Medicenna Therapeutics Corp. (MDNA) CEO Fahar Merchant on Q4 2022 Results – Earnings Call Transcript

Medicenna Therapeutics Corp. (NASDAQ:MDNA) Q4 2022 Earnings Conference Call June 22, 2022 8:30 AM ET

Company Participants

Dan Ferry – IR, LifeSci Advisors

Fahar Merchant – President & CEO

Martin Bexon – CMO

Liz Williams – CFO

Conference Call Participants

Matt Biegler – Oppenheimer

David Martin – Bloom Burton

Catherine Novack – JonesTrading

Swayampakula Ramakanth – H.C. Wainwright

Andre Uddin – Mackie Research Capital

Shubhendu Roy – Brookline Capital Markets

David Bautz – Zacks Small-Cap Research

Operator

Hello, and welcome to the Medicenna Therapeutics Fiscal Year-End Earnings Call. All participants are now in a listen-only mode. There will be a question-and-answer session at the end of this call. [Operator Instructions] Please be advised that this call is being recorded at the company’s request.

I would now like to turn the call over to Dan Ferry of LifeSci Advisors. Dan, please go ahead.

Dan Ferry

Thank you, operator, and thank you all for participating in today’s conference call. This morning, Medicenna issued a press release providing financial results and corporate updates for the fiscal year ended March 31, 2022. If you have not yet seen the press release, it is available on the Investors page of Medicenna’s website.

Before we begin, I would like to remind you that certain statements and information shared during this call constitute forward-looking information within the meaning of applicable securities laws. All statements other than statements of historical facts shared during this call, and that relate to the future operations of the company, and other statements that are not historical facts, including statements related to the clinical potential and development of MDNA11, MDNA55, and the BiSKITs programs, potential of the Superkine platform, partnering activities, cash runway, the presentation of additional data and other milestones.

Our forward-looking statements that are subject to risks and uncertainties. There could be no assurance that such statements will prove to be accurate, and actual results and future events could differ materially from those anticipated in such statements. Important factors that could cause actual results to differ materially from the company’s expectations, include the risks detailed in the recently filed Annual Information Form, Management’s Discussion and Analysis and Form 20-F of the company, and in other filings made by the company with the applicable securities regulators from time to time in Canada and the United States.

Listeners are cautioned that assumptions used in the preparation of any forward-looking information may prove to be incorrect. Events or circumstances may cause actual results to differ materially from those predicted as a result of numerous known and unknown risks, uncertainties, and other factors, many of which are beyond the control of the company. You are cautioned not to place undue reliance on any forward-looking information. Such information, although considered reasonable by management, may prove to be incorrect, and actual results may differ materially from those anticipated.

Forward-looking statements contained in this conference call are expressly qualified by this cautionary statement. Except as required by law, we do not intend and do not assume any obligation to update or revise publicly any of the included forward-looking statements, only as expressly required by Canadian and United States securities law.

Now, I will turn the call over to Dr. Fahar Merchant, President and Chief Executive Officer of Medicenna Therapeutics. Fahar?

Fahar Merchant

Thank you, Dan, and thanks to all of you joining us on today’s call. In addition to Dan, I’m joined by Dr. Martin Bexon, our Acting Chief Medical Officer; and Liz Williams, our Chief Financial Officer.

With the considerable progress made in the past fiscal year, we believe that we are now at the cusp of what is an exciting and pivotal time for Medicenna. This is being driven by the progress we have made with the initiation and advancement of the Phase 1/2 ABILITY study in patients with advanced solid tumors, which is the first clinical study of our differentiated beta only long-acting IL-2 super-agonist, MDNA11 and the promising signs of clinical activity we are reporting in the early stage of our dose escalation portion of the trial.

During the past 12 months, despite being in the midst of a global pandemic, we completed all of the CMC activities associated with GMP compliant manufacturing of MDNA11 for the Phase 1/2 ABILITY study. The IND enabling studies required for regulatory submissions to commence first in human clinical trials with MDNA11 and a secured clearance of the various applications submitted to regulatory agencies in Australia, U.S. and Canada.

As a result, we are well underway in our dose escalation portion of the ABILITY study and continue to enroll patients at multiple clinical sites in diverse geographic regions to establish the recommended Phase 2 dose for the dose expansion phase of the study, both as a single agent and in combination with a checkpoint inhibitor. We have continued to also build our pipeline of new long-acting IL-4 and IL-13 Super-Antagonists, as well as our Bifunctional Superkines for ImmunoTherapies or BiSKITs such as the anti-PD-1 MDNA19 cis-targeting fusion protein.

Furthermore, we have completed a comprehensive commercial opportunity analysis of our MDNA55 program for treatment of recurrent glioblastoma and other brain cancers. With compelling clinical data and an attractive registration pathway, MDNA55 scored highly among KOLs in Europe and the U.S. and was rated very favorably by payers for reimbursement based on projected pricing. We look forward to a positive outcome as we advance our discussions with interested parties.

Finally, we closed the year end with a strong cash balance of $20.5 million and have made modifications to our budget in order to extend the cash runway well into Q2 calendar 2023, taking us well past our anticipated first substantial clinical efficacy readouts from the ABILITY study.

In the Phase 1/2 ABILITY clinical study of MDNA11, in patients with advanced and metastatic solid tumors by primary objectives are to investigate safety and tolerability and determine the recommended Phase 2 dose, while the secondary objectives are to evaluate pharmacokinetics, pharmacodynamics, immunogenicity and preliminary anti-tumor activity in both the monotherapy and the combination arms of the study.

Since dosing the first patient in the ABILITY study this past September, we have observed very encouraging data in the first three dose escalation cohorts, consistent with MDNA11’s anticipated differentiation from competing IL-2programs. MDNA11 is demonstrating an acceptable safety and tolerability profile, as well as promising early signs of clinical activity in the first eight patients, while dose escalation continues to enroll in cohort 4.

Although, it is too early to draw meaningful conclusions on efficacy potential of MDNA11 from the dose escalation portion of the clinical trial. We have seen very encouraging signs of CD8 T and NK cell activation and proliferation in the periphery, in most patients treated so far as well as early signs of tumor control in three out of eight patients.

Further, the PD data was from peripheral blood sampling and we expect that this PD data may have a different profile and durability of activation of cancer fighting immune cells in the tumor and the tumor-draining lymph nodes. Given that the therapy is well tolerated as we escalated from 3 micrograms per kilogram in cohort 1 to 30 micrograms per kilogram in cohort 3. Medicenna has implemented a step up dosing regimen in all subsequent dose escalations.

Cohort 4 is currently enrolling at the target dose of 60 micrograms per kilogram following two priming doses at 30 micrograms per kilogram. As we continue to escalate, we could see different dynamics emerge at higher doses. We therefore look forward to data updates throughout 2022 for more safety, PK/PD and efficacy data.

In the second half of 2022, we expect more fulsome data for MDNA11 as well as early data from the single-agent dose expansion cohorts in a restricted number of tumor types such as metastatic melanoma and advanced renal cell carcinoma.

Management expects approximately 10 more patients in the dose escalation portion of the study in addition to 13 patients already enrolled to date in cohorts 1 to 4. With encouraging PK/PD and safety data and early signs of tumor control in three out of eight patients in cohorts 1 to (ph) 3, we expect more meaningful signals of efficacy at higher doses as we continue with the dose escalation portion of the ABILITY study.

As the ABILITY study has advanced over the past fiscal year, we have been consistently monitoring the data it has generated, changes in the regulatory environment, as well as data reported from clinical trials of other IL-2 variants. Although, recent clinical results from trials of PEGylated IL-2 have not shown clinical efficacy. It is important to note three key points.

First, IL-2 is a validated target that when administered at high dose, it is known to drive meaningful clinical benefit. Second, MDNA11 is clearly differentiated from these competing agents in ways that we expect will translate through superior efficacy. The data we have seen from the ABILITY study supports this view, which is a topic Martin will cover in more detail.

And third, we have the benefit of leveraging the learnings from recent trials of competing IL-2 variants to optimize our clinical development plans in a data driven manner to increase our chances of success. One of these learnings comes from early safety data that shows modest adverse events such as fever or chills being more prevalent after the initial dose of MDNA11 than after subsequent doses.

Based on this observation in the clinic, and in non-human primate studies and to ensure we are able to achieve a maximum MDNA11 dose before reaching dose limiting toxicities. We are utilizing a step up dosing strategy from cohort 4 onwards. This strategy entails first treating patients with two priming doses to habituate them to MDNA11, before stepping up to the higher fixed dose that is being evaluated.

This is expected to increase our chances of identifying MDNA11’s optimum dose and is in line with FDA’s recently released Project OPTIMUS initiative, which encourages companies to do more early on in clinical development to find the optimal dose for oncology drugs. Given the dose dependent, PD effects, and early signs of clinical activity, MDNA11 has displayed thus far in the ABILITY study, ensuring that we are able to identify its optimum recommended Phase 2 dose will further improve our chances of clinical success. Our failure to reach the optimal dose is something that may have hampered other IL-2 programs such as the PEGylated variant I mentioned earlier.

While the step up dosing regimen we are pursuing with MDNA11 will allow us to achieve higher doses and position the ABILITY study for success, it does take longer to dose each patient as two priming doses are required before administering the target dose. This has impacted our follow-up period for each patient to eight weeks instead of four weeks when using the fixed dose approach. Thus enrollment in the fourth and subsequent cohorts will take longer and delay our ability to collect patient scans following the target dose.

We expect updated PK/PD data from cohort 4 in July 2022, first follow-up CT scans at the higher dose cohort 4 in Q3 of calendar 2022, with a full set of efficacy data for all dose escalation cohorts in Q4 of calendar 2022. To help ensure, the MDNA11 program is advanced as efficiently as possible. We made it a point this past fiscal year to assemble world class advisory councils, including our Development Advisory Committee and Scientific and Clinical Advisory Boards.

These include some of the world’s leading experts on drug development and cancer immunotherapy, which allows us to gain invaluable insights and complementary perspectives on our drug discovery and development efforts. These have been crucial to the advancement of not only MDNA11, but also to the advancement of our preclinical stage Superkines and BiSKITs.

We recently highlighted two of these preclinical assets in posters at the AACR meeting this past April. One poster focused on Fc-MDNA413, which is derived from our Superkine platform and consists of an IL-13 super-antagonist fused to the Fc domain for half-life extension and the second poster featured a preclinical candidate from our BiSKITs program.

As a reminder, BiSKITs are Bifunctional Superkines designed to combine two distinct and synergistic immunotherapy mechanisms of action into a single molecule. This poster outlined preclinical studies on a BiSKIT consisting of an anti-PD-1 antibody linked to an IL-2 super-agonist similar to MDNA11.

We believe our ability to incorporate checkpoint inhibitors, which are widely successful commercial drugs into novel BiSKITs, may provide important intellectual property advantages as the first generation of checkpoint inhibitors come off patent. This in turn could spark valuable collaborations with the leading developers of these agents.

Over the past 12 months, we have seen that some of the world’s renowned academic labs have independently published results, demonstrating the exceptional potential of our core MDNA109 IL-2 Superkine platform when incorporated in Oncolytic viruses, CAR-T based therapies, conditionally activated Superkines or when combined with STING agonists. This provides external validation of our Superkine platform, especially the MDNA11 asset.

Looking forward, we expect the continued advancement of our preclinical Superkines and BiSKITs and to provide important value creation opportunities to supplement our lead MDNA11 program.

With that, I will now turn the call over to Martin to discuss the ABILITY study status, recent data, and future outlook. Martin?

Martin Bexon

Thanks, Fahar. Since our last earnings call in February, we reported pharmacodynamic data from the ABILITY study’s third dose escalation cohorts and are currently enrolling patients in cohort 4 with clinical trial sites open in the United States, Canada and Australia. We have not observed any dose limiting toxicities in the study to date and remain on track to report additional PK/PD data at the end of July and the Cytokine Summit to be held in Boston. In the second half of calendar 2022, we expect to identify MDNA11’s recommended Phase 2 dose and initiate the study’s single agent expansion phase.

Before moving on to discuss the ABILITY study recent data and what we believe it means to the program, I’d first like to provide some context by briefly mentioning the recently reported results of the randomized Phase 3 trials evaluating a different IL-2 variant in patients with previously untreated advanced melanoma and metastatic renal cell carcinoma. For those of you who may be unfamiliar with this trial, it evaluates the PEGylated IL-2 in combination with the checkpoint inhibitor Opdivo versus therapy with a tyrosine kinase inhibitor.

An analysis of the data from the trial showed no clinical benefit in double therapy arm. While the results from this other program are obviously disappointing for patients, I should emphasize that we do not expect them to be applicable to MDNA11. In fact, seeing the results of this trial have provided us with valuable learnings that we believe will increase our chance of success with MDNA11, which is something I will discuss shortly. Before I do this, however, I would like to explain why we believe MDNA11 is positioned to overcome the shortcomings that have affected PEGylated IL-2 variants and how the ABILITY study’s recent data strongly support this hypothesis.

I’ll begin by emphasizing a point Fahar made earlier, which is an IL-2 is a validated immunotherapy target since high dose IL-2 is required to bind and activate effector immune cells via the intermediate receptor comprising the IL-2 beta receptor and has been approved for the treatment of renal cell carcinoma and metastatic melanoma. We therefore know that successful simulation of the IL-2 receptor complex via the beta receptor can drive meaningful clinical benefits as high dose native IL-2 or Proleukin has shown efficacy.

The rationale behind developing IL-2 variants such as MDNA11 or PEGylated IL-2 is to improve upon Proleukin’s safety profile due to its ability to bind to the high affinity receptor, which also comprises the IL-2 alpha receptor. Consequently, Proleukin’s pharmacokinetic profile necessitate doses in the ICU every eight hours of five days with severely strict treatment durations and therefore, overall target exposure and uptake.

Given that the toxicity associated with Proleukin seems to be linked to its affinity for the IL-2 receptor alpha, the next generation IL-2 programs are focused on reducing affinity for this receptor subunit. While PEGylation is able to decrease IL-2 receptor alpha binding affinity and improve half-life, we are of the view that this is a suboptimal approach for a few reasons.

A key limitation of using PEGylation to decrease IL-2 receptor alpha binding affinity is that it also leads to a reduction in binding to the IL-2 receptor beta, which is critical for the activation of the anti-cancer immune cells that drive response to IL-2 therapies. This is in stark contrast to MDNA11 which has significantly enhanced affinity for IL-2 receptor beta.

Additionally, past data has shown that PEGylated IL-2s are not truly not alpha molecules since all pegmoities will gradually dissociate from IL-2 following administration, which leads to unintended IL-2 receptor alpha binding, resulting in toxicity and may also activate pro-tumor Treg cells, which are known to limit the efficacy of immunotherapies.

Based on both MDNA’s inherent design and all the data we have seen from the ABILITY study to date, we are confident that its long-acting beta only IL-2 binding approach is the best approach to improve patient outcomes while overcoming the concerns associated with Proleukin. As a reminder, MDNA11 was engineered using direct evolution to enhance binding to the IL-2 receptor beta, resulting in a 30-fold improved binding compared to that of Proleukin and has two additional mutations that avoid its ability to bind to the IL-2 receptor alpha, therefore, avoiding Treg stimulation and improving its safety profile.

Finally, to improve its pharmacokinetics, we engineered IL-2 is [indiscernible] to directly to albumin, a protein scaffold that is known to improve tumor accumulation and localization of tumor-grade lymph nodes. As I alluded to earlier, these features are expected to translate to enhanced efficacy and safety compared to other IL-2 programs. The ABILITY studied preliminary data indicate that MDNA11 is behaving in the clinic very much it was designed to do. We have observed dose-dependent preferential simulation of anti-cancer immune cells with limited stimulation of pro tumor Tregs and no significant increases in eosinophils, which are associated with toxicity.

Notably, MDNA11 increases in cancer find to immune cells are greater than those seen with competing agents, administered equivalent IL-2 doses. This provides strong evidence that MDNA’s superior preclinical results are translating in the clinic as expected and may, therefore, demonstrate superior efficacy as the ABILITY study continues to advance.

Diving a little deeper into the recent ABILITY study PD data, we can see a biological profile emerging, which is well in line with what we are aiming to achieve. On our last earnings call, I mentioned we had to see higher levels of CD8, and natural killer cell simulation relative to Treg activation in the ABILITY study subsequent cohorts. This is exactly what we saw with our recent data from cohort 3, a CD8-positive T to Treg, and NK to Treg ratios increased by 2.6 fold and 4.4 fold over baseline, respectively.

I also mentioned having to see increases in the market of immune cell activation. I’m pleased to say that we are successful in this one as meaningful post-treatment increases in both CD25-positive and ICOS-positive CD8+ T cells were observed in our most recent data release. Taken together, these early pharmacodynamic data suggest that MDNA11 has a biological profile that could translate to superior efficacy, and we look forward to continued evaluation of this hypothesis in the ABILITY study. Safety data collected in the study to date have been encouraging. As we have not yet recorded any dose emitting toxicities, which allows for continued dose escalation from 30 micrograms per kilogram at cohort 3 to 60 micrograms per kilogram in cohort 4 following 2 priming doses at 30 micrograms per kg.

Looking ahead, the data we have seen to date gives us confidence in MDNA11 potential to be a best-in-class IL-2 therapy. We see the Superkine inducing a selective and resolute anti-cancer immune response without the activation of cells associated with toxicity or protein release approaching immune suppression. This indicates that MDNA11 is potentially engaging its intended target. The safety and pharmacokinetic profile displayed to date are promising and suggested it can overcome the shortcomings of the only approved IL-2 therapy Proleukin. We are eagerly anticipating reporting additional clinical data from the trial in the third calendar quarter this year and providing a fulsome clinical update in calendar Q4 across all dose cohorts.

With that, I’ll turn things over to our CFO, Liz Williams, to discuss the financial results for fiscal year 2022. Liz?

Liz Williams

Thanks, Martin, and good morning, everyone. Before I begin, I’ll note that all references are in Canadian dollars unless otherwise stated. Medicenna remains well capitalized through key anticipated catalysts during the ABILITY study, including single agent efficacy results. We had cash, cash equivalents and marketable securities of $20.5 million as of March 31, 2022, which based on our current projections is expected to fund our operations late into calendar Q2 of 2023.

Net loss for the year ended March 31, 2022, was $22.6 million or $0.42 per share compared to a loss of $17.3 million or $0.35 per share for the year ended March 31, 2021. The increase in net loss for the year ended March 31, 2022, compared with the year ended March 31, 2021, was primarily a result of increased expenditures related to the MDNA11 development program as well as higher general and administrative expenses associated with the company’s NASDAQ listing in August 2020.

Research and development expenses of $14.7 million were incurred during the year ended March 31, 2022, compared with $10.9 million incurred in the year ended March 31, 2021. The increase in research and development expenses in the current year was primarily attributable to costs associated with the development of MDNA11, including one-time IND-enabling studies and manufacturing of GMP materials for the clinical trial as well as clinical and regulatory costs associated with the initiation of the Phase I/II ABILITY study.

General and administrative expenses of $7.8 million were incurred during the year ended March 31, 2022, compared with $6.5 million during the year ended March 31, 2021. The increase in expenditures year-over-year is primarily attributed to a full year of costs associated with Medicenna’s NASDAQ listing and corresponding directors and officers liability insurance premiums compared with only eight months of expense in the prior year period.

For further details on our financials, please refer to our financial statements and management’s discussion and analysis, which will be available on SEDAR and EDGAR, respectively.

I’ll now hand the call back to Fahar for some concluding remarks prior to the Q&A session.

Fahar Merchant

Thanks, Liz. As we look ahead into fiscal 2023, we are pleased to be advancing towards key potential value inflection points, including clinical data from the first three cohorts as well as PD and PK data from cohort 4 at the Cytokine Summit at the end of July. The pharmacodynamic data we have seen thus far from the three cohorts is encouraging. We have incorporated key early learnings from the trial into its design moving forward and continue to enroll patients in its fourth dose escalation cohort.

In parallel, our Superkine and BiSKITs platforms continue to fuel our preclinical efforts, which we expect to provide additional opportunities for pipeline expansion and value creation. I’d like to thank all of those who have contributed to the considerable progress we’ve made over the past last year under challenging circumstances. This includes our employees, partners, investigators and clinical trial participants and their families. Their efforts have us well positioned for success as we continue our work to generate shareholder value by advancing towards our ultimate goal of developing novel cytokine-based immunotherapies that provide patients with meaningful clinical benefits.

And with that, we’ll now open the lines for questions. Operator?

Question-and-Answer Session

Operator

Thank you. We will now be conducting a question-and- answer a question. [Operator Instructions] Our first questions come from the line of Matt Biegler with Oppenheimer. Please proceed with your question.

Matt Biegler

Hey, Guys. Thanks for the update. Two from us. First, can you comment on the mix of patients you’ve enrolled in ABILITY so far? It seems like many or most of the patients had tumor types like a sarcoma that you wouldn’t really expect to respond to immunotherapy or a checkpoint inhibitor or Proleukin for that matter? And then I had a question maybe on the safety signal that you’re seeing so far, interesting commentary around the priming dose. It seems to us like maybe that’s a way to get around some of the CRs related side effects.

So with that said, and I appreciate the commentary around bempeg, especially because I know that CRs is kind of what they saw and that’s what their dose-limiting toxicities were I believe. So what types of DLTs would you expect now for this drug, maybe something like a neutropenia or changes in blood count because with the non-alphas, we wouldn’t really expect to see vascular leak syndrome, right? And that’s something that obviously Proleukin struggled with. So I’m just kind of interested in kind of what you think we should be looking out for in terms of the drug safety profile going forward. Thanks.

Fahar Merchant

Great. Thanks, Matt. Thanks for your questions. So I’ll pass it on to Martin in just a moment, but with respect to the tumor types, as you recall, in the clinical trial during the dose escalation portion of the study, we had kept it open to a wide range of tumor types covering a pan tumor profile of patients. So not only have we included patients with metastatic melanoma in the study so far in the first eight patients, we’ve seen patients as you’ve — as I’ve noted, patients with pleomorphic sarcoma, again, metastatic version of that tumor. We’ve also had patients with pancreatic ductal adenocarcinoma as well as patients with squamous cell carcinoma of the tonsil, et cetera.

So it’s a mixed patient population and as we plan to proceed with the dose expansion phase of the study, we will be focusing very much on metastatic melanoma and renal cell carcinoma with potentially another group of patients that we may — as we see these patients beginning to see benefit during the dose escalation will include that cohort of patients as well. So we haven’t finalized on the sort of the third group of patients that we may include. But clearly, as you said, you’re right. When you look at both the sarcoma is that we’ve seen patients have tumor control, that’s encouraging sign considering these patients had rather large tumor masses of over 20 centimeters in total.

So with that, we — I will pass it on to Martin, who can sort of give you a bit of background on the safety features of the drug and what we are seeing so far. Martin?

Martin Bexon

Sure. Thanks, Fahar. I think you’ve described it well as with a lot of these first-in-human studies in the lower ranges of a dose range, we do tend to throw the neck cell wide in terms of tumor types and/or to expedite that early stages of study where we’re not really expecting to be able to look all that definitively at clinical efficacy with safety being dose limiting consideration. And as such, yeah, as Fahar said, we’ve had a bit of a mixed bag. We certainly had a [indiscernible], but also head and neck cancer, upper GI coupled sarcoma, as you know, not at all atypical in terms of, let’s say, early-stage dose ranges, and we will look to narrow that down as we go into the doses where we might expect to see certain clinical effects.

Matt Biegler

Then maybe just a comment on the safety profile?

Fahar Merchant

I think it seems like Martin’s line is not coming through. But — so basically — sorry, Martin, can you — okay. So I think you are sort of cutting off. Let’s see if you can — the question was about what sort of expected safety features of DLTs, we might expect, yeah.

Martin Bexon

What we’ve seen so far in terms of toxicities, and it is an emerging pattern, I would say, is consistent with that, that we’ve seen with a whole range of immuno-oncology agents by way of without terms of infusion reactions, patients with fevers, with chills and light cold, sometimes some abdominal [indiscernible] intestinal upset and I think this is a past uncertainly in terms of severity, it is consistent with that those I’ve seen for a whole range of this in process of immune active drugs whether those are bispecifics or monoclonals or across the families really. And what the investigators are telling us are, these have not been a worse events in terms of the clinical experience to date. These are things that are managed easily in the normal work setting of the clinic with simple measures. And so to date, that pattern is reassuring, I think. And as I say, consistent with multiple classes of immuno-oncology treatment.

And what do we expect to see by way of DLTs? Well, I think as you acknowledge, the step-up dosing is designed to minimize the risk of seeing that. And I think what we might end up doing is reaching a biologically effective dose without having seen dosing toxicities. So I think if we stay on top of things in the way that we have done to date and that would be my hope that we would go maybe one or two further dose steps. But what we’re already seeing in terms of the levels of activity pharmacodynamically suggest that we wouldn’t need to go a whole lot further than that. So quite possibly, we won’t be in a toxicity limited status when we expand for the next phase of the study.

Dan Ferry

Okay. Thank you, Martin.

Operator

Thank you. Our next questions come from the line of David Martin with Bloom Burton. Please proceed with your questions.

David Martin

Hi. My first question is, could the fever be an early sign that you will see vascular leak syndrome or is it disconnected from BLS?

Fahar Merchant

Martin, your thoughts on that?

Martin Bexon

Yeah. I think it’s a non-specific finding. As I say, it’s — the pattern and the severity are more consistent, I would say, with the general IRR pattern seen across multiple classes of IL drug, but that isn’t to say that it’s impossible that some individuals might have features more consistent with BLS. Yeah, it’s a bit non-specific instead of periodic dose.

David Martin

But there was no sign of eosinophilia at these doses.

Martin Bexon

That’s correct. So far the eosinophilia counts have remained outside of the high-risk categories that have been described previously with IL-2 therapy.

David Martin

Okay. Next question. Have you taken any of the patients in cohort 4 to the third step-up dose and has the strategy being successful as far as reducing the tolerability issues?

Fahar Merchant

Yes. Sorry. Yeah, Matt, I just wanted to — David, just wanted to when you say cohort 4 to the next step up, can you clarify a bit more what you mean? So yes, we have patients that have gone through the priming dose and gone to the 660 microgram dose already. So that’s been the case. Is that what you mean?

David Martin

Yeah. How many of those patients has that happened with and are they tolerating the drug at 60?

Fahar Merchant

Yeah. So we have — as you know, we do have the first three patients in the study would be monitored for DLTs in this cohort 4 for that matter any cohort. And essentially, we’ve had — if I’m not mistaken, at least two patients that have gone through to the fixed dose of 60 micrograms and we haven’t seen any DLTs yet.

David Martin

Okay. Which cohort were the three patients with disease control? Were they all in the 30?

Fahar Merchant

So we had — in terms of — when you’re looking at target lesions, the first two tumor control patients were at the 10 microgram dose. We also had 1 patient in the 30 microgram dose, but in the 30 microgram dose, which was the third cohort, we had a total of four patients in that cohort. Out of those four patients, we had three patients with a target lesion was in sort of, call it, tumor control with these patients having signs of additional lesions showing up, but the target lesions had stabilization. So three out of four patients in cohort 3, so benefit on the target lesions with one of them not having any additional lesions showing up post treatment. So it’s too early to break it down, but we’ve seen, as I said, activity as early as the 10 microgram dose.

David Martin

And all the patients in the third cohort they have had scans at this point. Were there any shrinkage like disease control can include a wide range of response to the tumors? Was there any with shrinkage?

Fahar Merchant

Yes, they were.

David Martin

Okay. And are the patients still on the drug and what has been the duration of disease control?

Fahar Merchant

Yeah. We will provide more of that data we expect at a conference late in July. So we’ll hold off on all those other additional data for later on.

David Martin

Okay. And last question, in the third cohort, were there any melanoma or renal cell carcinoma patients who progressed?

Fahar Merchant

Again, we’ll sort of break it down in more detail at the conference so that we have the ability to compile more information for that conference and share those data, not only additional PK/PD data, but also the data on individual patient profiles, including type of tumors, tumor burden and some of the sort of the prognostic factors of each of the patients and what the prior treatments were, et cetera.

David Martin

Can you at least say what the third patient who had disease control, what type of tumor they had like two sarcomas and what was the drug?

Fahar Merchant

Yeah, one was melanoma.

David Martin

Okay. That’s it from me. Thanks.

Operator

Thank you. Our next questions come from the line of Catherine Novack with JonesTrading. Please proceed with your questions.

Catherine Novack

Hi. Thanks so much for taking my question. The first, I want to ask, can you remind us of what degree of lymphocyte expansion is associated with clinical responses in IL-2? And then given the low baseline count of the patients currently in the study, how translatable are these early dose escalation results? And then my second question is on the BiSKIT program, given the cash runway extending measures you are taking, can you give us an updated time line on getting the BiSKITs into the clinic? Thank you.

Fahar Merchant

That’s great. So with respect to answering your second question first regarding the BiSKIT program, as you know, we have just reported some data at the AACR meeting with the first BiSKIT that we’re working on, which is an anti-PD-1 IL-2 Superkine fusion. So that’s a program that we see quite a bit of interest and excitement around. The plans would, essentially for us at this moment in time, continue to optimize this particular molecule with respect to the anti-PD-1 domain. The work that we’ve done so far is obviously using a mouse version of the anti-PD-1.

So we will be looking to identify the right kind of potential partnering with a company that has its own human anti-PD-1. So until that happens, and we have completed additional optimization preclinical studies with the molecule version that would eventually go into the clinic, I would say, we are very early in the process to be ready for initiating a clinical trial any the next 12 months or so, perhaps more towards the end of 2023. So in that scenario, we are not looking at a situation where the impact of our work on the BiSKITs is going to materially impact the spend as it’s still very much a research project at the moment.

Now the other question that you raised was around the expansion of the lymphocytes, et cetera. You’re right. At the moment, we actually don’t — if you go back to data from other prior studies with Proleukin or others, there’s no confirmed correlation with respect to increases in population of specific immune cell types at least that’s demonstrated a correlation between changes in those population versus tumor responses, for instance. However, we have seen that with Proleukin, for instance, increases in lymphocyte counts of about two to threefold are associated with better outcomes with respect to tumor response and so on. We’re already seeing that with MDNA11, although I must say that the baseline counts of these patients have been low. We have — as of our sort of going forward with future cohorts, we’re sort of screening for patients that have a better lymphocyte count baseline.

As you know, most of the work that has been done with Proleukin and other competing agents out there, you’ll see typically that the baseline lymphocyte counts tend to be well above 1,000. That’s what we would hope to enroll patients in doing dose escalation going forward at these high doses, including doing the dose expansion so that we can get the patients to benefit the most from the drug. So we expect the effect of MDNA11 to be a lot more pronounced going forward as we enroll patients with baseline counts that are more typically used in immunotherapy patients, et cetera. I don’t know, Martin, if you want to add any more to that?

Martin Bexon

No, I don’t really have an awful lot. I mean, I think we’re continuing to analyze this data and to look at subpopulations. I think going forward, we have a couple of additional biomarker presentations in the calendar that we will aim to provide a bit more insight as we go.

Fahar Merchant

Right. And I think what we are really very encouraged about is seeing the level of tumor control in these patients despite that the baseline lymphocyte counts have been much lower than what would normally be the threshold baseline count. So that’s for us a really compelling with respect to the kind of increases we have seen and also to see tumor control at these levels despite the fact these patients have very poor pretreatment or baseline lymphocyte counts or CD8 T cell counts, NK cell counts, et cetera.

And despite that, what we’re seeing in these patients who are heavily pretreated have large tumor burdens to see tumor control is for us, I think, at the moment, looks really exciting, particularly as we climb ahead with the higher doses that we are expecting to see and enroll patients that have a much more reasonable baseline lymphocyte counts in the clinical trial. So look forward to, I would expect much greater increases in actual populations of the CD8 T cells, NK cells going forward instead of the first three cohorts where the lymphocyte counts were generally much lower at baseline.

Catherine Novack

Got it. Is that something that we can expect to see starting in cohort 4? Or can you give me a little bit more granularity on that?

Fahar Merchant

I would say that we’ve set up the protocol. The amendment has now been approved with all three regulatory agencies so that we expect that in cohort 5 onwards. And of course, into those expansion phase as well, yes.

Catherine Novack

Yeah. Got it. Appreciate it. Very helpful

Operator

Thank you. Our next questions come from the line of RK with H.C. Wainwright. Please proceed with your questions.

Swayampakula Ramakanth

Thank you. Most of my questions have been answered with that. Just two general questions and probably you have given answers to these already, but I’m just trying to make sure. So for this cohort 4 in the ABILITY where you’re going to be priming with two doses, I’m assuming these are increasing doses like dose level 2 and 3 so that you can increase the exposure before you go to dose four. So is that yes or no, is the dose two and dose three? And also, what’s the timing interval between the two planning doses and before you get to the final to the fixed dose?

Fahar Merchant

Yeah. So just to give you a bit of background here that the first two priming doses as are at 30 microgram per kilogram dose. And it is at a dose that is — as we’ve seen so far at a dose which is clinically beneficial for the patients. So we are not dosing patients at much lower doses. We’ve actually seen tumor control at the 10-microgram dose. And therefore, the 30-microgram dose, although we call them priming doses, I would say that those 30 microgram doses are substantially effective in stimulating the immune system very profoundly. So that’s really one of the first things that we are doing here.

And then moving on to the 60-microgram dose, the interval between treatments has not changed. That’s every two weeks, irrespective of whether it’s a priming dose or once reduced the fixed dose. So the dosing regimen has stayed at once every two weeks. Does that answer your question, RK?

Swayampakula Ramakanth

Yeah. Fantastic. Then the other question I have is from the data that you have seen so far in various tumors and also the data from your competitors, what type of tumors do you think are a good target for MDNA11 outside of the two that you’re planning on right now?

Fahar Merchant

I would say that what was very surprising for us to see a stable disease in sort of patients with sarcomas, both of these are aggressive forms of sarcomas, rare kind of sarcomas and therefore, considering that these patients had baseline large tumor burdens to see tumor control was very encouraging in that patient population. As you know, sarcomas are not generally used with IL-2, neither have — are they sort of generally used with different immunotherapies or checkpoint inhibitors. So that was a novel new finding that we found very encouraging.

Going forward, of course, we’ll continue to enroll as our protocol mandates that will be enrolling patients with different tumor types. However, the focus will have to be on tumor types that generally respond or have a prior history of responding to checkpoint inhibitors, for instance. So that’s going to be sort of our expectation that patients with prior exposure to checkpoint inhibitors or patients that would normally qualify for immunotherapies would likely do even better. So as we continue to enroll patients going forward, we will be more selective in making sure that the patients that are enrolled in the study are those patients that normally do respond to immunotherapies rather than those patients that have no prior exposure to or immunotherapies have not been approved for those patients.

So we are sort of focusing on those tumor types that we expect the immune system to play a major role, although, as I say, in addition to sarcomas, we’ve had two patients with pancreatic cancer as well. We know that those patients typically again, would not respond to checkpoint inhibitors or other immunotherapies. So we are fine-tuning the patient population as we escalate the dose with the intent, of course, to get into the dose expansion phase with the right patient population that is likely to benefit most with immunotherapies, such as our drug, MDNA11.

Swayampakula Ramakanth

Perfect. Thank you very much for that color. Appreciate it and good luck.

Fahar Merchant

Thank you.

Operator

Thank you. Our next questions come from the line of Andre Uddin with Research Capital. Please proceed with your questions.

Andre Uddin

Hi, Fahar and Liz. Just wondering if you could give us a business development update on the licensing of MDNA55 and how that’s progressing? Thanks.

Fahar Merchant

Right. Yes. So as we put out in our press release, what we’ve done, and of course, in the call today, also mentioned that we have, as you know, earlier this year, completed a very comprehensive analysis that would be supportive of the commercial potential for MDNA55 with respect to conducting a thorough primary market research and adoption of MDNA55 at different hospitals across both Europe and U.S. following interviews with about 40 different KOLs, 20 in Europe, and 20 in the U.S.

And of course, also from a market opportunity, whether it’s us, ourselves, but nevertheless, for partner purposes, for collaboration, we needed to make sure what the pricing might be for MDNA55, which was something that we were able to complete as well as getting feedback from payers and insurance and reimbursement agencies to find out what kind of expectation there might be.

In all these cases, we’ve seen very positive feedback from these KOLs, from payers, from insurance companies, reimbursement agencies, et cetera, with respect to what the pricing might be. And that was really important for us to have in place, which we now have in place. And I would say that our interactions with potential partners address those — that bit of information that was not available. So it does give us additional two check boxes that we are progressing with.

But I think the other key feature of our discussions going forward with potential partners is the fact that localized administration of a drug is something that’s sort of discouraged potential partners in the past, administration of a drug intracranially is something that’s not out there. There is nothing approved until very recently, where Daiichi announced that they had a virus based therapy, which is being administered directly in the brain tumor as well, which was approved by Japanese authorities. So that third bit of information and has substantially improved the profile of MDNA55 from that perspective.

And also there is, as you can see, a consistent or increased awareness of using an external control arm in different oncology clinical trials. So over a period of this past several months, we’ve seen quite a bit of renewed interest on MDNA55, and we are progressing and advancing those discussions, and that process continues. And we’ll provide updates as we get closer to a time when we can make more meaningful announcements regarding a partner, but we are definitely fully engaged with the process at the moment.

Andre Uddin

Great. Thank you, Farah.

Operator

Thank you. Our next questions come from the line of Kumar Raja with Brookline Capital. Please proceed with your questions.

Shubhendu Roy

I’m Shubhendu for Kumar. Thank you for taking our questions. So with regards to the BiSKITs program, so how are you thinking about it, for the IL-13 MDNA413 and the MDNA109 programs, do you plan to test it further in non-human primates before taking it to the clinic? And if you can provide some color on the sort of implications you want to test it in? Thank you.

Fahar Merchant

Right. So as I mentioned earlier, the anti-PD-1 IL-2 BiSKIT, that particular molecule, as I said, so far, we’ve been working with the mouse version of anti-PD-1 to be able to demonstrate whether this concept or this approach is feasible, which we have done, of course. The next steps typically will be to identify the right human version of anti-PD-1 that we could fuse our IL-2 with, whether that comes with us bringing it into Medicenna, which is something we are not planning to do. Our preference is, of course, to work with companies that have checkpoint inhibitors.

So going forward, we’ll be looking at analyzing and approaching different potential collaborators that we can use or work together with their checkpoint inhibitors that are in the clinical already in the marketplace so that this sort of provides some additional comfort that we are not starting from scratch with a different checkpoint inhibitor and Medicenna clearly does not have a checkpoint inhibitor program. So that process will proceed. And as we’ve done in the past, including with our IL-2 Superkine program, particularly with MDNA11, we’ll generally take programs.

We like to identify an ideal candidate to take into the clinic. But sometimes you end up in situations where you have two molecules that are just as good as each other, and we might do some pilot non-human primate studies. But these are not being planned in the next nine months to 12 months. These are obviously further away from that point. But nevertheless, we expect that we would be in a position to pursue with IND-enabling studies towards the sort of the second half of next year with this bifunctional Superkines.

With the 413 molecule, we’ve seen that it works not only on itself, particularly in cold tumors, but also when combined with our IL — MDNA11 and therefore, there will be some additional optimization that we plan to work on, our 413 molecule is currently fused to the Fc domain. We expect to do further optimization with the right protein scaffold. It might be trying it with albumin for instance, et cetera. So again, that molecule, although, we have demonstrated proof-of-concept in mouse models, that molecule is again not quite ready for nonhuman primates or IND-enabling studies at this stage. There’s further work to be done, and we will continue to report more data at conferences with respect to these new optimized versions of both the BiSKITs as well as the MDNA413 molecular as well.

Shubhendu Roy

Okay. Great. Yes, that’s very useful. And just with regards to the ABILITY study, you were planning to do some combination studies with checkpoint inhibitors. So when do you think you could initiate those combination studies? And also when you recruit the patients, would they have fair CPI treatment or would they be naive? And any time line that you can share with that?

Fahar Merchant

Yeah. So the combination study is part of our Phase 1/2 ABILITY study at the moment. Once we’ve established the recommended Phase 2 dose, the next step, of course, is to conduct the dose expansion phase of the study with the single-agent monotherapy and that will help us identify which of the three different patient populations are benefiting in a single-agent setting. We certainly want to see single-agent activity. We want to see tumor responses. We expect that, that is a reasonable threshold for us to get there.

The plan is to combine MDNA11 with an anti-PD-1 molecule that’s already in the market. We will announce that in the future. And the plan is obviously towards the first half of next year would be the right time for us to proceed with initially optimizing the dose in the combination setting before we expand into the combination setting. So typically, what happens is, although we’ll have the recommend Phase 2 dose in a single-agent setting, it is very likely that we will — when we combine the two therapies and administer them at the same time, it’s not unusual to start at the RP2 dose minus 1 level in the combination setting before finalizing the dose in the dose expansion phase of the combination arm as well. So that’s more likely that I said in the first half of next year.

Shubhendu Roy

Thank you so much.

Fahar Merchant

You’re welcome.

Operator

Thank you. Our next questions come from the line of David Bautz with Zacks Research. Please proceed with your questions.

David Bautz

Hey. Good morning, everyone. Just one question on MDNA11 from me. For your pharmacodynamic results that you’ve seen so far with T cell and natural killer cell responses, have those been consistent across the different tumor types in the study or have you seen any other patient characteristics that kind of correlate with those responses?

Fahar Merchant

Yeah, patient — obviously, the number of patients is just eight patients, and therefore, difficult to make a judgment as to what correlations, if any, exists. But as I mentioned, we’ve seen changes or expansion of the CD8 T cells, NK cells, et cetera, across all different tumor types. So that is really encouraging. So it’s irrespective of what tumor type, but of course, each patient has a different baseline levels. So that might have some kind of an impact, but we haven’t got enough data at this moment. With data on just eight patients, it’s difficult for us to correlate those numbers with different tumor types, et cetera. So we would expect to get more data as we continue to enroll more patients and see if there are any trends coming through. I would expect that we’ll probably see more of that during the dose expansion phase of the study. We’ll be able to see more clearly if the PD changes are occurring based on other tumor characteristics or patient profile or not.

David Bautz

Okay. Great. Thanks for taking the question.

Fahar Merchant

You’re welcome.

Operator

Thank you. We have reached the end of our question-and-answer session. I’d now like to hand the call back over to Fahar Merchant for any closing remarks.

Fahar Merchant

Well, I would say thank you, operator, and thanks again to all of you who have joined us today. Clearly, we’re excited with the data that we’ve seen so far, although these are the early first three cohorts that are the lowest dose cohorts in the study so far as we escalate. We hope to see further benefit of MDNA11 in this difficult-to-treat patient population. So we will be providing periodic updates over the coming months on our progress. And finally, let me wish everyone a very good day. Thank you.

Operator

Ladies and gentlemen, this does conclude today’s presentation. Thank you once again for your participation. You may now disconnect your lines.