Good morning and welcome to BiomX First Quarter 2021 Financial Results and Corporate Update Conference Call. Currently, all participants are in a listen-only mode. There will be a question-and-answer session at the end of this call. I'd now like to turn the call over to Marina Wolfson, Senior Vice President of Finance and Operations at BiomX. Please proceed.

Thank you and welcome to the BiomX first quarter 2021 financial results and corporate update conference call. The news release became available just after 6:30 AM Eastern Time today and can be found on our website at biomx.com. A replay of this call will be available on the Investor Section of our website. Before we begin, I'd like to review the Safe Harbor provision. All statements on this call that are not factual or historic statements may be deemed forward-looking statements. For instance, we're using forward-looking statements when we discuss on the conference call potential markets opportunities, the capabilities of the BOLT platform, the design, aim, expected timing, and interim and final results of our preclinical, clinical trials and studies, the sufficiency of our existing cash, cash equivalents and short-term deposits, our pipeline and momentum and the potential of our product candidates. Except as required by law, we do not undertake to update forward-looking statements. The full Safe Harbor provisions, including risks that could cause actual results to differ from these forward-looking statements are outlined in today's press release, which as noted earlier is on our website. Joining me on the call this morning are Jonathan Solomon, our Chief Executive Officer; Dr. Sailaja Puttagunta, our Chief Medical Officer; and Assaf Oron, our Chief Business Officer. With that, I will turn the call over to Jonathan.

Thank you, Marina, and good morning to everyone. In the first quarter of 2021, we continue to make substantial progress across our pipeline and we remain committed to achieving our goal of delivering novel natural occurring and synthetically engineered phage therapies that target pathogenic bacteria in the microbiome patients with unmet medical needs. We are excited to be part of the leading efforts in the microbiome space as this is a field which holds a lot of promise. Our approach is compromised the targeting specific strains of pathogenic bacteria in the microbiome that are strongly associated with the diseases and conditions we are investigating. Our rationally designed phage cocktails have the potential to restore the natural, healthy balance of the microbiome to provide patients with safe and effective treatment options. Using our proprietary BOLT platform, we can generate and screen large libraries of phage, prioritizing potential candidates based on cell activity and potency, as well as a number of other parameters that are important for drug development such as safety, stability, and ease of manufacturing. With a focus on executing our priorities, we have successfully and rapidly advanced our phage cocktail candidates in five indications and we expect that potentially clinically meaningful readouts in four different indications within the next 14 months. These important clinical milestones include a Phase 2 readout from our program of BX001 in acne-prone skin or results from the 8-week treatment period are expected in the third quarter followed by results from the 12-week treatment period in the fourth quarter. Next, for our BX001 program in cystic fibrosis, we expect results from Part 1 of our Phase 1b/2a trial in the first quarter of 2022 and results in Part 2 of this trial in the second quarter of 2022. We are also planning a Phase 1b/2a readout for BX003 program in Inflammatory Bowel Disease and Primary Sclerosing Cholangitis expect in the second quarter of 2022. Finally, by the first half of 2022, we expect Phase 2 proof-of-concept results for BX005 in atopic dermatitis. The combination capabilities of our BOLT platform along with broad acceptance of phage inherent safety enables to develop, manufacture and formulate novel phage therapy candidates that target particular pathogenic bacteria at an unprecedented speed. Having all these capabilities in-house has helped us build a diverse portfolio spanning various indications. To that end, I would like to discuss each program in detail. I will start off with BX001 in acne-prone skin. BX001 is a topical gel comprised of a cocktail of naturally occurring phage the target to bacteria Cutibacterium acne or C. acne, which is implicated in the pathophysiology of acne vulgaris. In March, we announced the initiation of our Phase 2 cosmetic clinical trial, and today, we are announcing completion of enrollment of 140 subjects with the results at the 8-week and 12-week treatment period expecting the third and fourth quarters of this year, respectively. The Phase 2 study will evaluate 140 subjects with mild-to-moderate acne vulgaris over a 12-week period and the key endpoints include safety, tolerability, and efficacy of the BX001. Additionally, we'll evaluate the clinical meaningful improvement of acne-prone skin as well as a reduction in C. acne burden, and we look forward to reporting on these results in the upcoming months. In February, we announced positive Phase 1a pharmacokinetic result of BX002 in Inflammatory Bowel Disease or IBD, and Primary Sclerosing Cholangitis or PSC. The data demonstrated that BX002 was safe and well tolerated when orally delivered with no serious adverse events. Additionally, the study met its objective in delivering high concentrations of viable phage to the gastrointestinal tract approximately 10 to the 10th plaque forming units, which equals approximately a 1,000 times more viable phage compared to the anticipated bacterial burden of Klebsiella pneumoniae in the stool of IBD patients. To the best of our knowledge, this was the first ever clinical study describing pharmacokinetics of an orally delivered phage under a U.S. Food and Drug Administration approved IND protocol. With these results in hand, we plan to advance this program through Phase 1ba trial of BX003 orally administered to either healthy subject or IBD or PSC subjects who are confirmed carriers of the target bacteria Klebsiella pneumoniae in their gut. Results are expected in the second quarter of 2022. With key endpoints evaluating safety, tolerability and efficacy of BX003, as measured by the reduction of the amount of target bacteria measured in stool. As you may recall, in November 2020, we consolidate our IBD and PSC programs into one product candidate named BX003 for both indications with a single broad host range phage cocktail that targets Klebsiella pneumoniae strains. Next, I will turn to our Cystic Fibrosis or CF program and our atopic dermatitis program, in which we recently announced BX004 and BX005 respectively, as a newly selected phage cocktail for each indication, respectively. We believe that our ability to quickly select these phage cocktail candidates further validates the cutting edge methodologies and capabilities of our BOLT platform. I will now turn the call over to Sailaja Puttagunta, our Chief Medical Officers, to discuss our CF program. Dr. Sailaja Puttagunta: Thank you, Jonathan. BX004 is a newly selected phage cocktail candidate designed to target Pseudomonas aeruginosa, or P. aeruginosa, a bacteria that causes chronic respiratory infections, and is the main contributor to morbidity and mortality in patients with CF. The current treatment options available to CF patients suffering from these chronic infections typically require prolonged and repeated courses of various antibiotics. And over time, their effectiveness diminishes as multi-drug resistant strains appear. BX004 has the potential to be both active against antibiotic resistant strains of P. aeruginosa and to penetrate biofilm, an assemblage of surface-associated microbial cells enclosed in an extracellular polymeric substance and one of the leading causes of antibiotic resistance. Based on our interactions with the FDA, we need to seek guidance, but due to the well established safety profile of phage, we could advance the BX004 directly into a proof-of-concept trial in CF subjects, thereby skipping preclinical toxicity and healthy volunteer studies. With the Company's desire to address as many patients as effectively as possible, we are working closely with the cystic fibrosis therapeutic development network, a network of leading U.S. based CF physicians. As a result, we are updating a Phase 2 proof-of-concept study to a Phase 1b/2a trial comprised of two parts in order to accommodate the recommendations of the cystic fibrosis developing network. These are the recommendations that the therapeutic developing network makes to all programs at this stage to help ensure steady consistency and patient safety. Additionally, we are pleased to announce that Dr. David Nichols, an experienced cystic fibrosis clinical investigator and clinician will be assisting us with this trial as the academic principal investigator through the Therapeutic Development Network. Part 1 of the Phase 1b/2a trial will evaluate the safety, pharmacokinetics, microbiological and clinical activities of BX004 with a single ascending dose, followed by multiple doses in eight CF subjects that are confirmed to have chronic P. aeruginosa respiratory infections. Results from Part 1 of this trial are expected in the first quarter of 2022. Part 2 of this trial will evaluate the safety and efficacy of BX004 treatment over 10 days in '21 CF subjects with chronic P. aeruginosa respiratory infections, the same population as Part 1. Results from Part 2 of this trial are expected by second quarter of 2022. We look forward to continuing to work closely with the Cystic Fibrosis Foundation in order to bring the safe and effective treatment to patients with CF. And now, I will turn the call back to Jonathan Solomon to discuss remainder of our programs.

Thank you, Sailaja. Turning our attention to atopic dermatitis program, we have recently selected a phage cocktail BX005 designed to target Staphylococcus aureus or S. aureus a bacterium associated with the development and exacerbation of inflammation in atopic dermatitis. S. aureus is known to be more abundant over the lesional skin of atopic dermatitis patients compared to the skin of healthy individuals or non-lesional skin of atopic dermatitis patients. The targeted bacteria also increases in abundance and becomes dominant when patients experience flares. We expect results in Phase 2 proof-of-concept clinical study evaluating the safety and efficacy of the BX005 in atopic dermatitis patients in the first half of 2022. Finally, the last program we'll discuss today is our Colorectal Cancer Program in which we're developing synthetically engineered phage designed to target strains of bacteria found in colorectal tumors. Currently, only a small percentage of new colorectal cancer cases respond to immunotherapy, which is believed to be due to the lack of novel tumor antigens and scarcity of immune cells and colorectal tumors. Our approach enables the phage to deliver cancer therapeutic payloads directly to tumors that are hard to reach or impact. We have observed in vitro and in vivo that our phage therapy can target strains of Fusobacterium nucleatum or F. nucleatum a bacterial species that is enriched in colorectal tumors. We are exploring phage-mediated delivery of payload genes such as dose and coatings immune-stimulating proteins, GM-CSF and IL-15, to colorectal tumors while also eradicating the target bacteria. Preclinical results from animal studies evaluating the use of our phage therapy in combination with checkpoint inhibitors are expected in the second and third quarters of 2021. As just described, our progress this quarter sets up for potentially meaningful results in four indications in the next 14 months. As we advanced toward mid-stage development in the microbiome space, we will continue to provide insights on restoring health to the microbiome by using phage therapies to remove bacteria that potentially drive pathology in diseases and chronic conditions. With all of our capabilities in-house and the understood safety of phage, we have the opportunity to provide patients with better treatment options. We are excited to continue investigating the clinical safety and efficacy of phage therapies for existing indications as well as possible new indications. Before I conclude, I would like to mention that we'll be holding a virtual KOL event highlighting BX003 for the treatment of IBD on Wednesday, May 26 at 8 a.m. Eastern Time. We believe that there is considerable potential for phage therapy to restore the balance in the microbiome for this condition. This will be a very interesting event with Dr. Ryan Balfour Sartor, a renowned academic expert in IBD, will be leading the discussion, and we hope you will join us. We look forward to keeping you informed on our progress. I'd like now to turn the call over to Marina Wolfson, our Senior Vice President of Finance and Operations to cover our financial results for the first quarter of 2021.

Thank you, Jonathan. As a reminder, the financial information is available in the press release we issued earlier today and also in more detail in our Form 10-Q, which will be filed later today. I will walk you through some of our brief highlights. Cash balance and short-term deposits as of March 31, 2021, were $53.6 million compared to $57.1 million as of December 31, 2020. We estimate that existing cash, cash equivalents and short-term deposits will be sufficient to fund the Company's current operating plan until at least mid-2022. Research and development expenses are $5.8 million in the first quarter of '21 compared to $3.5 million for the same period of 2020. The increase is primarily due to stock-based compensation and salaries and related expenses, mainly due to the growth in the number of employees in R&D, and clinical activities and expenses related to conducting preclinical and clinical trials of our product candidates. General and administrative expenses with $2.5 million in the first quarter of '21, compared to $2.1 million for the same period in 2020. The increase is primarily due to stock-based compensation, salaries and related expenses, mainly due to the growth in the number of employees and an increase in expenses associated with operating as a public company, such as directors' and officers' insurance. Net loss was $8.4 million in the first quarter of 2021 compared to $5.9 million for the same period of 2020. Net cash used in operating activities, $6.4 million for the three months ended March 31, 2021 compared to $6.9 million for the same period of 2020. We'd now like to open the call for questions. Operator?

Thank you. At this time, we will be conducting a question-and-answer session. [Operator Instructions] Our first question is from the line of Kristen Kluska with Cantor Fitzgerald. Please proceed with your question.

Hi, everyone. Thanks for taking my questions and congrats on completing enrollment in the acne study. The first question I have here is a big picture one. So, there was a recent study published in Nature, highlighting that the microbiome might have been more diverse in the past from comparing some samples that were up to 2,000 years old, and the authors also highlighted that the present microbiome has more of the antimicrobial resistant strains. So not sure if you're familiar with this particular paper, but I wanted to ask how you believe overtime microbiome composition has changed and how this could correlate with some of the more prevalent and chronic indications including some of what you're evaluating?

Hi, Kristen, pleasure you're chatting this morning. Very familiar with the paper, I think, very interesting work that follows on a bunch of papers before. And in general, I think you see more and more loss of diversity of the microbiome. And I think, there's a greater need to kind of engineer it precisely and avoid antibiotic resistance. So I think, at BiomX, we feel that this will play an essential role A picking up specific material without blasting the microbiome with more antibiotics, which is just causing more loss of diversity. And second, what we're seeing in some of these pathogens, kind of occupying niches, that, they're dominant in it. So with a phage, we can kind of open up the niche and enable engraftment of more diverse bacteria. So I think it all supports what we're all saying in research, from all across, right. We need greater diversity. We need to avoid using antibiotics as a therapy for these chronic indications.

And then, as you're progressing along the pipeline to the BOLT platform and also resorting to a personalized phage therapy approach for some indications because you remind us of the current phage bank you have on hand and efforts to expand this. And then what work would need to go into finding new phases if necessary to keep it within the rapid timeframes you've laid out?

Right. So, I think at BiomX, our conclusion has been that instead of investing in a large phage bank, we're actually investing in infrastructure and a large sample collection from whether it's various body of water, sewage, et cetera, whatever you can think of or we don't want to discuss it early in the morning. And you can see the progress, like I think when we came out with BX003, which is a broad cocktail that targets the strain of cocktail, both in IBD and PSC. That was quite an undertaking that we were skeptical, and it took us almost two years to complete. And now with Staph aureus would BX005, within two, three months, we already had a phage cocktail that covered 90% of the strains. So I think you're seeing kind of the economies of scale and the platform mature, as we learn how to handle, move quickly and sort of optimize all of our computational pipelines and robotic infrastructure.

Thanks. And for the atopic dermatitis study, could you walk through why you decided to evaluate a potential eight-week trial?

Sure. I'll let Sailaja to address that question. Dr. Sailaja Puttagunta: Thank you, Jonathan, and good morning Kristen. So, the atopic dermatitis because of the mechanism of action of phage where the hypothesis is, if we reduce the bacterial burden of Staphylococcus, that would then lead to a downstream change in the immune response and clinical improvement. So, to accommodate that, we wanted to at least allow an eight-week period to allow us to detect the downstream effects of reducing the bacterial burden of Staphylococcus.

Our next question comes from the line of Keay Nakae with Chardan Capital Markets. Please proceed with your question.

Jonathan, you've given us the timelines to report data from the various studies. I'm wondering with respect to BX003, BX004 and BX005, what are the gating items before you advance these into the actual clinical studies?

Right, so first, good morning, Keay. It was a pleasure. So I think generally at BiomX, we don't give guidance on initiation of studies. But as you know, the advantage of using this phage approach is that there is no talk study. There's no healthy volunteers study, right? So you can go straight to patient. So say most of these causes are currently in various stages of GMP manufacturing, kind of goes back, I think, to the question Kristen brought before, we quickly put together phage cocktails that look very promising. At that point, we can move straight to manufacturing, get ready and gear up for clinical study. And that's why we think these are maintained in the timeline to be updated on.

Okay. And in terms of the CF study design, when we think about the BOLT platform and the ability to use the learnings from initial patients to kind of zero in on an ideal formulation to advance. Are these numbers large enough to allow you to fully optimize the capabilities of both to get to that ideal compound?

It's an excellent question. I think in CF, we feel I would say more comfortable since there are case studies. The dozen patients that were treated so we have some data that we're basing our thinking and rationale, and again are benefiting from the support the therapeutic development network, the CF Foundation that are all part of this. But to your point, we're going to get a lot of data from these studies, right. We know exactly what strain the patients have. We know the effect, we know how their material composition looks after treatment. So far, we feel that BX004 looks very promising and could be the final product the go-to-market. But we can use a BOLT platform to make these tweaks and we think that there will be enough information, if needed to make these tweaks.

Okay. And then just back to the acne study. Congrats on completing the enrollment. From here, what do you need to I guess keep close tabs on to make sure that, when we get to the readout, no other, I guess unforeseen variables enter into the equation?

Keay, just a clarification question, you mean from the clinical aspect or like business development or? Q - Keay Naka: Yes, the first, Jonathan.

From the clinical aspect, okay. I'll let Sailaja to address that. Dr. Sailaja Puttagunta: Thank you, Jonathan, and good morning Keay. So yes, we're very pleased that we completed enrollment in this study and feel like we are on track to deliver top-line results from the 8-week endpoint in Q3 and then from the 12-week endpoint in Q4 of this year. Really, in terms of unforeseen variables that affect those deliverables, at this point, there we don't see any major obstacles, Keay and we believe we are on track to deliver.

[Operator Instructions] At this time, our next question is from the line of Joe Pantginis and this with H.C. Wainwright. Please proceed with your question.

Good morning, everyone. This is Matt Keller on for Joe. Thanks for taking the question. I’ve got one for you. Related to BX003, based on the previous data showing impressively high levels of gut PSC you guys have shown. How confident are you that you're in the right dose range? And relatively, how do you see fitting into possible FDA discussions possibly down the road when it comes to identifying a minimally effective dose?

Right. Good morning, Matt. I think as we feel rather confidence is at the levels we've seen had abundant levels of phage over bacteria. So again, what we know from the field, multiple studies our internal work is that usually you want to have around 10 phage for every given target bacteria. As a reminder, we achieve levels which were a thousand times higher than that. So there's definitely an abundance of phage, so that gives us a good therapeutic window together with the fact that the phage level stayed high for a few days. So I'd say, we're fairly confident moving into the next study, that we should get high exposure levels and hopefully detect a significant reduction in the bacteria accounts. In general, what we're trying to do in these initial clinical studies is actually to kind of go with a highest dose that is practical because you want to maximize the chance that there's abstaining an effect. Again, if we see a strong effect, we can start titering down the doses. But currently, this is not due to the cost of goods with phage not being prohibitive. It's not a major issue. So I think we can move forward with the current dose, but later in the clinical development we know it was a bit titer down.

Next question is coming from the line of Michael Higgins with Ladenburg Thalmann. Please proceed with your question.

Hi guys, thanks for taking the question and congrats on continued progress. Question for you on the couple of -- a couple I guess on the Phase 1/2 studies. Specifically in CF, what kind of dose range are expecting to be tested in the Phase 1b portion and again quantified by specific numbers at least some sort of a range from bottom to lower the interesting? Thank you.

Good morning, Michael. I let Sailaja address that question. Dr. Sailaja Puttagunta: Yes, thank you, Jonathan. So in terms of the dose change, the Phase 1a in CF, that study we're going to start with the single dose. That is in the lower end and in terms of going into specific testing a single dose first, plus safety and then we'll move into single dose that will be two logs higher than the original one. And we, like with all of our other phage there will be candidates, we don't anticipate any safety issues here but -- and so anticipate moving rapidly through the multiple dose phase of the Part 1b.

Thank you. And then I just a quick follow-up in terms of atopic dermatitis same question, I suppose. What can you provide for us in terms of what doses may be tested in that study?

Sailaja, please go for it. Dr. Sailaja Puttagunta: Okay. Thank you. So, in the atopic dermatitis the first in human study, we're only planning to take the one dose relative to placebo in that study, and move that forward we do believe that, that will be the effective dose. So, there's no dose ranging study planned for atopic dermatitis.

I guess this is a follow-up on that. What gives you confidence that you found the right dose to take into the Phase 2?

So I can jump in. I think here on the atopic derm rash is benefiting from the knowledge that we've seen in acne, right. And what we've seen to-date is that, usually, we want to go with the highest dose that we can. As Sailaja mentioned, there is no dose limiting toxicity to feel confident that that's the way you want to proceed. And again, we can calculate the ratio of phage to bacteria and we feel we're well within a good therapeutic window.

That's great and then just one follow-up on atopic dermatitis. How do you think you will work with other therapies in this study? Are they limited from using steroids gels and other atopic dermatitis treatments? Or is it a kind of an all-comers [indiscernible]?

I think let's Sailaja to address the clinical study and I can talk about just the general thinking of phage approach with other therapies. So Saliaga, please go ahead. Dr. Sailaja Puttagunta: Great. Thank you. So, for the clinical study, we are not planning any exclusions there and we're pretty much taking all comers. There will be some changes in terms of the washout periods based on existing therapies that patients have been on, but sort of that nothing really major.

Thank you. At this time, I'll turn the floor over to Jonathan Solomon for closing remarks.

So everyone, I wanted to thank you for joining us this morning. I want to thank the BiomX team, who worked hard to continue to develop phage therapies across a wide range of conditions as well as shareholders for the support and the patients participating in our clinical trials. It's a very exciting period for BiomX with actually four meaningful clinical readouts in the next 14 months, and we're excited to see the next few months. So everyone please have a wonderful day and please reach out to us if you have any additional questions.

Thank you. This will conclude today's conference. You may disconnect your lines at this time. Thank you for your participation.