Q4 2022 DiaMedica Therapeutics Inc Earnings Call
Speaker 1: beep beep
Speaker 2: Good morning, ladies and gentlemen, and welcome to the Diomedica Therapeutics Remedy 2 update conference call. An audio recording of the webcast will be available shortly after the call today on Diomedica's website at www.diomedica.com.
Speaker 2: in the investor relations section.
Speaker 2: Before the company proceeds with its remarks, please note that the company will be making forward-looking statements on today's call. These statements are subject to risks and uncertainties that could cause actual results to differ materially from those projected in these statements.
Speaker 2: More information, including factors that could cause actual results to differ from projected results, appears in the section entitled Cautionary Note Regarding Forward-Looking Statements. In the company's press release issued yesterday and under the heading Risk Factors in Diamantica's Most Recent Annual Report.
Speaker 2: call speak only as of today, March 29, 2023, and may no longer be accurate at the time of any replay or transcript rereading.
Speaker 2: Diomedica disclaims any duty to update its forward-looking statements.
Speaker 2: Following the prepared remarks, we will open the phone lines for questions. I would now like to introduce your host for today's call, Mr. Rick Pauls, Diomedicus President and Chief Executive Officer. Mr. Pauls, you may begin, sir.
Speaker 3: Thanks, Paul. Hello, everyone. And welcome to our fourth quarter conference call. I'm joined this morning by Kirsten Grues, Archive Medical Officer, and the Director of the National Archive Medical Officer. I'd like to start off today. This is called by updating everyone on the status of our work to remove the clinical hold on a remedy to phase two slash.
Speaker 3: of switching to a new ID bag formulation in a Remedy 2 trial.
Speaker 3: In our prior Remedy 1 Phase 2 trial, the IV bag made from polyolefin retained up to half of the DM-199 drug.
Speaker 3: In our pivotal phase two slash three remedy two trial, we switch to the new PVC IV bag formulation, which does not retain any of the DM-109. Effectively, delivering up to twice as much DM-109 to study participants. We believe that this is what caused the transient clinically significant
Speaker 3: blood pressure drops, or hypertension in those three participants. In our initial safety studies, we identified hypotension as a dose limiting tolerability for DM-199. As a result, drops and blood pressure are consistent with the mechanism of action for DM-199.
Speaker 3: And we believe that the hypotensive events at least indicate that DM-19 is clearly active in patients. In the FDA's October Continue Full Clinical Hold letter, their most significant request was to expand our IV bag compatibility study to stimulate real-world usage, which is referred to as an in-use study.
Speaker 3: We had originally expected that we would need to request a Type A meeting with the FDA to discuss the requirements for the study. However, in December we received written communication from the FDA which provided their expectations for our in-use study. Since we're only entitled to one Type A meeting, we are pleased that this written communication is available to the FDA.
Speaker 3: Save this from having to use our type I meeting for a discussion on the in-use study requirements. We incorporated the FDA's feedback into the study protocol and submitted the updated protocol to the FDA with the request for confirmation that the protocol would satisfy the requirements. Last month, we received a follow-up notification indicating that the FDA believed
Speaker 3: that our in-new study protocol was reasonable.
Speaker 3: The in-use study is being conducted in two parts. Part one simulates actual use in the hospital with IV bag and the tubing using a pump to administer DM-19. Part two tests, worst case scenarios, such as varying storage, duration, temperatures, and light.
Speaker 3: The first part of the in-new study is complete and we believe that the data from this part confirms the conclusion we reached in our prior testing. Specifically, it confirmed that up to approximately 50% of the DM-19 was retained in the IV bags, used in the remedy one as compared to the IV bags used in the remedy two.
Speaker 3: and supports our earlier proposed revision to the IB dose from Remedy II from 1 to 0.5 micrograms per kg. These results have been submitted to the FDA along with a request for feedback and confirmation that we now have addressed all issues of the clinical hold once the part 2 of the in-use study is submitted.
Speaker 3: We are currently conducting part two of in-use study, and the results once complete will be submitted to the FDA, which we anticipate occurring in April . Note that part two of in-use study, what we learned will likely only affect handling procedures for the IV dosing and not the dose rates.
Speaker 3: Late last year and early this year, while we were awaiting feedback from the FDA on the in-use study protocol and preparing to run the in-use study, we developed a more sensitive assay for measuring K-O-K-1 levels and enhance the consistency in our assay that measures the activity levels of K-O-K-1.
Speaker 3: We chose to do this as the FDA had posed a question about our existing assay methods. While we believe our existing assays were reasonable, we decided to be prudent in ultimately less time-consuming to complete this work and eliminate a risk that the FDA might have additional questions and further delay the resumption of a remedy to trial. The FDA had also asked whether tripsum could be a potential cause for trial.
Speaker 3: to that trypsin was fully removed from the DM-189 during the manufacturing process. This testing confirmed that there is no, or at least not detectable, residue trypsin in DM-199. In February , we submitted reports to the FDA confirming that trypsin was not measurable in DM-199 and provided the update validated methods assays to the FDA for review.
Speaker 3: We recently received their feedback that the assays developed appear appropriate and our assessment of trips and levels is also acceptable. At this point, I'm pleased to say that we believe we have a good ongoing dialogue with the FDA. We appreciate their engagement and we are confident that an end is in sight to our clinical group.
Speaker 3: Note that the FDA has up to 30 days to review and respond to our complete response letter requesting the lifting of the clinical hold. Once we receive the response, we will provide an update on expected timing for getting Remedy 2 restarted. Yesterday we also announced that we have initiated a Phase 1C Open Label.
Speaker 3: single ascending dose study of the IV dosing of DM-19 in the IV bags made from PVC used in the Remedytu trial. This was not requested by the FDA but as a proactive measure on our part decided before starting the in-use study. We chose to do so for two primary reasons. First,
Speaker 3: For some reason, the FDA is not satisfied that the results of the in-use study provided sufficient basis for adjusting the IV dose levels going forward in remedy two, then the results of the Phase I C study will conclusively demonstrate the serum concentration levels of D-29 achieve with their proposed IV dose.
Speaker 3: The second reason has to do with driving confidence in the physician investigators. This study demonstrates our commitment to the patient safety. I mean, I hope that will help us start strong when we resume enrollment in Remedy 2. Enrollment in Phase 1C study began last week in the first three cohorts.
Speaker 3: which gets us to 0.5 micrograms per kg dose level, we propose to use going forward. Should be complete in April with preliminary data available in May.
Speaker 3: I would like to also recognize and give a special thank you to our clinical team for getting this study designed, planned, and initiated in a remarkably short period of time.
Speaker 3: We've learned a lot through this process, and as a result, the diamanica will come out stronger and better prepared to resume trial activities once cleared by the FDA to do so.
Speaker 3: This is also due in no small part to some key additions to our management team in 2022. Dr. Kirsten Gruus, our chief medical officer, is aboard certified neurologists with extensive experience in medical practice and drug development in bringing several drugs through FDA approval.
Speaker 3: Kirsten has also been instrumental in leading the response to the FDA and managing our FDA communications.
Speaker 3: Dominic and Dari, our Chief Commercial Officer, you will recall he managed the TPA franchise at Jettentech for 30 years and came out of retirement to join Di America because of his passion for the stroke community and the potential benefits of DM199. We also added significant late-phase clinical operation expertise.
Speaker 3: with Julie Dave's Senior Vice President of Clinical Development Operations, bringing vast experience in clinical trial planning and execution and has a reputation for completing trials on time and under budget.
Speaker 3: In addition, at the board level, we recently announced that Tanya Lewis has joined us. Tanya's extensive global regulatory expertise. This includes positions as chief development officer, chief regulatory officer, and chief quality officer. She has been involved with other clinical hold situations and has been responsible for several products making their way through.
Speaker 3: the regulatory approval process with the FDA. It's a privilege to work with these individuals and entire Diematica team. As you can tell here this morning, we look forward to getting out from under this clinical hold and resuming the development of DM-1-9 to bring this important treatment to distro patients. We see a bright horizon with the team we have built.
Speaker 3: and we will continue to grow as we move forward. One additional point that I'd like to make this morning, an important rationale for developing DM-19, a synthetic form of the KELKI1 protein, is the current usage of the KELKI1 protein in China. As many of you know, in China, a form of the KELKI1 protein is isolated from human urine. That product is called the KELKI.
Speaker 3: has been treating patients for over a decade now. In 2019, Cali-Kang was added to the National Reimbursement Medicine List. This spurred a dramatic increase in usage in China. There were more than 600,000 patients treated for stroke in 2021 alone.
Speaker 3: To put this into perspective, that's approximately 15% of the estimated 4 million annual strokes per year in China. This gives us extensive knowledge of the KELKI-1's clinical use and even more confidence that our recombinant form of the KELKI-1 therapy can bring this much-needed treatment to the
Speaker 3: and the rest of the world for patients who today do not have a treatment option.
Speaker 3: I would like to now turn over the call up Scott Callan to review the financial highlights.
Speaker 4: Thanks Rick and good morning everyone. As Rick mentioned, we announced our full year 2022 financial results and filed our annual report on Form 10K yesterday afternoon. These documents are both available on either the Diametic or the SEC websites. Starting with our balance sheet as of December 31, 2022.
Speaker 4: Our combined cash and investments totaled $33.5 million, down $2.6 million from $36.1 million as of the end of Q3 2022, and down $11.6 million from $45.1 million as of our prior year-end. This is a cash viral because we got a lot of wealth by the time882 was released.
Speaker 4: Our 2022 cash usage was 11.6 million compared to 12.3 million in the prior year, and our cash usage was lower than planned due primarily to the halting of the enrollment in our remedy to trial. This should scale back up as we complete our response to the FDA and prepare for resuming enrollment.
Speaker 4: And, Sir Rick mentioned we intend to provide an update on the timing for the resumption of the trial in the near future.
Speaker 4: We also reiterate that we believe our current cash will support the clinical development of DM-199 and our operations into the fourth quarter of 2024.
Speaker 4: Our research and development expense is decreased to 7.8 million for the year ended December 31, 2022, down from 8.8 million for the full year of 2021.
Speaker 4: This decrease was driven primarily by reduced costs incurred during 2022 for the wrap-up of our Redox Phase II CKD trial.
Speaker 4: and decreased non-clinical testing costs, a significant amount of which were incurred during 2021 in preparation for initiating the Phase 2-3 Remedy 2 trial in 2022.
These decreases were partially offset by increased personnel costs associated with expanding our RD operations and increased manufacturing process development activities.
Our general and administrative expenses were 6.2 million and 4.9 million for the years ended December 31, 2022 and 2021 respectively. This increase was primarily driven by increased directors and officers liability insurance.
Increased personnel and professional services costs to support our expanding clinical programs, and increased legal fees for our lawsuit against PRA.
These increases were partially offset by reduced non-cash share-based compensation costs. With that, let me turn the call back over to Rick.
Thanks, Scott. With that, we'd like to open the call for questions. Paul, if you could please introduce the first analyst.
If you would like to ask a question, please press star 1 on your telephone keypad now. You will be placed into the queue and the order received.
Please be prepared to ask your question when prompted.
Once again, if you have a question, please press star 1 on your phone now.
And our first question comes from Thomas Fletten of Lake Street Capital.
Your line is open. Good morning. Thanks, guys, for taking the questions. Just a couple of questions on the Phase I C study. Was that protocol developed in conjunction with FDA? Or is this something you did completely independently as kind of a backup, a backup data set?
Hi, so I'll take that question. This is Kirsten. We developed it independently, the protocol, in our, was your last response to have in our back pocket. But we explained our situation to the...
the sites and the local ethics board in terms of what we wanted to measure in that study. And in fact, then we can, our previous phase one trial we did, that we did using the polyulphaline bag, we basically are going to be able to compare that data with this new data and just confirm.
that we have the right dose range.
And is there any risk that a normal, intensive patient would suffer a significant blood pressure drop outside of what you might see in a stroke patient?
No, we wouldn't expect that because the prior phase one that was done with the polyolophane bags that were mentioned, there were no problems with healthy volunteers who were normal intensive having lower end of their blood pressure.
And then one final one, Rick, you mentioned that FDA has 30 days to respond to your final response. And if I'm reading the press release correctly, that response will go in in April , so May would be the timeline for response on whether or not you've...
if you've satisfied their outstanding questions. Yeah, as soon as we have the part two of the in-use study, and that's already initiated, it's a few weeks for that study to be completed. So as soon as we have that completed, we'll submit, and the FDA will then have up to 30 days.
I think we're encouraged by the fact that over the last few months, we've had a good dialogue. We've been able to submit data along the way and then getting positive feedback. So I think this will be helpful instead of waiting to the end and submitting everything together. Thanks. Thanks for taking the questions.
that over the last few months, we've had a good dialogue. We've been able to submit data along the way and then getting positive feedback. So I think this will be helpful instead of waiting to the end and submitting everything together. Excellent, thanks for taking the questions. Thanks Thomas.
Thank you. Our next question comes from Alex Nowak from Craig Hallam Capital Group.
Your line is open. Okay, good morning everyone. I think last call we had, I think there was...
something some strong confidence at the time that we weren't good in the other safety study in patient and now we're lost in the phase one C study. So, you know, was there something that you saw in the end use study, anything in the FDA commentary that ultimately led you to say we want to have this in our back pocket? Like, what's changed here from the last call we had in October ?
It's just for additional level of competence, Alex. So we initiated the Phase 1C. We started planning this well before even starting the in-use study. And so part of also the rationale is that when we were looking at some different scenarios...
we actually were able to find a clinical site in Australia that had a slot open.
that allowed us to get this study up and going quickly. So at this point here, we anticipate to ideally having the results in early May. And while we didn't want to be in a situation that we run the in-use study, and for some reason we see something unexpected, and then we'd have to go back and run a Phase 1C trial.
that could then put this out until this fall. So I think it was an important step here to giving us some comfort, backup plan, and then importantly it also helps with just providing some confidence for the sites that we're taking patient safety very importantly and will give us just some additional data here to support this trial.
Australia, go back a couple years ago. So I mean, I know we don't have a clear answer on that, but what's the risk of the FDA, even when you provide all this information back to them, they say, okay, fine, but we'd like you to do another Phase II study before relaunching this Phase II slash Phase III study. Sure. So the initial Phase I study we did support the Phase II for stroke.
That study was really designed on the IV portion was to match the drug level, so the PK profile, to what's been shown with the calicang, the human urinary form. So we did that with the polyoform bag and then we went to our phase 2 trial and we used the same bag.
And so then what we discovered here is that close to half the drug was sticking. We went and pivoted to the phase 2 slash 3 with a PVC bag and, you know, effectively we were overdosing by twofold. So we've now confirmed this now two studies, the IV bag study we did last fall.
and then now with the in-use study. So we feel that for us and patient safety, we think we've identified the right range, but we're gonna also have this data here in really a matter of weeks from this additional phase one trial that's ongoing. Okay, and walking through it like that, I think that makes sense.
I think that should be a good argument to the FDA. Final question here, once the clinical hold is lifted, maybe it's in the May timeframe, how quickly can you reactivate sites and start enrolling patients? Are you really starting from square one there, or can you decide to activate or reactivate relatively quickly?
Before we had the clinical hold, if you're looking at clinical trials like that, we had 15 sites. Really, we're going to do all we can to get that up and going. I think importantly, with having Kirsten and Julie joining our team since last year.
I think we're going to be in a lot better position here to get this study up. It's going to take a little bit of time, but I think importantly after we get it up and running, we've been doing a lot of work since then and just getting all of our documents and materials cleaned up and in really good shape. So as soon as we get off, after we get off the clinical hold, we'll provide an update here in terms of some of the timings.
Okay, appreciate the update. Thank you.
Thanks Alex.
Thank you.
And our final question comes from Francois Bicibos.
of Oppenheimer, your line is open.
Hi guys, this is Dan on for Frank. Thanks for taking my question. Just to follow up from the other 2 on the phase 1. Could you share some color on the doses that you are going to be using?
using in the single-accenting dose study. I believe the original phase two, the original plan for the Remedy 2 was to use both one microgram per kilogram and three microgram per kilogram. So just in terms of what the maximum dose that you're testing in this study. Thanks.
Sure, so there's two doses. So the first is the IV dose that's being tested in the Phase I-C. So maybe just a step back for a moment. So when a patient has a stroke to come into the hospital and they will get the IV dose of D-M-19. So in our Phase I-C we're planning three initial doses of 0.1, 0.25, and 0.5 micrograms per kg. Okay.
We believe the 0.5 will be the dose that we're using based upon the in-use data, the IV bag study and in our previous work.
And then that's followed then clinically with subcutal dosing and that's at three micrograms per KG. And there's no change in that. So the subcutal dosing occurs twice a week for three weeks and then I'll get three micrograms. And there's no impact on that dosing with this hold.
Great, that makes sense. Thanks for taking my questions. And we have no further questions in queue. I'll turn the call back over to our house.
All right, again, we'd like to thank everyone for joining us this morning and for your continued support. The goal of bringing this important treatment to stroke patients is as quickly as possible. We appreciate your interest in Diomedica and your continued support. And this concludes our call today. Thank you.
That concludes today's conference call. Thank you for joining and have a pleasant day.