Greetings, welcome to the PolyPid fourth quarter and full year 2022 conference call. At this time, participants are in a listen-only mode. As a reminder, this call is recorded. I would now like to introduce your host for today's conference, Brian Ritchie from LifeSci Advisors. Mr. Ritchie, you may begin.
Thank you all for participating in PolyPid's fourth quarter and full year 2022 financial results conference call. Joining me on the call today will be Dikla Czaczkes Akselbrad, Chief Executive Officer of PolyPid, Ori Warshavsky, Chief Operating Officer for PolyPid's U.S. operations, and Jonny Missulawin , PolyPid's SVP Finance. Earlier today, PolyPid released financial results for the three and 12 months ended December 31, 2022. A copy of the press release is available in the investor section on the company's website, www.polypid.com. I'd like to remind you that on this call, management will be making forward-looking statements within the meaning of the federal securities laws.
For example, management is making forward-looking statement when it discusses the regulatory pathway for the potential NDA submission for D-PLEX100, including the potential of the SHIELD I results and SHIELD II study to provide support, the potential for wide use of D-PLEX100, the timing of resumption, completion of patient recruitment, the design and top-line results of the revised SHIELD II study, the company's expectations regarding its cash runway and financing opportunities, goals for 2023, including with respect to interactions with European regulatory authorities, its ability to attract additional partners and then enter collaborations and the potential timing thereof, and the expected timing for the commercial manufacturing process and packaging validation for D-PLEX100. Forward-looking statements are subject to numerous risks and uncertainties, many of which are beyond our control, including the risks described from time to time in our SEC filings. Our results may differ materially from those projections.
These statements involve material risks and uncertainties that could cause actual results or events to materially differ. Accordingly, you should not place undue reliance on these statements. I encourage you to review the company's filings with the Securities and Exchange Commission, including, without limitation, the company's Form 20-F, which identifies specific factors that may cause actual results or events to differ materially from those described in the forward-looking statements. PolyPid disclaims any intention or obligation, except as required by law, to update or revise any financial projections or forward-looking statements, whether because of new information, future events or otherwise. This conference call contains time-sensitive information and speaks only as of the live broadcast today, February 8, 2023. With the completion of those prepared remarks, it is my pleasure to turn the call over to Dikla. Dikla?
Thank you, Brian. On behalf of our team at PolyPid, I would like to welcome everyone to our fourth quarter and full year 2022 earnings call. Before discussing the details of our clinical program, I would like to reiterate how thrilled we are to now have a clear regulatory pathway for the potential NDA submission for D-PLEX100 in the U.S. following a positive Type D meeting communication with the U.S. FDA on the SHIELD I Phase III data. As a reminder, in advance of the Type D meeting, we provided the FDA currently available data from the SHIELD I study evaluating D-PLEX100 in abdominal colorectal surgery.
Based on these data, particularly the 54% reduction observed in the primary endpoint in a pre-specified subgroup analysis of 423 patients with surgical incisions greater than 20 cm compared to standard of care, which represented a P value of 0.0032, the FDA acknowledged that the SHIELD I result may provide supportive evidence on this population. The agency also recommended that the company conducted an additional study to support a potential NDA submission. The FDA confirmed that the ongoing SHIELD II study, which to date has enrolled approximately 40 patients with the appropriate large surgical incision, could potentially serve as such a study. Importantly, the FDA also recognized that since D-PLEX100's proposed indication is for the prevention of infection, it has potential for wide use.
While we are currently working expeditiously to finalize the design of the revised SHIELD II trial and expect to resume patient recruitment next quarter, we wanted to take the opportunity today to provide some color around what that study will look like. First, we view SHIELD II as a de-risked Phase III trial, giving the more focused patient population in which we have already generated highly positive data in SHIELD I and the fact that it will not be conducted within the tight COVID-related restrictions that were in play during the pandemic and throughout the duration of SHIELD I. Moreover, we have the opportunity to leverage the key learnings from the SHIELD I study, notably with regard to countries and specific sites and patient profile.
In order to ensure we are appropriately leveraging these key learnings, we conducted a clinical advisory board meeting late last year to gather clinical feedback from key U.S. opinion leaders specialized in SSI, including both surgeons and infectious disease specialists. We intend to recruit a total of approximately 600 patients or an additional 550 subjects behind the 40 patients already recruited into SHIELD II. Total recruitment time into the study is expected to be approximately 12 months from the time we resume SHIELD II enrollment next quarter. Topline results are expected mid-next year, three months from completion of enrollment. I would highlight that this anticipated timeline is similar to the one seen in SHIELD I. We also plan to conduct an unblinded interim analysis once a total of approximately 400 patients complete their 30 days follow-up.
To put this in context, you will recall that it took us 22 months to recruit 977 patients into SHIELD I, and it was during the most challenging period of the COVID pandemic. Importantly, the ability to leverage the ongoing SHIELD II study will significantly reduce the time and resources needed as compared to having to initiate a new trial. The design of the SHIELD II trial will be very similar to the SHIELD I study in terms of primary and secondary endpoints, with patient intervention arm receiving D-PLEX100 on top of standards of care and subject in the control arm receiving standards of care alone. The primary endpoint of the trial will be a combination of SSI re-intervention and mortality rate at 30 days post index surgery as defined in the CDC SSI guidelines. Patient safety will be monitored for an additional 30 days.
The study will take place in the U.S., EU, and Israel. In Europe, as we have done with the FDA in the U.S., we are also preparing for expected near-term interactions anticipated in the first half of this year with the European regulatory authorities regarding D-PLEX100. I should add that we are working closely with our European partner, ADVANZ PHARMA, with regards to the EU pathway and are fully aligned on the regulatory strategy for this region. In regard to our financial position, we continue to expect our current cash runway to extend well into the third quarter of this year. With that said, we anticipate having a number of compelling financing opportunities to enhance our balance sheet in 2023 and to fund SHIELD II to a successful completion. We are grateful for the continued support shown by our largest institutional shareholders.
Moving on, we have a number of operational goals in 2023. I will now ask Ori to review those. Ori.
Thank you, Dikla. We view 2023 as a potentially transformational year, not only in the clinical and regulatory areas, but also on business development and manufacturing fronts. From a business development perspective, first, we intend to focus on attracting additional strong partners for D-PLEX100 in different geographic territories like U.S. and China. Second, SHIELD I validated the PLEX technology platform in a large clinical trial, providing local and controlled release of drug molecules directly at the disease target organ over a predetermined period of time. This validation of the platform can serve as a starting point for platform-related collaborations. Importantly, we have in-house research, development, and GMP manufacturing that can support various potential partnership opportunities. Using our in-house capabilities, it is a matter of only months to encapsulate new API into the PLEX platform and achieve proof of concept.
PLEX platform collaborations will be focused on two key areas. The first, the delivery of innovative drug, specifically local delivery, where systemic delivery is either not effective enough or too toxic, for example, in oncology. Second, the lifecycle management of an approved drug where prolonged local delivery provides significant clinical benefit. Specialty companies are always looking to differentiate their existing product portfolios, and leveraging the PLEX technology is an excellent way to accomplish this. Our planned objective is to formalize two partnerships in 2023, although the exact pace of partnership discussion is inherently difficult to predict. On the operation side, we expect to complete the commercial manufacturing process validation and packaging validation for D-PLEX100 in the first half of this year. We plan on having the CMC and preclinical data needed to support an NDA submission by the end of the year.
With that, it is my pleasure to turn the call over to Johnny to review our current financials. Johnny.
Thank you, Ori. As of December 31, 2022, the company had cash equivalents and short-term deposits of $12.6 million, as compared to the $32.2 million at the end of 2021. Now let's turn to our income statement. Research and development expenses for the three months ended December 31, 2022 were $4.7 million, compared to the $9.6 million in the same three-month period of 2021. The decrease in R&D expenses resulted primarily from the completion of the SHIELD I Phase III clinical trial. For the full year ended December 31, 2022 and 2021, R&D expenses were $28 million and $30.6 million, respectively.
Marketing and business development expenses for the fourth quarter of 2022 were $350,000, a decrease from the $1.1 million during the prior year period. General and administrative expenses for the fourth quarter of 2022 were $1.6 million, compared to the $2.9 million recorded in the same three-month period of 2021. For the fourth quarter of 2022, the company had a net loss attributable to ordinary shares of $6.5 million, as compared to the $13.5 million in the fourth quarter of 2021. For calendar year 2022, the company had a loss attributable to ordinary shares of $39.5 million, compared to a loss of $42.6 million in the full year of 2021. We will now open the call to your questions. Operator.
Thank you. To ask a question, you will need to press star one and one on your telephone and wait for your name to be announced. To withdraw your question, please press star one and one again. Once again, if you would like to ask a question, please press star one and one. We will now go to our first question. One moment, please. Your first question comes from the line of Brandon Folkes from Cantor Fitzgerald. Please go ahead. Your line is open.
Hi. Thanks for taking my questions and congratulations on the progress. Maybe just a few from me, if you don't mind. Maybe just as we think about SHIELD II, can you just elaborate in terms of how you control for the potential of a lower infection rate in the comparator arm? Similarly, how do we think about the health economic benefit? Assuming we are successful in SHIELD II, you know, how do we think about the proposition to hospitals when commercializing the product in this sort of larger incision surgeries? You know, just any pushes and pulls there. Maybe just I'll ask also, yeah, Fran, if you don't mind. On the interim analysis, what should we expect there? Any chance of stopping early? Thank you.
Brandon, first thank you for joining us and good morning. I will start with the first question around the infection rate and how we look at it in terms of SHIELD II, and then I'll let Ori elaborate about the health economic, and I will also cover the aspect of the interim. First of all, what we've done, we now have a very robust data of close to 1,000 patients, which is the basis for our assumption. Although it was all conducted during COVID, and we mentioned several times that this had an influence on the infection rate, we are taking what we've seen in this period, although might be a bit conservative as our baseline assumption.
This is also when we're talking about the de-risk program, from our perspective, this is another aspect of why we think this is a de-risk Phase III, because we are taking on the assumption infection rate that were during the two years of COVID. There are a number of papers showing that there was a reduction in infection during this time, and this is a plus obviously that we're taking with it. Other than that, and we referred to it briefly in today's prepared remarks, we've done a process to evaluate as many as the lesson learned that could be taken both internally but also with external advisor.
We had, at the end of last year, a clinical advisory board trying to evaluate and look at the patient population, many parameters that were reviewed, and some of them are also potential health economics, and how-In the future, surgeon, hospital would look at the product, but also looking at the specific country, specific centers. All of these parameters are now into the protocol as well as into the operational planning. As to the interim. The interim is, has obviously a possibility for an early start due to efficacy, also sizing modification as well as if things are not as we expect, stopping for futility.
It's a, it's a full interim and we do have prior to the interim we also have some, as we did also in SHIELD I, blinded assessment that can help us refine things as we go along. Ori, you want to touch the aspect of the health economics?
Yes. Hey. Hi, Brandon. Good morning. I think what we see in this trial is the story itself hasn't changed from a health economic. If anything, we just even made it a little bit more clearer to the hospitals. We're now better defined the population. We make it easier for the surgeon to understand where the potential issue is, right? If a patient comes in with other, either patient-related risk factors or a procedural-related risk factors, the surgeon can flag this as this is a patient in risk and apply D-PLEX.
When a hospital kind of assesses the risk factor or where the problem is, I think we're making it a little bit more clear for them. As before, right? When there is an infection, there's additional costs from additional time in the hospital, reintervention, readmissions and so on. We just. If anything, we just made the story a little bit clearer to the hospital.
Great. Thank you for all the color and best of luck.
Thank you.
Thank you.
Thank you. We will now go to our next question. One moment please. Your next question comes from the line of Balaji Prasad from Barclays. Please go ahead. Your line is open.
Hi, everyone. Good morning. This is Shaw from Balaji. Thanks for taking our questions. You mentioned that it took about 22 months to recruit 990 patients for SHIELD I and for SHIELD II. Given that the, you know, patient eligibility criteria could be different for the two trials, what is your expectation on timing of the patient enrollment for SHIELD II? Thank you.
First of all, good morning. Thank you for this question. We were very clear on that. We expected the recruitment time will be 12 months. This is also what we've done here. We've also looked at the pace of recruitment of patient in SHIELD I, those specific more focused population, what was the pace during SHIELD I, and how fast we got to those numbers and extract from that.
We, by the way, we are hopeful that we'll have a faster rate, although again, our assumption were based on what we've seen in SHIELD I, because we need to remember, SHIELD I was completely conducted during the COVID time, which obviously slowed down processes in terms of opening centers as well as patients going and taking surgeries and having laparoscopy tests and then getting surgery when needed. All of those points slowed down recruitment, but still at the end of the recruitment, we had around 250 patients per quarter, and close to 45% out of those patients were patients with incision length of over 20 cm. This can give you a sense of what's our expectation in terms of recruitment at the peak.
Got it. This is very helpful. Thank you.
Welcome.
Thank you. Once again, if you would like to ask a question, please press star one and one on your telephone and wait for your name to be announced. To withdraw your question, please press star one and one again. We will now go to our next question. Your next question comes from the line of Roy Buchanan from JMP Securities. Please go ahead. Your line is open.
Hi. Thanks for taking the questions. I guess just to follow up on the, on the last few questions. I wanna make sure I'm clear on the, what's the pre-specified patient group for the, for the primary endpoint in SHIELD II? Incision over 20 cm. Are there any other criteria? I think you just said, Dikla, but I kinda missed it. I think you had about 200 patients in SHIELD II and 40 with a large incision, implies about 20% with the appropriate criteria. Is that accurate? Thanks.
Hi, good morning, Roy. Yeah. First, yes, this is right. We had about 20% of the SHIELD II meeting the pre-specified criteria or the more focused population that we are targeting in SHIELD II. I'll just remind everyone that SHIELD II originally had a broader eligibility criteria. It wasn't just open abdominal colorectal, but also minimally invasive. It makes sense that you wouldn't see the same ratio of large incision that we've seen in SHIELD I. This is why in SHIELD I, we had around 45% of the patients having longer incision, and in SHIELD II, with the 200, it's about 20%. Now that we are focusing the trial based on the FDA feedback, we expect to see this number growing. You had another point that you wanted to cover, Roy?
Yeah.
The eligibility.
Right.
The change in eligibility. Yeah.
Yeah. Exactly.
Same type of surgery, same patient population that we had in SHIELD II. We are just focusing on the subgroup, the pre-specified subgroup that we had in SHIELD I, which was the longer incision, where we received a P value of 0.0032, and also discussed this with the FDA, and the FDA view it as a supportive data and recommended that we add additional data focusing on this group.
Okay, great. Thank you. Then a couple on the interim. you know, in SHIELD I, you had a max enrollment, threshold. Does that also apply for the unblinded interim in SHIELD II? You mentioned some blinded assessments prior to the unblinded assessment. Do you have a sense of when you can expect the first blinded assessment to occur?
Those are. First of all, there is, the blinded assessments are done internally on an ongoing basis. There's no real point to do that until the point we have a sufficient patient where we can actually get some understanding. This is something that was done in SHIELD I and will be done in SHIELD II on an ongoing basis. It's something that helps us see that we are within the statistical plan, within the underlying assumption. Obviously, there is no blinding here, so nothing about the effect, but an idea about the overall management of the trial and that things are going well. With regards to the interim, we do have, in the interim, the possibility to have a sample size reassessment.
I think it is a bit early to go into those details because the blinded assessment, what we are doing is around the SSI or I would say the primary endpoint, the understanding of the primary endpoint versus as an overall, versus our underlying assumption. Once we'll start to see how this is progressing, we can discuss in more detail. We do have the possibility, if needed, to have a sample size reassessment.
Okay, great. Thanks. Sorry, a couple more. You had partnering discussions ongoing for D-PLEX100 previously. Are those pretty much continuing, or did you kind of have to hit reset with the SHIELD I data? What about OncoPLEX? What, you know, what about partnering that? It seems like it's gonna be kind of on hold for a year or more, as you deal with D-PLEX100. Is that true? Any way to get that advanced maybe more expeditiously? Thanks.
Well, again, I'll start with the latter part of your question. Our top priority right now is obviously D-PLEX100, but we are fully intended to continue the development of OncoPLEX and potentially also other products in our pipeline, and it remains a priority. What we have done up until now is developing the CMC processes. As we continue our effort to begin clinical development, this will be a very valuable asset to get to this stage. I think another thing that is quite in a good stage is the preclinical package. Obviously, we will need additional tox study to go into the clinical stage, but this is a priority. You're right. As I said before, our focus is D-PLEX100, so obviously the resources that are invested in OncoPLEX in the near term are limited.
Yeah. I can add on the D-PLEX partnerships. All of the conversations that we had in the past, we're still in contact with all of these potential partners. There's actually a few new ones from other geographies that they showed interest in a partnering for different territories. This is all ongoing. Obviously, a lot of it will depend on the trial, but no one really stepped back and lost interest in the product.
Great. Thank you.
I would add to that one thing, which is the new thing that we are seeing with the robust data, the robust clinical data that we have, from SHIELD I, is a better understanding and some additional interest around our platform, around collaborating around the PLEX platform, pairing it with novel or known molecules in different area. This is very encouraging for us.
Okay. Very good. Thank you.
Thank you. There are currently no further questions. I will hand the call back to you.
Thank you for joining PolyPid's fourth quarter and year-end 2022 financial results conference call. I would like to emphasize firmly, we continue to believe in our long-term prospects, especially the potential of our promising late-stage product candidate, D-PLEX100. We remain grateful to our team members and all of our external partners for their commitment to our mission and their support in continuing to advance towards achieving our goal of bringing D-PLEX100 to healthcare providers and patients as quickly as possible. We look forward to speaking with you again on our next call.
Thank you. This concludes today's conference call. Thank you for participating. You may now disconnect. Speakers, please stand by.