Greetings, and welcome to the PolyPid third quarter 2022 conference call. At this time, participants are in a listen-only mode. As a reminder, this call is recorded, and I would now like to introduce your host for today's conference, Bob Yedid from LifeSci Advisors. Mr. Yedid, you may begin.
Thank you all for participating in PolyPid's third quarter 2022 earnings conference call. Joining me on the call today will be Dikla Czaczkes Akselbrad, Chief Executive Officer of PolyPid, and Ori Warshavsky, Chief Operating Officer for U.S. operations. Earlier today, the company released financial results for the three and nine months ended September 30th, 2022. A copy of the press release is available in the investors section on the company's website, www.polypid.com. I'd like to remind you that on this call, management will make forward-looking statements within the meaning of the federal securities laws. For example, management is making forward-looking statements when it discusses our ongoing clinical trials and the timing thereof, our expectation to extend the company's cash runway into the third quarter of 2023.
Our intention to publish important results from the SHIELD I study in a medical journal as soon as it is practical, top-line results indicate that patients undergoing complex surgeries with large incisions or patients with risk factors could potentially benefit from D-PLEX100. Our intention to use the impressive data from SHIELD I in discussions with potential partners regarding future pipeline products, including in oncology. Our belief that significant reduction in superficial and deep SSIs in large surgical abdominal colorectal wounds and in high-risk patients, as well as the safety data, are very encouraging. Our intention to discuss with the FDA the lower than anticipated overall infection rate in the study, driven by COVID-19 safety restrictions that were in place while our trial was being conducted.
Our intention to discuss the regulatory pathway for D-PLEX100 for the prevention of SSIs in abdominal surgery with U.S. and EU regulatory authorities in the first quarter of 2023, and the potential of D-PLEX100 to prevent SSIs in abdominal surgery. The potential innovation behind our lead product and preparations with ADVANZ PHARMA, and discussions with other potential partners, and the potential outcome of our anticipated meeting with the FDA and EU regulatory authorities. 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 which could cause actual results or events to differ materially. Accordingly, you should not place undue reliance on such 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 risk factors that may cause actual results or events to differ materially from those described in 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, November 9th, 2022. A copy of the slides the management team will review on this call can be found on the investors section, PolyPid's website at investors.polypid.com. With the completion of those prepared remarks, it's my pleasure to turn the call over to Dikla Czaczkes Akselbrad, CEO of PolyPid. Dikla.
Thank you, Bob. On behalf of our team at PolyPid, I would like to welcome everyone to our third quarter 2022 earnings call. I'm pleased to have the opportunity to provide you with a corporate update today during such an eventful period for PolyPid. I will begin with a discussion of the top-line results from the SHIELD I phase III study of D-PLEX100 for the prevention of surgical site infections or SSIs in abdominal surgeries, which we announced in early September. Beginning with slide three, as a reminder, SHIELD I, the largest study of infection prevention in colorectal surgery in over a decade, is a prospective global randomized double-blind phase III trial designed to assess the efficacy and safety of D-PLEX100 administered along with standard of care compared to standard of care alone arm in the prevention of post-abdominal surgery incisional infection.
The primary endpoint of the trial is the combination of incisional SSI, mortality, and surgical re-intervention due to SSI or wound complication, and determined by a blinded and independent adjudication committee within 30 days post-surgery. A total of 977 patients were randomized into the study, consisting of 488 subjects in the D-PLEX100 treatment arm and 489 patients in the control arm. The study was well-designed and well-executed as it was balanced on all baseline characteristic and demographic parameters. Importantly, the trial took place during the COVID-19 global pandemic, with the first patient recruited in July 2020 and the last in May 2022. We believe the precautionary measures put in place in hospitals during this time reduced overall infection rates. These precautionary measures included a reduced number of surgeries being conducted, disallowing visitors, and increased personnel and hospital hygiene practices.
We believe that these critical external factors significantly impacted the trial's statistical plan. On slide four, we take a closer look at the study population. Per FDA request, a pre-specified subgroup analysis was done based on incision length. The circle on the left indicates that 43% of total study subjects underwent complex surgeries with large incisions. The middle circle shows that nearly 70% of the total patients in the trial had at least one personal risk factor, including a BMI of over 30, smoking or COPD, diabetes, and hypertension. Of significance, each of these risk factors has the potential to increase the risk for SSI and other post-surgical complications. The circle on the right demonstrates that more than three-quarters of the total study subjects were cancer patients. Let's move on to the top-line results on slide five.
As we previously reported, in the intent-to-treat population, the local administration of D-PLEX100 and standard of care in 485 patients resulted in a decrease in the primary endpoint of 23% compared to standard of care alone in 4,489 subjects, representing a P-value of 0.15. However, in a pre-specified subgroup analysis requested by the FDA of a total of 423 subjects with incision lengths greater than 20 cm, the local administration of D-PLEX100 resulted in a statistically significant reduction of 54% in the primary endpoint compared to standard of care alone, representing a P-value of 0.0032. As I highlighted on the previous slide, this statistically significant reduction was achieved in a large subgroup representing over 43% of the patients in the intent-to-treat population.
Since the initial top-line readout was announced, we have continued to gather and analyze additional data from SHIELD I. This data has been increasingly encouraging. While we cannot get too granular at this time, as we intend to publish these important results in a medical journal as soon as practical, I would like to highlight that in a post-hoc analysis, D-PLEX100 also demonstrated a clinically important reduction of 34% in the primary endpoint in high-risk surgical patients, those with at least one personal risk factor, representing a P-value of 0.047. Now let's take a deeper dive into the large incision subgroup on slide 6. Most importantly, we see a large effect size in all efficacy parameters.
I'd highlight the decrease in the first two secondary endpoint, where the infection rate at 30 days post-abdominal surgery was 10% in the standard of care only arm, versus 4% in the D-PLEX100 treatment arm. I'd also point out the lower mortality rate in the D-PLEX100 treatment arm, as well as significantly fewer patients treated with IV antibiotics as treatment for adjudicated SSI. To conclude, on the efficacy aspects of the trial, we believe that the top-line results indicate that patients undergoing complex surgeries with large incisions or patients with one or more risk factors could potentially benefit from D-PLEX100. As you can see on slide seven, D-PLEX100 showed good safety profile in SHIELD I. Of significance, there was no impact on mortality in the D-PLEX100 arm compared to the standard of care.
In addition, there was 40% reduction in surgical reintervention in the D-PLEX100 treatment arm versus standard of care alone. Also, severe treatment adverse events occurred in 12% of the patients receiving D-PLEX100 versus 16% in the standard of care arm, and serious treatment adverse events occurred in 14% of the patients receiving D-PLEX100 versus 20% in the standard of care alone arm. Moving to slide eight. I think it is important to highlight how the overall results of SHIELD I truly validates the ability of our proprietary PLEX technology to locally deliver treatment over a prolonged predetermined period with minimal systemic effects. PK data collected in the trial showed very low concentration of doxycycline in the plasma for a prolonged period of 30 days as designed.
We intend to use this impressive data in discussions with potential partners regarding future pipeline products, including in oncology. In summary, on slide nine, while the overall top-line results for D-PLEX100 did not meet study statistical assumptions. The significant reduction in superficial and deep SSI in large surgical abdominal colorectal wounds and in high-risk patients, as well as the safety data, we believe are very encouraging. As such, we are in the process of preparing a package of data from SHIELD I and prior positive phase II studies for submission to the FDA and intend to discuss with the agency the lower than anticipated overall infection rate in the study, driven by COVID-19 safety restrictions that were in place while our trial was being conducted.
As previously stated, we expect to meet with the FDA regarding the regulatory pathway for D-PLEX100 for the prevention of SSI in abdominal surgery in the first quarter of next year. We plan to meet with EU regulatory authorities shortly thereafter. Based on the totality of the data generated to date, we remain confident in the potential of D-PLEX100 to prevent SSI in abdominal surgery. As we approach this anticipated meeting with the FDA, it is critical to contemplate a few potential outcomes. For example, the FDA may potentially agree that data could be sufficient for seeking approval in a narrower patient population based on the current collective data set. The FDA could require us to conduct another clinical trial or generate additional data. If we were to conduct another pre-approval trial, we currently believe that this trial would be a smaller, more targeted study.
From a regulatory perspective, we were pleased to recently receive confirmation from the European Medicines Agency, or EMA, that D-PLEX100 is eligible for submission of marketing authorization application in the EU under the agency's centralized procedure. The centralized procedure allows the submission of a single marketing application to the EMA that, if approved, enables the product to be marketed in all EU member states as well as in Iceland, Liechtenstein, and Norway. The centralized process eligibility is granted to D-PLEX100 under the therapeutic innovation criteria, which underscores that D-PLEX100 provides a new innovative alternative to patients in preventing abdominal SSIs. On a related note, I think it is important to also highlight that we proceed with our regulatory preparations with our European partner, ADVANZ PHARMA. In addition, we remain engaged in partnering discussions in multiple additional geographies for D-PLEX100.
Of course, it is unlikely that we will enter into any additional partnerships prior to the receipt of regulatory feedback. I would now like to provide a brief update on OncoPLEX, our lead intra-tumoral product candidate in oncology applied as a paste to the tumor resection area during surgery. OncoPLEX remains a priority for PolyPid, and we are currently finalizing CMC processes as we continue our efforts to begin clinical development for this promising product candidate. Moving on. As you know, we recently announced a cost reduction plan, including a 20% decrease in headcount across all departments. As we prepare for our planned regulatory interaction regarding D-PLEX100 early next year, we expect that these decisive actions will extend our cash runway into the third quarter of 2023 and further enhance the company's long-term growth strategy.
That is a good transition to now move into a review of our current financials. As of September 30th, 2022, the company had cash equivalents and short-term deposits of $18.1 million, which includes the $2.6 million upfront payment from ADVANZ PHARMA received in the third quarter. Also, as it relates to our balance sheet, during the third quarter of 2022, we sold approximately $600,000 worth of ordinary shares from our existing at-the-market facility. To reiterate, we expect that our current cash runway will extend into the third quarter of next year. Now, let's turn to our income statement. Research and development expenses for the three months ending September 30th, 2022 were $6.2 million compared to $7.3 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. Marketing and business development expenses for the third quarter of 2022 were $840,000 compared to $445,000 for the same period of 2021. General and administrative expenses for the third quarter of 2022 were $1.7 million compared to $2.1 million recorded in the prior year period. For the third quarter of 2022, the company had a net loss of $9.3 million as compared to $9.9 million in the prior year period. We will now open the call to your questions. Operator?
Thank you. As a reminder, to ask a question, you will need to press star one and one on your telephone keypad. Star one and one to ask a question and please wait for your name to be announced.
We will now take 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, appreciate all the color today. I'd love to just get, you know, just any color if there's precedent to get a sort of label for a certain size of incisions above 20 cm, whether, you know, in the U.S. or ex-U.S. Then how do you think that affects the commercial opportunity? You know, I can see it sort of playing out both ways where it gets on formulary and maybe gets used a little bit more broadly or maybe stays with formulary. Just any color in terms of your market research at this stage, if you did get sort of that narrower label, how do you think that may play out in practice? Thank you.
Thank you, Brandon Folkes, and good morning. I will start, and I'll let Ori Warshavsky elaborate more on the commercial opportunity. In terms of the labeling, our first discussions, our coming discussion with the FDA is regarding the regulatory path and the path for an NDA. Labeling will be discussed on a later stage. We do see very nicely with if you, for example, look at some of the negative pressure wound therapy, that the labeling is around prevention of or how they refer it, wound complication. They refer to wound complication. You do see that for example, if you look at Heron Therapeutics, their expansion of the indication that was granted, I think it was around May or June last year, the labeling is referring in their case to small to mid incision.
The reference to length of incision does exist. I think for us it's the next step. We first wanna make sure that we have a clear regulatory path for NDA submission, but definitely this is something that we are evaluating and we'll be discussing with the regulatory. You do see, as I just gave these two off the top of my head examples, you see reference in this line.
Maybe I'll take the commercial opportunity part. I think first, you know, maybe generally we need to understand that the trial was done during COVID. Even with COVID, we see almost close to 20% infection rate in these high-risk groups. Like one in six, one in five of the patients. You know, you can see how this can expand and even be even broader implications once hospitals go back to kind of, let's say, baseline or to normal operation. When we looked in market research, actually earlier this year, we asked doctors about their processes, how do they look at patients, what do they see?
Doctors know before the operation which patients are they're high risk, which operations will be more and more complex, which patients are more prone for infections. We ask them to assess or quantify this part of the population. In abdominal surgeries, which was actually a little bit surprising to us, 40% of surgeries are patients that are high risk. The way we want doctors, surgeons to look at our product is one more tool in their toolkit when they think of a prophylaxis, when they think of, okay, I need to, you know, do whatever I can to prevent infection in this high-risk group.
Now they have another tool in the toolbox that showed 50% reduction in complex surgeries and, you know, similar trends in the high-risk patients. Overall, I think there's an attractive starting point here. Of course, the plan is always and was from the beginning, let's get the approval and then generate more data and expand into a broader label. We believe that with COVID going away and volumes in the hospitals going back up and kind of returning to baseline, we will see the need just growing more and more.
Thanks very much. I appreciate the color.
Thank you. Thank you. We will now go to our next question. One moment please. Your next question comes from the line of Elliot Wilbur from Raymond James. Please go ahead. Hello, Elliot. Is your line on mute?
Yes. Can you hear me all right?
We can hear you now.
Okay.
Good morning.
Good morning. Dikla, I want to ask a question about the additional post-hoc data that you presented today in subpopulation with one or more risk factors.
Mm-hmm.
I mean, it looks like that is in isolation, independent of incision size, and I just wanted to confirm that. I'm just, you know, thinking about the interaction of the two categories. If in fact you've looked at data within large incisions with the additional inclusion criteria of having one or more risk factors. I just want to get your thoughts on that idea.
For Ori perhaps, just thinking about some of the additional secondary data points that have been presented, you know, seems like quite a few of those are gonna resonate well with payers and on the commercial side, but just, you know, wondering if you think any of these sort of stand out, you know, or maybe more favorable than original expectations, you know, heading into the trial and specifically thinking about number of reinterventions post-infection or number of subjects treated with antibiotics in order to adjudicate SSIs. But just any thoughts on some of the additional secondary efficacy endpoints that you think will resonate really well on the payer side. Thanks.
Thank you, Elliot . With regards to the post-hoc analysis regarding risk factor, you are correct. It's separate, and it's a separate group. It's 70%, by the way, of the patient population of this trial that has at least one patient-related risk factor versus the complex surgery with long incision is about 43% of the patient population in the trial. Of course, there is some overlap, quite significant overlap because in many cases the patients that are requiring more complex surgery also have risk factors. Most of the patients in the trial had at least one patient-related risk factor. Those are two different analyses. I can tell before I turn to Ori that in general this is the largest phase III in abdominal colorectal done in over a decade.
There is so much data that was gathered, both in terms of medical relevance, health economics. As we said in our today's prepared remarks, we can't get too granular about things because we do plan to publish it in a medical journal or in more than one article. We wanted to give a sense to investors and analysts since this is the first call since we published the top line of how much information and how much data has been gathered since and give the understanding of where we're focusing both our discussions with the regulator as well as with our partner and potential marketing. Ori, you want to follow to the second point?
Yeah. Hi Elliot. You know what I'm looking at, I think as a whole is around the complication. I think this is the message that will really resonate with the hospital, the reducing complications and time in the hospital. This is kind of a collection of what you mentioned as reinterventions and IV antibiotics and time at the hospital and readmissions and all this data. A lot of this data we're still working on. In some of this data, you know, we will need to further kind of investigate. I think there's a nice trend here around wound complication.
Another thing that actually Dikla and I were talking earlier today, you know, with this complexity you can see, you can think of impact on pricing, for example. You know, the higher risk group is the, you know, from the manufacturer there may be an opportunity here to look at the. It's more of a expensive product here. There's a few things we're looking into around this data.
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.
Good morning. This is actually Michaela on for Balaji, but thank you for taking our questions. You mentioned you're engaged in partnering discussions across multiple additional geographies. Just wondering if you could provide a bit more color on what we can expect here and really just the key criteria you're looking for in additional partners. Thank you.
Thank you and Hi Good morning. As we also said in our prepared remarks, we are continuing the discussions that started prior to the top line. Surprisingly for us, all of those discussions are continuing. We were very clear to say we don't think it's in our best interest before we have further clarity on the regulatory pathway forward to go into any final discussions even. It's just to reassure the interest and the continued interest and the unmet need. I think that Ori mentioned it a bit in his previous answer. If investors and listeners and stakeholders really think about it, D-PLEX was tested in the best condition maybe ever existed for hospital for surgery.
Best in terms of hygiene, best in terms of overloading the hospital, there was never before such a period that surgeon, hospital, patient had this extreme precautionary measure. Still, in this condition, especially in the complex surgery and with the lung incision, you see an overall reduction. This is indicated in slide five. You see an overall reduction in the primary endpoint from 18%- 8%. Companies that are focusing on this area are very much engaged and interested. I think that it's too early to set expectation here because we think it's in our interest to first meet with the FDA. As we said before, this is planned for the first quarter of next year, and only after that we can make a better assessment on what's the path forward in this discussion.
Thank you. We will now go to our final question. One moment. Your final question comes to the line of Roy Buchanan from JMP Securities. Please go ahead.
Hey, thanks for taking the questions. Yeah, I had a few. I guess SHIELD II did that remain in slow mode pending the regulatory meetings? Have those meetings actually been scheduled for the first quarter? It sounds like you have an agreement from the EMA that you can submit to MAA. I guess what do you need to get out of the meeting in Q1?
Let me first start with the last part. What we got from the EMA is a very lucrative path for a centralized process. It's not yet any indication of how they will evaluate the data or how they will review. As we also said in today's release, after setting a meeting with the FDA, shortly after, we intend to meet with the European authorities for, again, an advisory meeting. Once we follow that, we will have the option to then approve the product in a centralized procedure, which will enable us to get an approval at one time, and we will not be required to go country by country.
This is not really an indication on the path forward in terms of a actual approval, but just a very lucrative process in the sense that it's granted to products that showed innovation and it strengthens their our understanding of how they view the results that we've submitted from the phase II, as well as the innovative which the D-PLEX suggests in the anti-infective space. That's with the European authorities. Again, we said in the prepared remark, we are now in the process of preparing the package. We are in the last stages of preparing it and intend to submit it quite in the next few weeks.
Knowing the timeframe that is required from the time we submit the package to have a meeting, we are confident that we can meet with the FDA at the first quarter of next year. To answer your question, there is still not a specific date it was set.
Okay, great.
Oh, sorry. You also asked about SHIELD II. Yes, you described it correctly. It's in a very low-key mode, waiting for clarity on the path forward, and then we will decide if we can use this infrastructure or maybe convert it into a post-approval. We'll need to decide once we know what's the path forward.
Okay, great. Sorry, maybe I missed it, but what? How do you estimate the proportion of colorectal surgeries in the U.S. that have an incision larger than 20 cm? Then I think there was a directive in SHIELD I to use two vials of D-PLEX100 if the incision was larger than 20 cm, I believe. Was that followed, and is that a possible explanation for the superior results in that group, basically a dose effect? Thanks.
I'll start with the second part, and Ori will relate to the first part. The dosing, it is not specific to this trial. The dosing in abdominal surgery is based on the length of the incision. Up to 10 cm, one vial is sufficient. Moving on to 10 to 20, two vials are required. Over 20 cm, it is three vials that are administered. We did not see any indication at this stage that there were dosing issues, and we don't believe this is the case.
We do see, and if we need to explain, based on the information that we have now, on why there wasn't a statistically significant effect in the lower 20 cm, what we think is that the best explanation for that is that because of the various precautionary measures that we're taking during COVID, the overall infection rate in the standard of care arm was very, very low, less than 5%, which we haven't seen ever reported in abdominal colorectal resection prior to that. This really created a situation where there wasn't enough events to show statistically significant effect.
Maybe just on your question on the market. What we looked at in the past, what I mentioned before is looking at the complexity or the risk for infection. This was part of the market research, and this was 40% of patients coming into colorectal resection. It was all of our abdominal surgeries, but colorectal was very much in that same numbers. We're now looking into these large incisions. This was a group that we did not look previously in market research, so we're looking into that as well. But again, just to reiterate this, in any case, this is the starting point.
This is the initial label at approval, and we'll build or extend the label from there.
Okay. Thank you.
Thank you. I will now hand the call back for closing remarks.
Thank you for joining our third quarter earnings conference call. I would like to emphasize how firmly we continue to believe in our long-term prospects. We remain grateful to our team members and all 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.