain of a new milestone. So it’s very almost black and white. So which is actually makes it very easy both for the clinicians who evaluated the patients, the video reviewers who are blinded, as well as when the FDA hopefully sees our videos, it will make it obvious that our product actually works. And keep in mind that this entire process of video recording, central raters, blinding, etcetera, came from our Vexus experience many years ago, and we have most of the team here at Tasia that will continue to execute on this program and hopefully reproduce what we were able to do for a semi population using Vexis one zero one, which is now Zolgensma. Thank you.

Conference Operator: It appears we have no further questions at this time. I’ll turn the program back to the speakers for any additional or closing remarks.

Sean Mullen, Chief Executive Officer, Taysha Gene Therapies: We appreciate everyone taking the time this morning to join us. Have a good day. Thank you.

Conference Operator: This concludes today’s program. Thank you for your participation, and you may disconnect at any time.