Cybin Inc (CYBN) 2026 Q2 法說會逐字稿

Good morning, and thank you for joining the Cybin second-quarter 2026 financial results and corporate update call. As a reminder, our press release detailing today's updates is available in the Investors section of our website.

On today's call, you will first hear from Eric So, Cybin's Interim Chief Executive Officer and Executive Chair. Following Eric's remarks, Amir Inamdar, Cybin's Chief Medical Officer, will provide an update on our lead programs, CYB003 and CYB004. Finally, Greg Cavers, Cybin's Chief Financial Officer, will review the financials. Eric will then return with closing comments before we open the lines for Q&A.

Before we get started today, I would like to remind everyone that certain statements in this update are forward-looking statements and are prospective in nature. In preparing these forward-looking statements, several assumptions were made by Cybin, and there are risks that actual results obtained by the company will differ materially from these statements.

The company cannot guarantee that any forward-looking statement will materialize, and you are cautioned not to place undue reliance on them. We refer current and potential investors to the forward-looking information section of the company's management discussion and analysis available at sedarplus.ca and on EDGAR at sec.gov.

Forward-looking statements represent Cybin's expectations as of November 13, 2025. Except as required by Securities laws, Cybin does not undertake any obligation to update any forward-looking statements, whether as a result of new information, future events, or otherwise.

I will now turn the call over to Eric for his introductory remarks.

Good morning and thank you for joining us. This is an important quarter for Cybin, one that sets the stage for an active year of milestones. In September, Doug Drysdale stepped down as Chief Executive Officer. On behalf of the Board and the company, I want to thank Doug for his contributions. As Co-Founder and Executive Chair, I stepped in as Interim CEO to lead the transition while maintaining continuity and momentum. The Board's search for a permanent CEO is underway.

Through this transition, our priorities remain the same: patient-focused rigorous science, disciplined education as our execution and clear communication. We have tightened operational cadence and disclosure discipline, and we'll be adding targeted talent and scientific advisory board expertise to support late-stage execution and launch readiness.

Our strategy starts where care happens: in the clinic. What I mean by this is that we are designing therapy days that fit within existing schedules with short predictable sessions and a staff-light workflow that clinic teams can run without new infrastructure. From there, we focus -- our focus turns to maintaining wellness. Durability is built into the plan with an efficient retreatment approach that aims to reduce visit burden compared with today's multi-visit standards, so clinics can scale capacity and patients can plan their lives.

Progress with regulators follows the same discipline. We move step by step, anchored in data rather than speculation, and we'll communicate milestones as they are achieved. The capital plan matches that pace. Following our recent $175 million financing, we are focusing on advancing our programs towards major data readouts.

With that context, let me turn to the quarter and the progress we've made. Before we proceed to the agenda, a brief overview of our pipeline. For those of you who are new to the Cybin story, we have two lead programs. CYB003, our proprietary deuterated psilocin analog is in Phase 3 studies for potential adjunctive treatment of major depressive disorder. And CYB004, our deuterated dimethyltryptamine or DMT program for the potential treatment of generalized anxiety disorder is in Phase 2.

Clinically, our Phase 3 CYB003 program, which is an a breakthrough therapy designation in major depressive disorder, has continued to progress, including being granted additional clearances to commence EMBRACE, our second Phase 3 study in new geographies.

In generalized anxiety disorder, the Phase 2 CYB004 study completed enrollment and remains on track for our first calendar quarter 2026 top-line readout. Amir will share more details about both programs shortly. At the same time, we advanced preparations for scale, including manufacturing and commercial groundwork aligned to a practical clinic workflow.

We also strengthened our capital position with the closing of a significant registered direct offering, which provides flexibility to execute through upcoming milestones with clear internal decision dates by program. Across both programs, we are deploying capital with discipline. We are prioritizing global site activation and conduct for EMBRACE and APPROACH, database lock and analysis for CYB004, and manufacturing readiness for CYB003.

With that framework in mind, I'd like to turn the call over to our Chief Medical Officer, Amir Inamdar, to review our clinical and regulatory process. He'll begin with CYB003 in major depressive disorder, focusing on that study status, global footprint, and how the design supports real-world clinic operations and durable outcomes.

Dr. Inamdar will then review CYB004 in generalized anxiety disorder, including trial design, operational status following enrollment completion, and the timing and scope of the next data update.

Thank you, Eric. Our Phase 3 PARADIGM program is moving forward as planned. Dosing is underway in APPROACH across US sites and participants have rolled over into extend to generate durability data once the double-blind period concludes. In parallel, EMBRACE has been cleared to commence in the United States, UK, multiple countries in the European Union and Australia, giving us a truly global footprint.

The study targets approximately 330 participants across about 60 clinical sites and is structured with three arms to evaluate two active doses against placebo in patients with depression whose symptoms remain inadequately controlled on background therapy. The primary endpoint is the change from baseline in MADRS total score at six weeks after the first dose.

The design is built for clinical reality. CYB003 is intended to run as a predictable staff-light session that fits within existing clinic infrastructure. Prior clinical data showed sustained response and remission at 12 months after two 16-milligram doses, and our extension work is aimed at translating that durability into an efficient retreatment approach that reduces visit burden compared with today's multi-visit standards.

On the regulatory front, our posture remains conservative and specific. Near-term touch points focus on clean study conduct, global site activation, and data quality reviews as we advance towards pivotal readouts.

In anxiety, the work is tracking on schedule. We have completed enrollment in the randomized double-blind Phase 2 study of CYB004 and remain on track for top-line data in the first calendar quarter of 2026. The study evaluates two intramuscular doses given three weeks apart with efficacy assessed at 6 and 12 weeks and optional follow-up out to 12 months. The design permits concomitant antidepressants or anxiolytics and allows comorbid depression, which helps the results reflect real clinical populations.

Just as important, intramuscular administration supports short, predictable sessions that fit a standard clinic day, so sites can manage throughput with existing rooms and personnel. The protocol also captures information to guide an efficient treatment -- retreatment approach if patients need it, aligning durability with practical clinic operations.

I will now turn the call back to Eric to discuss the platform and commercial readiness.

Thank you, Amir. Our focus is to make these therapies workable in the real world, not just on paper. Achieving that goal begins with dependable supply. With Thermo Fisher in place for both drug substance and capsule drug product in the United States, we have a manufacturing footprint size for Phase 3 and commercialization, which gives sites the predictability to plan therapy days within their existing four walls.

From there, we extend into the clinic. Through our partnership with Osmind, we have access to a broad network of psychiatric practices, point-of-care software, and real-world data, so clinics can map out our protocols onto the schedules they already run. Staggered starts, defined observation windows, and clear rule definitions are intended to support predictable session scheduling within existing rooms and teams without requiring new infrastructure.

Throughput only matters if the session itself is practical. CYB003 is designed to live inside a standard interventional psychiatry day, offering predictable timing for patients and staff. CYB004, delivered intramuscularly, targets a briefing clinic experience that simplifies room turnover and staffing compared with all-day alternatives. The combination is intentional; one program suited to establish clinic rhythms, another built for speed and simplicity, both aiming to raise capacity without raising complexity.

Durability is the other half of practicality. Phase 2 CYB003 data showed sustained response and remission at 12 months after just two doses. And our extension work is there to translate that durability into an efficient retreatment approach. The goal is fewer visits and more efficient planning for clinics and payers alike with clear criteria for when patients should return, how long a session should take, and how that fits across a full clinic day.

We're advancing this platform with a conservative regulatory posture and a disciplined capital plan. Underpinning it all is steady leadership. We manage the CEO transition in an orderly way. The permanent CEO search is active, and our governance cadence and disclosure discipline keep the organization aligned as we execute towards the next two major data events.

Before I turn the call over to Greg Cavers, our CFO, let me touch on our capital structure. Last month, we closed a registered direct offering with participation from prominent institutional healthcare investors. The structure paired common shares with prefunded warrants with a partial warrant, aligning capital to near-term objectives and giving us the flexibility to execute.

As noted earlier, this was an important step for Cybin. The financing provides the resource to advance our ongoing Phase 2 and Phase 3 trials towards key data readouts. We have used a portion of the net proceeds from the financing to repay the outstanding convertible debentures to High Trail. For the avoidance of any doubt, this debt has been fully retired in full. We believe that participation from such high-quality institutions in the financing reflects confidence in our science, our programs, and our ability to deliver.

I'd like to take this opportunity to thank our new investors as well as existing shareholders and investors for their continued support of our mission. We could not be happier with the partners that came into this financing and all prior financings that drive our programs forward.

Capital deployment is paced to measurable milestones. For CYB003, funds support global Phase 3 execution and manufacturing readiness, so sites have reliable supply and predictable therapy days. For CYB004, resources moved to database lock, protocol-specified analysis, and operational lift to top line. Corporate use remains limited and targeted.

The plan bridges us to the next two major data events while preserving flexibility. As data and regulatory interactions inform the path, we will adjust with discipline and continue to communicate clearly about our progress and next steps.

I will now hand it off to Greg Cavers, our CFO, to walk through our second quarter financial results.

Thank you, Eric. During the quarter, cash-based operating expenses consisting of research, general and administrative costs totaled $28.5 million for the quarter ended September 30, 2025, compared to $18.2 million in the same period last year. Net loss was $33.7 million for the quarter ended September 30, 2025, compared to a net loss of $41.9 million in the same period last year.

Cash flows used in operating activities were $34.5 million for the quarter ended September 30, 2025, again, compared to $19.1 million in the same period last year. Operating loss was $28.9 million and net loss for the quarter was $33.7 million or $1.39 per basic and diluted share based on a weighted average share count of 24.2 million shares.

We ended the quarter with cash, cash equivalents and investments of $83.8 million. Subsequent to quarter end, we closed a financing of $175 million, which together with our quarter end balance, provides flexibility to execute our plan.

We continue to allocate capital to measurable milestones and corporate uses remain limited and targeted. Based on our current operating plan, we expect our cash resources to fund key data readouts in 2026 and fund operations into 2027.

I will now hand it back over to Eric for closing remarks.

Thank you, Greg. In the quarters ahead, our focus is execution against measurable milestones across the business. For CYB003, we will continue dosing and approach and expand EMBRACE site activation across clear geographies, keeping study conduct and data quality at the center of the plan as we progress towards a Phase 3 top line in Q4 of 2026.

For CYB004, the path runs through database lock protocol-specified analysis and preparation of a clear top line package in the first quarter of 2026. In parallel, we will advance commercial and manufacturing readiness, so sites have reliable supply and a practical clinic day model as data matures, and we will continue to pace investment to milestones.

This forward plan also includes leadership. The CEO search is active and progressing, and we'll provide an update when there is news. Day-to-day execution remains stable under the current structure with operating cadence and disclosure discipline intact. Taken together, clinical progress, measured capital deployment, commercial preparation, and leadership continuity position the company to navigate the next two data events and the steps that follow.

To summarize, we have executed through a leadership transition, advanced our late-stage programs, strengthened the balance sheet, and prepared for scale with a model built for clinical reality. The work ahead is clear: deliver clean data on time, maintain a conservative and specific regulatory posture, and keep capital focused on milestones that move the programs forward.

I want to thank all of our employees, investigators, investors, partners, and most importantly, the patients and families who make this progress possible. We look forward to updating you as we meet our milestones.

Operator, please open the phone line for questions.

(Operator Instructions) Pete Stavropoulos, Cantor Fitzgerald.

This is Sarah on for Pete. Two questions from us. One on the CYB004 and the other one on the 003 program. First off, around 004 and GAD, you completed enrollment in early September. Congratulations on that. And you have a readout on 1Q '26, where you enrolled a total of 36 patients.

What would you like to see from this study that would give you confidence to move forward into P3s? Is it statistical significance on the primary endpoint? Is it directional data suggesting improvement sufficient? And then what can we expect to see in 1Q? Are you going to provide the six-week data for the primary endpoint, HAM-A? Or will you provide efficacy data through 12 weeks?

I can take that one. Thank you, Sarah, for the question. And yes, we've completed enrollment in that study. As you probably know, it's a study with two arms, one low dose arm, which potentially is sub-psychedelic and a full threshold dose. We look at that as a dose response type of study.

We would love to see some separation between the two. As you state there, directional data is what we are looking for, a trend in change or trend in separation between the two and also within subject differences in change from baseline, at least with the threshold dose.

This is a proof-of-concept study, not necessarily designed as a fully powered study. But if we see a statistically significant difference, we'll be thrilled. But as you say, directional data, trend in improvement, and a dose response between the two arms is what we are looking for.

And we'll share this in first quarter. We will aim to share HAM-A data out through 12 (technical difficulty).

Awesome. Thanks. And then one more question from me. The P2 CYB003 data suggests that two doses may keep patients in remission for up to a year commercially. And then taking into account the psychologic experience associated with psilocin, what do you see as the minimum durability threshold needed to compete with SPRAVATO? And how are you thinking about the trade-off between durability versus time spent in clinics from both a payer perspective reimbursement?

Okay. One moment please while we reconnect Dr. Amir.

Can you hear me now? Sorry, I'm back.

Yes, sir. Now loud and clear.

Apologies for that. Can you repeat the question?

The P2 CYB003 data suggests that two doses may keep patients in remission for up to a year commercially and taking into account the psychedelic experience associated with psilocin, like what do you see as the minimum durability threshold needed to compete with SPRAVATO?

Yeah. I mean when you look at the guidance that the agency provides for evaluation of these therapies, they want data up to 12 weeks, which is three months. We will be thrilled to see effects that are maintained out to three months.

We are hoping for better. As you know, with our Phase 2 data, we showed durability out to a year. But based on what is the expectation of the agency, 12 weeks at a minimum would be great.

Patrick Trucchio, HC Wainwright.

Congrats on all the progress. I just wanted to get a clarification on the CYB004 program, just in terms of what we should expect as far as statistical powering and the definition of clinically meaningful HAM-A improvement? And then separately, I'm just wondering for CYB003, what operational milestones remain to complete enrollment in APPROACH and are site activations tracking to plan?

(technical difficulty) CYB004. As I stated earlier, it's not a formally powered study. We would, however, be looking at an improvement from baseline within subject, within the arms. A clinically meaningful effect would be somewhere around 4 points to 5 points on the HAM-A.

A trend to difference between the two arms would be important as well because we want to look at some dose response between the two arms. (technical difficulty) study in the sense that it's not a pivotal study, those statistical significance would be amazing.

You had a question on CYB003 as well. CYB003 is tracking as to plan. So we remain on target to complete enrollment by mid of next year and deliver top-line data by the end of next year.

Great. And if I could, just a separate question on -- as these programs are advancing into later stage and are in late-stage development, I'm just wondering what has been your engagement with payers at this stage and health economic modeling for both CYB003 and CYB004? And as well with the product profile that's emerging for both of these compounds, how you would expect positioning of them in the market relative to what's already available in TRD with SPRAVATO?

Given that this is, with CYB003, we're looking at MDD; CYB004, GAD. But I'm just wondering how you're thinking about this early payer engagement and as well the product profile positioning against both compounds available, but also those that are in development?

Hi. Thanks for that, Patrick. I'll take this one. So I mean, as you might imagine, at this stage, it's a little bit early, but payer engagement, of course, has begun. Commenting further, I guess, on how that develops and how, ultimately, with SPRAVATO, you could compare to the commercial model (technical difficulty)

All right. One moment. It looks like he has disconnected. If anybody else wants to take this question, while we reconnect him.

So while George is dialing back in, so we have been doing some preliminary market research. But as George reiterated, it is a bit early for -- at least for CYB004. And both the programs, we see them fitting into what is emerging now as an interventional psychiatry paradigm, which really has been spearheaded with SPRAVATO, creating the infrastructure out there.

We see these as intermittent treatments that will fit right into that model where patients come in for treatment on an intermittent basis, have the treatment in the clinic, and then return for their additional dosing as and when necessary. The infrastructure is there. And we believe with the GAD for CYB004 and with adjunctive and inadequate responder for CYB003, those address the spectrum of the most burdensome or most resource-intensive patients that you typically see in a psychiatry practice.

And George has reconnected.

Jim Molloy, Alliance Global Partners.

This is Laura Suriel on for Jim Molloy. Thank you for taking our questions. So for the ongoing APPROACH trial, you mentioned how you're planning to have a total of 45 clinical trial sites within the US. So you may just provide a bit more detail on the criteria behind choosing these sites and the activation process involved? And also as well as when you might think you have all 45 of these sites fully activated and onboard for the study?

Yeah. So I can take that. So we are using a mixture of sites that are experienced in clinical trials and a smaller proportion of sites that are less experienced in psychiatry trials. We also have a mixture of sites that are experienced in conducting trials with psychedelics. And then there are other sites that we have included that are experienced in CNS trials in general, but not necessarily psychedelics.

As you can imagine, with the number of clinical trials ongoing right now in psychedelics, there is, of course, competition for resources at sites, and we've been very careful in selecting sites that, one, either have a proven track record of delivering high-quality data or have the -- if they are not experienced in psychedelics, they have the necessary experience and expertise in the psychiatry space in general in other trials, and we are confident that they will deliver good quality data.

You referred to the number of sites. Yes, we've got 45 sites selected for this study. Virtually all of them are onboarded by now. What's important is with the number of sites that we have activated, we still remain on track to deliver or complete enrollment by mid of next year with top line data by the end of the year.

Great. Thank you. And then also, I know the current focus right now is on the CYB003 and the 004 programs. But can you just provide a bit more color on the preclinical 005 program, maybe just on the status of the preclinical studies and any potential partnership opportunities that you may be in discussions with?

Yeah. For CYB005, we are doing a number of preclinical profiling studies to characterize the receptor profile, the brain penetration, as well as the primary and secondary pharmacodynamics with a range of compounds in that class, which we believe would be well suited to -- actually with some of the neuropsychiatric conditions where there is significant unmet need. So that work is ongoing. And when there is information to share with the market, we will do so.

Eddie Hickman, Guggenheim.

Good morning. Thank you for taking my question. Congrats on all the progress. Just two for me. How much visibility do you have into the blinded baseline patient characteristic data from the APPROACH study? And can you talk at all about how this patient population will differ from a TRD population as it relates to baseline?

And secondly, what agreement do you have with the FDA related to the safety database for 003 and what you'll need to provide a regulatory filing? Is there a minimum number of retreatments per year needed in EXTEND?

(technical difficulty) I missed the second one. Can you repeat the second question? (technical difficulty)

Dr. Amir, you're cutting in and out. All right please stand by while we reconnect Dr. Amir --

Can you hear me now?

Yes, sir. Now, we can.

Yes, I can hear you.

Sorry, do you mind Eddie repeating that question?

Yeah. So I was asking the first question is how much visibility do you have into the blinded baseline patient characteristic data from the APPROACH study and how this population may differ from a TRD population? And then on the safety database, what you'll need in a regulatory filing, is there a minimum number of retreatments per year needed in the EXTEND trial?

Yeah. Thank you. So the safety -- as the trial is ongoing, the data is blinded. We are performing checks as necessary or as possible with blinded data, which essentially are quality checks in a blinded manner. And since this is a pivotal trial, we are, of course, being very careful with the data.

There are other checks built into the database, which ensures that there -- any flags with respect to data quality, they are raised to us immediately if there is a reason for concern. So far, we haven't had anything flagged in the database. So we are confident that the data quality is being maintained.

In terms of how this is different from the TRD population. So this group of patients is earlier in the treatment cycle. So these are patients who are inadequately responding. And they may have failed one treatment or they may have failed one and been on their second treatment, but not adequately responding, but not fully failed.

So they are not that one-third of the patient population that remains after multiple treatment trials. So it's about two-thirds of -- if you think of the depression population as a whole, this is the first two-thirds of those patients in the treatment cycle, whereas TRD would be the last two-thirds left after multiple treatment cycles.

In terms of ends, the -- or safety database, the safety database really is a function of the frequency of administration. Given that this is an intermittent treatment, what we have discussed with the agency as part of our BTD discussions is that the data that we will provide to them, the numbers that we provide to them across the three studies would be sufficient to support an NDA. But of course, again, it depends on what we find out in the long-term extension study with respect to treatment frequency.

Elemer Piros, Lucid Capital Partners.

Yes. Thank you. I just wanted to get maybe just one tiny detail on the loan repayment. If you could clarify how much was repaid and what was the prepayment penalty or the early repayment fees?

Thank you. Yes, we repaid High Trail $20 million and the repayment fee ended up being 10%.

10%, so it wasn't a $50 million loan?

The loan -- yes, the loan was structured as a convertible debt, and they had converted the other $30 million approximately.

Converted the other. Okay. That's all and thank you so much.

Sumant Kulkarni, Canaccord Genuity.

Good morning. And nice to see the progress and thanks for taking the questions. I have three. On CYB003, during your pivotal trial program, how important is it that patients remain compliant with their background antidepressant use?

All right. One moment, please.

Sorry, I was speaking on mute, Sumant, taking that question. The -- so for our patients in the APPROACH study and EMBRACE, because this is adjunctive, the instructions to the patients and requirements in the protocol is that they remain on their background antidepressant medication. We do not expect them or advise them to come off their antidepressant medication during the treatment period.

Got it. And then on 004, do you see an eventual pivotal program involving an intramuscular route of delivery? And what are some of the key challenges of developing an oral formulation? And my last question is, what are some of the specific qualities that you believe are must-haves for an incoming CEO?

I can take the first two. Eric can take the last one. So right now, yes, intramuscular is the route of administration that we plan to progress in Phase 3. It's a very convenient form of administration, which also gives us what we need in terms of the plasma exposures and the acute experience, which cannot be achieved with something like oral.

With oral, the elimination is pretty rapid. And DMP or CYB004 does not reach the plasma PK levels, the threshold that is necessary for a breakthrough experience, which, as we know, is necessary for therapeutic efficacy. That we are achieving with intramuscular. It's well tolerated so that is what we are going to take into Phase 3.

And maybe I can also add, Amir, that the intramuscular route is one that as we are aware from our market research with the interventional psychiatry clinics is one that is also being used currently by interventional psychiatrists administering ketamine. And so that gives us some confidence that it is a route that will get -- will reach adoption in the market.

And with regards to your question regarding CEO qualities, I mean, obviously, we've been at it for only about eight weeks right now. The Board is spearheading that process. And at the moment, we're looking for the qualities that this company and its shareholders deserve, a successful steward of capital that investors can feel confident in. Someone that has executed in the past, bringing a novel drug to market ideally through commercialization. An individual that has transacted and dealt with big pharma in the past as well. These are all table stakes for us and the next individual that will be sitting in the chair.

Thank you. At this time, there are no further questions in the queue. So I'd like to turn the call back over to Eric for any additional or closing remarks.

No further remarks. I just want to thank everybody for attending the call today. It's been a very exciting time for Cybin, and we look forward to delivering some fantastic updates for everybody in the future. Thank you all for your support.

Thank you, ladies and gentlemen. This does conclude today's program, and we appreciate your participation. You may disconnect at any time.